MASARYK UNIVERSITY • FACULTY OF MEDICINE BRNO • CZECH REPUBLIC
SYMPOSIUM
NONINVASIVE METHODS IN CARDIOLOGY 2010
Edited by: HALBERG F., KENNER T., FISER B., SIEGELOVA J.
BRNO 2010
The Symposium takes place under the auspices of
Prof. PhDr. Petr Fiala, Ph.D., LL.M., Rector of Masaryk University Brno
Prof. MUDr. Jiří Mayer, CSc, Dean of Faculty of Medicine Masaryk University Brno
Ing. Petr Koška, MBA, Director of The St. Anna Teaching Hospital in Brno
©2010 Masarykova univerzita ISBN 978-80-210-5356-4
noninvasive methods in cardiology 2010
CONTENTS
1. Kenner Thomas, Moser Max
STABILITY AND OSCILLATIONS - AND THE UNIVERSITY AS A COMPLEX LIVING SYSTEM......................................................................................................................................5
2. Halberg Franz., Cornelissen Germaine, Cegielski Ning, Hillman Dewayne, Halberg Francine, Schwartzkopff Othild, McCraty Rollin, Finley Judy, Thomas Faithe, Kino Tomoshige, Chrousos George , Sonkowsky Robert R, El-Khoury Maroun, Ilyia Elias CIRADIAN DYSFREQUENTIA OF CORTISOL, MELANTOIN, DHEA, TESTOSTERONE AND ESTRADIOL......................................................................................................................9
3. Halberg Franz., Conrnelissen Germaine, Sothern B. Robert, Barnwell Franklin, Cegielski Ning, Ilyia Elias, Siegelova Jarmila
THE MOON' S AND THE GENES' TIDES AND DOUBLE TIDES PULLING THE BIOSPHERE..............................................................................................................................23
4. Cornelissen Germaine, Babayev Elchin, Halberg Franz
GENDER DIFFERENCES IN THE CHRONOME OF SUDDEN CARDIAC DEATH INCIDENCE IN THE ABSHERON PENINSULA, AZERBAIJAN........................................46
5. Cornelissen Germaine, Halberg Franz, Guillaume Francis, Schwartzkopff Othild, Finley Judy, Cegielski Ning, Rosch Paul, Siegelova Jarmila, Ilyia Elias
GROUNDING OR EARTHING: GLIMPSES AT PHYSIOLOGY AND PATHOLOGY.........51
6. Cornelissen Germaine, Palermo Judy, Halberg Franz
AEOLIAN CHANGES AND GENDER IN THE INCIDENCE OF CARDIAC ARRESTS IN MINNESOTA.............................................................................................................................57
7. Huynh William, Cornelissen Germaine, Huynh Richie, Huynh Ryan, Halberg Franz FEASIBLE AMBULATORY BLOOD PRESSURE AND HEART RATE MONITORING IN AMERICAN SECONDARY SCHOOLS TO ASSESS CHRONOMES IN CLINICALLY HEALTHY ADOLESCENTS....................................................................................................64
8. Cornelissen Germaine, Halberg Franz, Siegelova Jarmila, Galvagno Andrea
THE MOON'S IMAGE IN PROLONGED HUMAN ISOLATION.........................................69
9. Cornelissen Germaine, Halberg Franz, Finley Judy, Thomas Faithe,, Siegelova Jarmila, Dusek Jiri, Fiser Bohumil
URINARY OUTPUT AND GEOMAGNETISM REVISITED................................................75
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10. Schwartzkopff Othild, Hillman Dewayne, Halberg Franz., Cornélissen Germaine, Engebretson Mark, Katinas Georgie S., Chibisov Sergei M., Siegelova Jarmila, Agarwal Rajesh, McCraty Rollin
CIRCASEMIDIAN AND CIRCASEMISEPTAN GAUGES OF VASCULAR ADJUSTMENT AFTER TRANSMERIDIAN CROSSING OF THREE TIME ZONES.........80
11. Watanabe Fumihiko, Cornélissen Germaine, Watanabe Yoshihiko, Halberg Franz
A FAR-TRANSYEAR IN THE BLOOD PRESSURE OF A 17-YEAR-OLD MALE.............86
12. Watanabe Yoshihiko, Cornélissen Germaine, Halberg Franz, Siegelová Jarmila CHRONOBIOLOGICALĽYINTERPRED ABPM (C-ABPM) IN DELAYED SLEEP PHASE SYNDROME................................................................................................................90
13. Watanabe Yoshihiko, Cornélissen Germaine, Halberg Franz, Hillman Dewayne, Fišer Bohumil, Dušek Jiri, Homolka Pavel, Siegelova Jarmila
INFRADIAN MODULATION OF THE DEVELOPMENT OF HUMAN TRUE WHITE-COAT MESOR-HYPERTENSION.........................................................................................104
14. Sothern Robert B., Halberg Franz, Cornélissen Germaine, Hillman Dewayne, Katinas Georgie, Siegelova Jarmila
COMPLEMENTARY YET DIFFERING RHYTHMIC ASPECTS OF A MAN S MOOD AND VIGOR IN VARIOUS SPECTRAL REGIONS.............................................................120
15. Fišer Bohumil, Siegelová Jarmila, Dušek Jiri, Pohanka Michal, Cornélissen Germaine, Halberg Franz
NIGHT-TO-DAY BLOOD PRESSURE RATIO DURING SEVEN-DAY AMBULATORY BLOOD PRESSURE MONITORING.....................................................................................128
16. Siegelová Jarmila, Havelková Alena, Fišer Bohumil, Dušek Jiri, Pohanka Michal, Mašek Michal, Dunklerová Leona, Cornélissen Germaine, Halberg Franz
DAY AND NIGHT BLOOD PRESSURE VARIABILITY DURING SEVEN-DAY AMBULATORY BLOOD PRESURE MONITORING...........................................................133
17. Dobšák Petr, Sosíková Michaela, Al-Mahmodi Nabil Abdullah Ibrahim, Frantisová Michaela, Tomandl Josef, Spinarová Lenka, Jančík Jiří, Pohanka Michal, Fišer Bohumil, Siegelová Jarmila
HOME BASED REHABILITATION PROGRAM USING TRANSCUTANEOUS
ELECTRICAL MUSCLE STIMULATION IN PATIENTS WITH CHRONIC
HEART FAILURE...................................................................................................................139
18. Konečný Lumír, Pochmonová Jaroslava, Havelková Alena, Siegelová Jarmila, Dobšák Petr
HEART RATE VARIABILITY IN MULTIPLE CEREBROSPINAL SCLEROSIS...............146
19. Havelková Alena, Pochmonová Jaroslava, Konečný Lumír, Fišer Bohumil, Pohanka Michal, Siegelová Jarmila
SECOND PHASE OF CARDIOVASCULAR REHABILITATION IN PATIENTS
WITH ISCHEMIC HEART DISEASE....................................................................................158
noninvasive methods in cardiology 2010
STABILITY AND OSCILLATIONS - AND THE UNIVERSITY AS A COMPLEX LIVING SYSTEM
Thomas Kenner and Max Moser
Department of Physiology, Medical University Graz, A-8010 Graz, Austria Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH). Abstract
The main interest of chronobiology usually is focused on phenomena, which are controlled by internal clocks. Influence from outside is considered as important if it has influence as Zeitgeber or trigger of internal synchronization or disturbance.
We intend to discuss processes, which influence the stability of some internal or external system and therefore, lead to oscillations. We refer to phenomena, which are connected with the names Schumpeter and Kondratjew and can be observed as oscillations of large living systems. As one example for such considerations we discuss the chronobiology of our University.
Introduction
Oscillations can be found everywhere in nature, in non-living entities of all magnitudes - from subatomic particles to galaxies and even to our whole universe. Well analyzed are glacial periods and correlated oscillations of the temperature of the earth atmosphere. Periods and oscillations in living systems from molecules to cells and from organs to bodies and populations belong to the field of chronobiology (1,2).
Oscillations within a living body may be induced from an external source, like the sound waves acting on the components of the ear: the tympanic membrane, the ossicles and the oval window. The analysis and discrimination of the incoming oscillations is initiated in the cochlea from where the information is sent to the brain centers.
The transmission of sound-generated waves along the basilar membrane is similar to the transmission of pulse waves in the arteries. The similarity of the arterial pulse waves and the travelling waves" in the basilar membrane is remarkable - as was early interpreted by O.F. Ranke (3) who was familiar with arterial pulse waves. It seems remarkable that the "grand-master of biomechanics", Y.C. Fung together with his coworkers (4) suggested that messages, which are carried from different organs in the arterial pulses may be detected by analyzing the radial pulse. The transmission and reflection of arterial pressure waves may explain the processes, which permit to extract information by feeling and interpreting the radial pulse according to TCM. In the paper the authors (4) state: "although the discrimination is not very strong, the phenomenon is novel, and warrants further investigation."
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noninvasive methods in cardiology 2010
Externally induced oscillations are related to auto-oscillations and resonance. E.g.: When a person drives in a car on a bumpy street, internal organs as well as tissues from skin to bone oscillate in resonance. In general, such oscillations markedly influence the "ride quality" within a carriage - a bike, a car or a ship. The appearance of sea-sickness, thus is a chrono-patho-biological phenomenon.
Everybody understands what stability means. Stability of standing straight is improved by very slight swinging oscillations of the body. In terms of control theory one can explain these oscillations, which continuously adjust the position to the correct set point. Similarly a driver adjusts his car to the correct path by slightly moving the steering wheel. Instability of a car is indicated by increasing oscillatory movements and skidding.
One special possibility to produce instability of a system is, to insert a delay between the controlled variable and the controller. One example: if for some reason or because an experimenter has intervened, the baroreceptors recognize a sudden decrease of blood pressure only after several seconds, then the central blood pressure control system reacts too late. The consequence is: the blood pressure starts to oscillate (5).
It is interesting to note that the cellular internal clocks of our body are functioning according to the described method of delay of information. The following is a simplified explanation: The clock-gene generates a protein, which then, after a certain time blocks the function of the gene. After a further time the gene is again activated and the process is repeated with a constant period.
Chronobiology of a University
A group of interacting persons or a society can be described as a living system. The reports about the current and previous crises indicate the appearance of oscillations. It is, therefore, worthwhile to mention the names of Nikolai Dmitry ewitsch Kondratjew (1892 - to 1938) and Josef Alois Schumpeter (1883 - 1850). The latter was Professor of Economy at the University of Graz from 1911 to 1921. Both names are associated with the socalled "Kondratjew-cycles" or "Schumpeter -waves". These cycles or waves, which last about 30 to 60 years are correlated with achievement and development of inventions like weaving, use of steam engines, automobile-engines, aviation, computers etc. Independent of the answer to the question whether this kind of oscillations is a phenomenon of chronobiology, what happens certainly is not possible without life.
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noninvasive methods in cardiology 2010
lesr -" "w......* leor ■ *- - ■ ■ --ew.......i&r ■"
Among old documents in the Department of Physiology in Graz we found the diagram shown in the figure. It demonstrates oscillations of the attendance of students to Phsiology-lectures between 1863 - the year of the foundation of the Medical Faculty - until 1903. There are similar more recent oscillations of the number of medical students in Austria. A recent new law, which since 2005 permits only a limited number of medical students per university and year. It is not clear if this interruption of oscillations has specific consequences.
As a physiologist in the position of Rector of the Karl-Franzens-University in Graz (1989-91) and in the position of Dean of the Medical Faculty (1992-97) I was able to observe my Alma Mater as a complex living organism (6). From the viewpoint of historical development Alois Kernbauer (7) has vividly described the life-cycles of affluence of our University since the foundation in 1585. One special peculiarity of complex systems like Universities is their nonlinearity. The basic living components like teachers, students and supporting personal have different time-cycles of presence and aging within the system. The system is not closed, but is open to exchange with the environment and, in particular, to influences from outside sources. This includes reforms, which in Austria are ordered by federal laws.
In order to understand the function of a system like a University the aspects of time and timing has to be examined. Quantity and quality of the input-output relations are important and at the same time the different flows of information as well as the relation between information and knowledge including the storage of information and knowledge.
A reform is always something like an experiment, which in any case generates a disturbance. Marked changes in structure and function are the consequence. There exist characteristic time intervals, time periods and time constants, which permit to estimate the time course of normalization after a disturbance. The reaction, at least in part, may be called remodeling indicating the adaptive reaction of the system. An overruling of this reactive process may lead to a condition of shock (8). As an example, the remodeling after the reform of 1975, which changed the university from a rather patriarchic form into a democratic structure continued for at least 10 years, in some peculiar aspects even up to 20 years. From the viewpoint of a physiologist therefore, any reform has to consider quality, quantity and time of necessary adjustments.
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noninvasive methods in cardiology 2010
The recent reform, which changed the former Medical Faculty to a Medical University had an effect like a cell division. The consequence besides the oppression of student oscillations is a tremendous increase of bureaucracy, and construction activity to create space for personal. One hesitates to discuss the question, if the reform had an influence on the output which justifies the effort of all the modifications.
REFERENCES
1. Cornelissen G, Halberg F. Introduction to Chronobiology. 1994; Medtronic Chronbiology Seminar
2. Hildebrandt G, Moser M, Lehofer M. Chronobiologie und Chronomedizin. 1998; Hippokrates Verlag, Stuttgart
3. Ranke OF. Die Gleichrichter-Resonanz Theorie. 1931; Verlag Lehmann, München
4. Dai K, Xue H, Dou R, Fung YC. On the detection of messages carried in arterial pulse waves. J. Biomech. Eng. 1985; 107: 268 - 273.
5. Kenner T, Baertschi AJ, Allison JL, Ono K. Amplitude dependence of the carotid sinus reflex. Pflügers Arch. 1974; 346: 49-59.
6. Kenner T. Der Elfenbeinerne Turm - Analyse eines Organismus. < Inaugurationsrede als Rektor vom 8.11.1989 > 1990; Verlag J .A. Kienreich - Graz
7. Kernbauer, A.. Glanz und Elend der Universität im Wandel der Zeit. Der Sachverständige 1997; 3: 2-5.
8. Stiglitz, J. Die Schatten der Globalisierung. 2002; Siedler Verlag
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ORCADIAN DYSFREQUENTIA OF CORTISOL, MELATONIN, DHEA, TESTOSTERONE AND ESTRADIOL
Franz Halberg1, Germaine Cornelissen1, Ning Cegielski2, Dewayne Hillman1, Francine Halberg1, Othild Schwartzkopff1, Rollin McCraty3, Judy Finley1, Faithe Thomas1, Tomoshige Kino4, George Chrousos5, Robert P. Sonkowsky1, Maroun El-Khoury2, Elias Ilyia2
university of Minnesota, Minneapolis, MN, USA, 2DiagnosTechs, Kent, WA, USA institute of HeartMath, Boulder Creek, CA, USA, 4National Institute of Child Health and Human Development, Bethesda, MD, USA, 5First Department of Pediatrics, Athens University Medical
School, Athens, Greece
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
Abstract
We report a circadian endocrine frequency desynchronization from the societal routine of human salivary Cortisol, dehydroepiandrosterone, melatonin, estradiol and testosterone, during the latter part of an adynamic episode in the winter of 2009-2010 in JF, a 62-year-old woman. A condition of extreme fatigue and depression that lasted for several months, had recurred half-yearly for the past 20 years. With the methodology of chronobiologic serial sections, we quantitatively assess temporal changes in rhythm characteristics with their uncertainties and explore the sampling requirements for these hormones' circadian variation in both the desynchronized and the 24-hour synchronized state and for salivary aldosterone in the synchronized state. We dub an altered period (i.e., an altered frequency) as ecfrequentia if transient or as dysfrequentia if associated with illness. Ecfrequentia and dysfrequentia have the advantages of being hybrids (hybrid vigor), of brevity, having fewer syllables than frequency desynchronization, of complementing another rhythm alteration, ecphasia, and thus as a pair they may be more likely to be recognized (ringing bells). The prefix ec- from the Greek preposition ek (ek), as in the word eccentric (off-center), added to the Latin frequentia (frequency), makes ecfrequentia mean "off or outlying from the usual pattern of frequency", i.e., outside a given reference standard of peers preferably of the same gender and age. Dysfrequentia includes the Greek prefix dys-, which like Latin mal- meaning "bad" is the opposite of the Greek eu- (Latin bene-). Ecfrequentia may be used as a general term, but notably in cases when the condition is asymptomatic and/or limited to a 7-day record; the term includes dysfrequentia when the condition is accompanied by symptoms of unwellness.
Case report
A selenosensitive 62-year-old woman's (JF) circulation and all of her endocrine variables investigated desynchronize from the societal 24-hour routine during a (half-yearly recurring) episode of extreme adynamia ("downtime") of an extent that prevents her from getting out of bed (1,2). We here present chronobiologic serial sections of salivary Cortisol, dehydroepiandrosterone (DHEA), melatonin, testosterone and estradiol that were determined both during a downtime and thereafter, and of aldosterone, determined only during a stage of synchronization with society. In all other variables, except for aldosterone, the data start in a downtime, during which an oblique delaying time course of acrophases (peaks in the fitted 24-hour cosine function) are in keeping with a period longer than the 24-hour cosine curve fitted to the data. During resynchronization, the time course of the
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noninvasive methods in cardiology 2010
circadian acrophases becomes horizontal. 5159 ELISAs are in keeping with endocrine circadian desynchronization of the hormones investigated during the downtime, with a lengthening of their period perhaps as a result of a pull by the moon exerted upon a built-in circadian period. The data also illustrate sampling requirements insofar as the noisier the variable, the longer was the span to demonstrate to the eye the time courses of the acrophases of the variables investigated. Data. The numbers of assays for each hormone are given on top of each figure. Some changes in the patterns of values, possibly related to changes in the kits used for assay, can be questioned with the naked eye, e.g., in aldosterone. By contrast, other changes may be related to a depression of body activity, such as a lower midline-estimating statistic of rhythm, MESOR, M, and lesser circadian extent of change, the double amplitude, 2A, of Cortisol and the opposite for DHEA during the episode extending from the start of determinations to cycle 1 as a whole and as compared to the M and 2A after cycle 2. Results. Figure 1 shows, in the top row, the original data, in this case of salivary Cortisol, as do other figures for other variables. In the second row, the lower curve is the MESOR (M), with the standard error, SE, of M leading from the M to a dot below. The distance between the two curves in row 2 is the circadian amplitude, A, computed by the least-squares fit of a 24-hour (h) cosine curve, and the distance between the upper curve and the dot above it is the SE of A. The circadian acrophase, §, is seen in row 3, where cycles 3 to 6 show a horizontal time course corresponding to 24-h synchronization, with the peak occurring around midday for Cortisol (around -180°). The dots bracketing <|)s are their CIs (95% confidence intervals). The dashed horizontal lines in this row correspond to midnight; when the <|)s approach midnight (0° or 360°), they are doubly plotted. The oblique time course of <|)s shows circadian desynchronization at the start and in cycles 1 and 2, and resynchronization in cycle 3 and up to and including the first part of cycle 6. The fourth row of P-values from tests of the zero-amplitude (no circadian rhythm) assumption shows a dashed horizontal line corresponding to the 5% level of statistical significance. When a 24-h cosine curve is fitted to consecutive 72-h data sections (intervals) displaced in 12-h increments, many of the P-values in Figure 1 are below 5%. The data on other salivary hormones also show the initial desynchronization and subsequent resynchronization to 24 h, as seen by a more or less oblique time course of <|)s in row 3 up to cycle 3 and 24-h synchronization in this cycle and thereafter. By contrast with Cortisol, DHEA and melatonin in Figures 1-3, where P<0.05 in many 72-h intervals, data in these intervals on estradiol, testosterone and aldosterone are more noisy, Figures 4-6. No determinations of aldosterone were made during the episode of adynamia, Figure 6. In Figures 4-6, the interval used for analysis should be lengthened, but the 72-h interval used suffices to suggest that estradiol and perhaps testosterone were desynchronized, since the somewhat erratic <|)s cover the 24 h at the start but do not do so thereafter. Discussion. Chronobiologic serial sections as a local analysis of data in 72-h intervals and global analyses of longer sections of the time series and/or of the series as a whole (2) render these results part of a glocal (global + local) analysis and await follow-up. It is noteworthy that in the summer episode of 2010, following these hormone determinations, the desynchronized circadian period of systolic blood pressure as well as heart rate was of 24.8 h, corresponding to the double tidal period (3). The endocrine determinations allow only the documentation of the earlier circadian desynchronization in the winter of 2009-2010, followed by resynchronization in 2010.
A lengthening of the interval used for analyses to 168 hours (1 week) yields mostly statistical significance, notably during the 24-hour synchronized cycles 3-6 for estradiol, for testosterone, and to a lesser extent for aldosterone, as it does for Cortisol. In the case of aldosterone, a phase jump of unknown origin is seen. The desirability of added hormone determinations in JF is apparent from data on systolic blood pressure in cycles 6 and 7 from the recurrence of desynchronization in the second half of cycle 6 and in cycle 7 (not here shown). Further ELISAs could examine whether all variables change concurrently or in a sequence. In the latter case, a hint of the critical mechanism may emerge.
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JF is presumably the first patient with an adynamia associated with ecfrequentia or rather dysfrequentia showing a double tidal period in her blood circulation during the last episode investigated (summer 2010) as well as in self-ratings of mood during the prior episodes (preceding winter and summer). The moon's image is also found in one out of three >7-day records in the diastolic blood pressure of her grandchild. It is the more interesting that certainly three major hormones ~ Cortisol, DHEA and melatonin ~ and probably also the noisier estradiol and testosterone in saliva are desynchronized from the societal 24-h routine in this 62-year-old selenosensitive woman in the winter 2009-2010 episode of adynamia investigated; their periods are longer than 24 hours, but shorter than 24.8 hours (2). In the first months of the first two episodes investigated, in self-ratings and of systolic blood pressure and heart rate of the third episode, the period found was 24.8 hours, in keeping with a pull by the moon that can lengthen the period to the point of actual lunar synchronization. Conclusion. Ecfrequentia, long extrapolated from spotchecks limited at most to daily profiles, is here documented in the phase domain by a scan of more than the entire 24-hour span by acrophases with a delaying oblique time course for over a (lunar) month with resynchronization documented by a horizontal time course of acrophases for the following month(s). The extent to which circadian desynchronization, here clearly established, contributes to concurrent unwellness, and how unwellness can perhaps be prevented by maintaining synchronization, remains to be established.
REFERENCES
1. Halberg F, Kino T, Siegelova J, Homolka P, Finley J, Cornelissen G, Dusek J, Fiser B. Amplitude ratios of half-weekly vs. daily variability in diastolic blood pressure in putative magnetolability: with appendix. In: Halberg F, Kenner T, Fiser B, Siegelova J, eds. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, July 7-10,2009. (Dedicated to the 90thAnniversary of Prof. Franz Halberg.) p. 192-207. http://web.fnusa.cz/files/kfdr2009/sbornik_2009.pdf
2. Halberg F, Cornelissen G, Ilyia E, Cegielski N, Hillman D, Finley J, Thomas F, Kino T, Chrousos G, McCraty R. Selenosensitivity: half-yearly recurrent adynamia and loss of adrenocortical and vascular synchronization with society. In preparation.
3. Doodson AT. The harmonic development of the tide-generating potential. Proc Roy Soc Lond A 1921; 100: 305-329. See also http://en.wikipedia.org/wiki/Arthur_Thomas_Doodson
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Figure-1: JF: Cortisol
CHRONOBIOLOGV LABORATORIES - UNIVERSITY Of MINNESOTA
PHASE REF. 2009 5101 0000 PERIOD 24. DO HR INTERVAL 72. 0 0 HR START TIME 2010 Ollfl 0000
N OF DATA 949 INCREMENT 12. 00 HR END TIME 2010 0710 2355
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Figure 1. Chronobiologic serial section of salivary Cortisol in JF showing, in the third row, initial circadian desynchronization by an oblique time course of acrophases and subsequently, starting in cycle 3, 24-hour synchronization, apparent from the horizontal time course of acrophases. Note in row 4 that with the 72-hour intervals the zero-amplitude assumption can be rejected, more often than not by P-values under the horizontal dashed 5% line. See Figure 10 for most P-values at or below 1% with 1-week intervals used for analysis. © Halberg.
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noninvasive methods in cardiology 2010
Figure 2: JF: DHEA
CHROMOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF. 2009 0101 0000
PERIOD 24. Oft HR INTERVAL 72. 00 HR START TIME 201Ü ftllfl 0000
N OF DATA 94 9 INCREMENT li.OOHR END TlVE 20 1C 0710 235 9
1 2 3 4 5 8
TIME {days: numbers are lunar months)
Figure 2. Chronobiologic serial section of salivary dehydroepiandrosterone (DHEA) in JF showing, in the third row, initial circadian desynchronization by an oblique time course of acrophases and subsequently, starting in cycle 3, 24-hour synchronization, apparent from the horizontal time course of acrophases. Note in row 4 that with the 72-hour intervals the zero-amplitude assumption can be rejected, more often than not by P-values under the horizontal 5% line. Most P-values are at or below 1% with 1-week intervals for analysis (not shown). © Halberg.
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Figure 3: JF melatonin
CHRONOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF. ZOO 3 0
PERIOD 24. 00 HR INTERVAL ?2. 00 HR START TIME 2010 0
NOFQATA 737 INCREMENT 1!. CO HR EUD TIME 201D 0
101 D000 118 0000
710 23sa B9. s:
TIME (days: numbers are lunar months)
Figure 3. Chronobiologic serial section of salivary melatonin in JF showing, in the third row, initial circadian desynchronization by an oblique time course of acrophases and subsequently, starting in cycle 3, 24-hour synchronization, apparent from the horizontal time course of acrophases. Note in row 4 that with the 72-hour intervals the zero-amplitude assumption can be rejected, more often than not by P-values under the horizontal 5% line, mostly at or below the 1% or lower bottom line. © Halberg.
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Figure 4: J F testosterone
CHRO NO BIOLOGY LABORATORIES ■ UNIVERSITY OF MINNESOTA
PHASE REF. 2009 0101 0000 PERIOD 21. 00 HR INTERVAL 72.00HR START TIME 2010 D11B 0000
N OF DATA 94S INCREMENT 12.00HR END TIME 2010 0710 235$
1 2 3 4 5 S
TIME {days: numbers are lunar months]
Figure 4. Chronobiologic serial section of salivary testosterone in JF showing often that the zero-amplitude assumption cannot be rejected, but covering 360° in the first two cycles, but not thereafter. © Halberg.
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noninvasive methods in cardiology 2010
Figure 5: JF estradiol
CHRONOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF.
PERIOD 24. 00 HR INTERVAL T2. 00 HR START TIME
N OF DATA 944 INCREMENT 12.00HR END TIME
2009 0101 0000
2010 011S 0000 2010 0710 2399
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Figure 5. Chronobiologic serial section of salivary e stradiol in JF showing often that the zero-amplitude assumption cannot be rejected with the 3-day (72-hour) interval analyzed. The difference in phases scanning the 24-h span in cycles 1 and 2, but not thereafter, is nonetheless apparent. © Halberg.
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Figure 6: JF: aldosterone
CHRO NO BIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF.
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Figure 6. Chronobiologic serial section of salivary aldosterone in JF showing often that the zero-amplitude assumption cannot be rejected and suggesting a phase jump rather than a drift. © Halberg.
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noninvasive methods in cardiology 2010
Figure 7: JF estradiol (interval lengthened to 1 week)
CHRONO BIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF. £010 0101 OOQC PERIOD 24.00 HR INTERVAL 163, 00 HR START TIME 2010 Ol1fl 0ÖÖC
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Figure 7. Often statistical significance is gained with a lengthening of the interval used for analysis. Results with an interval of 168 hours are in keeping with initial desynchronization followed by resynchronization of salivary estradiol. © Halberg.
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noninvasive methods in cardiology 2010
Figure 8: JF testosterone (interval lengthened to 1 week)
CHRONOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF. 2010 0101 DO 0 0
PERIOD 24. 00 HR INTERVAL 16S.00HR START TIME 2010 Ollfl DODO H OF DATA B49 INCREMENT 12. 50 HR END TIME 201 0 0710 23S9
12 3 4 5
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Figure 8. Analyses with a 168-hour interval are in keeping with initial desynchronization followed by re synchronization of salivary testosterone. © Halberg.
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noninvasive methods in cardiology 2010
Figure 9: JF aldosterone (interval lengthened to 1 week)
CHRONOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHASE REF. 2010 0101 OOOfl
PERIOD 24. 00 HR INTERVAL 1S800HR START TIME 2 010 01 13 OOOfl hi OF DATA 031 INCREMENT 12.00HR END TIME £010 0 710 2 35fl
12 3 4 5
TIME (days: numbers are lunar months)
Figure 9. For the case of aldosterone, with intervals of 1 week used for analysis, phase jumps are more clearly apparent from cycles 3 to 4 and from 4 to 5. © Halberg.
20
19999999999996645777299999^^777029999933296067^^99992636
noninvasive methods in cardiology 2010
Figure 10: JF Cortisol (interval lengthened to 1 week)
CHROMOBIOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
PHA.SE REF. 2010 {11(11 OOOC
PERIOD 24. QU HR INTERVAL 1B8.00HR START TIME 2010 Q11 8 OOOC N OF DATA 949 INCREMENT 12.C0HR END TIME 2010 071 0 235S
1 t 3 4 5 5100 ELISAs pointing to the hypothalamic-pineal-pituitary-adrenal network, with circadian acrophases of Cortisol, DHEA, melatonin and sex steroids scanning obliquely (delaying) more than the entire 24-h scale during desynchronization associated with an adynamic episode. The endocrine acrophases change to a horizontal time course after re synchronization (Figure 11).
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noninvasive methods in cardiology 2010
Take-home message
~24.8-h and ~12.4-h periods are in keeping with a genetically-anchored resonance of living matter with earth-air and moon, as well as sea tides, among other critical periodicities of our solar system and from beyond it. A lunar pull may also act when periods happen to be intermediate between 24.0 h and 24.8 h. Two round (not flat), moving (not fixed) and heterogeneous magnets ~ sun and earth with its moon ~ interact, as seen along an evolutionary scale from an archaeon to a healthy person in isolation from society for 267 days and in a number of dominant 24.8-h periods in a selenosensitive grandmother and her granddaughter. The pull of the moon in a magneto-sensitive person may lead to an alteration of period (ecfrequentia) that may become a vascular variability disorder (dysfrequentia) associated with the circulation, Cortisol and other endocrines all getting out of sync with society and, with an accompanying loss of vigor, a half-yearly recurring adynamia lasting 2-3 months. The alternative of purely endogenous free-running is "simpler", perhaps only in the sense of making things as simple as possible but not simpler, as phrased by Einstein (47) "... the supreme goal of all theory is to make the irreducible basic elements as simple and as few as possible without having to surrender the adequate representation of a single datum of experience." The tidal and double tidal periods each are such data of experience.
REFERENCES
1. Halberg Franz, Cornelissen G, Katinas G, Syutkina EV, Sothern RB, Zaslavskaya R, Halberg Francine, Watanabe Y, Schwartzkopff O, Otsuka K, Tarquini R, Perfetto P, Siegelova J. Transdisciplinary unifying implications of circadian findings in the 1950s. J Orcadian Rhythms 2003; 1: 2. 61 pp. www.JCircadianRhythms.com/content/pdf/1740-3391-2-3.pdf
2. Halberg F. Physiologic 24-hour periodicity; general and procedural considerations with reference to the adrenal cycle. Z für Vitamin-, Hormon u Fermentforsch 1959: 10(3/4): 225-296.
3. Halberg F, Cornelissen G, Otsuka K, Katinas G, Schwartzkopff O. Essays on chronomics spawned by transdisciplinary chronobiology: Witness in time: Earl Elmer Bakken. Neuroendocrinol Lett 2001; 22: 359-384.
4. Halberg F. Physiologic considerations underlying rhythmometry, with special reference to emotional illness. Symposium on Biological Cycles and Psychiatry. In: Ajuriaguerra J de, ed. Symposium Bel-Air III. Cycles biologiques et psychiatric Geneva: Georg / Paris: Masson et Cie; 1968. pp.73-126.
5. Sanchez de la Pena S, Halberg F, Galvagno A, Montalbini M, Follini S, Wu J, Degioanni J, Kutyna F, Hillman DC, Kawabata Y, Cornelissen G. Circadian and circaseptan (about-7-day) free-running physiologic rhythms of a woman in social isolation. Proc 2nd Ann IEEE Symp Computer-Based Medical Systems, Minneapolis, June 26-27, 1989. Washington DC: Computer Society Press; 1989. pp. 273-278.
6. Halberg F, Cornelissen G, Sonkowsky RP, Lanzoni C, Galvagno A, Montalbini M, Schwartzkopff O. Chrononursing (chronutrics), psychiatry and language. New Trends Exp Clin Psychiatry 1998; 14: 15-26.
7. Apfelbaum M, Reinberg A, Nillus P, Halberg F. Rythmes circadiens de 1'alternance veille-sommeil pendant l'isolement souterrain de sept jeunes femmes. Presse Med. 1969; 77: 879-882.
8. Wever RA. The Circadian System of Man: Results of Experiments under Temporal Isolation. New York: Springer-Verlag; 1979.276 pp.
9. Sothern RB. Essay 12.1: Self-measurements in «Aschoff's Bunker.» In: Koukkari WL, Sothern RB. Introducing Biological Rhythms. New York: Springer, 2006, pp. 540-544.
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10. Miles LEM, Raynal DM, Wilson MA. Blind man living in normal society has circadian rhythms of 24.9 hours. Science 1977; 198: 421-423.
11. Remler O. Untersuchungen an Blinden über die 24-Stunden-Rhythmik. Klinische Monatsblatter fur Augenheilkunde und fur Augenarztliche Fortbildung 1948; 113 (2): 116-137.
12. Bryson RW, Martin DF. 17-ketosteroid excretion in a case of manic-depressive psychosis. The Lancet 1954; 267: 365-367.
13. Orth DN, King PH, Nicholson WE. Free-running circadian plasma Cortisol rhythm in a blind human subject. 58th Annual Meeting of the Endocrine Society, New York, June 1975, abstract 304.
14. Katinas GS, Chibisov SM, Schwartzkopff O, Cornelissen G, Halberg F. ~ 12-hour and ~84-hour oscillations during human adjustments to crossing time zones: more than waveform descriptors. Geronto-Geriatrics (in press).
15. Schwartzkopff O, Hillman D, Halberg F, Cornelissen G, Engebretson M, Katinas GS, Chibisov SM, Agarwal R, McCraty R. Circasemidian and circasemiseptan gauges of vascular adjustment after transmeridian crossing of 3 time zones or changing drug dosages. J Appl Biomed (submitted).
16. Barnwell FH, Halberg F, Cornelissen G. Chronomics of an intertidal fiddler crab's locomotor activity under aquatically tideless laboratory conditions. Proc Int Conf Frontiers Biomed Sei: Chronobiology, Chengdu, China, September 24-26, 2006, pp. 89-92.
17. Mikulecky M (ed.) The Moon and Living Matter. Kosice, Slovakia, Sept 23-25, 1993. Bratislava: Slovak Med Soc; 1993. 97 pp.
18. Mikulecky M (ed.) Sun, Moon and Living Matter. Bratislava, Slovakia, June 28-July 1, 1994. Bratislava: Slovak Med Soc; 1994. 159 pp.
19. Mikulecky M (ed.). Chronobiology & Its Roots in the Cosmos. High Tatras, Slovakia, September 2-6, 1997. Bratislava: Slovak Med Soc; 1997. 287 pp.
20. Kelly IW, Rotton J, Culver R. The moon was full and nothing happened: a review of studies of the moon and human behavior and human belief. In: Nickeil J, Karr B, Genoni J, eds. The Outer Edge. New York: CSICOP; 1996. pp. 17-34.
21. Koukkari WL. Essay 6.1: Earth tides. In: Koukkari WL, Sothern RB. Introducing Biological Rhythms. New York: Springer, 2006, pp. 214-216.
22. Whitehead K, Pan M, Masumura K-i, Bonneau R, Baliga NS. Diurnally entrained anticipatory behavior in archaea. PLoS ONE 2009; 4 (5): e5485. doi:10.1371/journal.pone.0005485
23. Halberg F, Conner RL. Circadian organization and microbiology: Variance spectra and a periodogram on behavior of Escherichia coli growing in fluid culture. Proc Minn Acad Sei 1961; 29: 227-239.
24. Cornelissen G, Halberg F. Do "protists" talk "circaseptan" as well as "circadian"?. Biochim Clin 1991; 15: 162-163. and: Chronobiologia 1991; 18: 114-115.
25. Halberg F, Cornelissen G, Faraone P, Poeggeler B, Hardeland R, Katinas G, Schwartzkopff O, Otsuka K, Bakken EE. Prokaryotic and eukaryotic unicellular chronomics. Biomed Pharmacother 2005; 59 (Suppl 1): S192-S202.
26. Fix JD. Astronomy. 2nd ed. Boston: McGraw-Hill; 1999. 641 pp; cf. p. 181.
27. Sothern RB. Essay 2.2: Time on Earth as we know it. In: Koukkari WL, Sothern RB. Introducing Biological Rhythms. New York: Springer, 2006, pp. 26-29.
28. Koukkari WL, Sothern RB. Geological history and rhythmic components. In: Introducing Biological Rhythms. New York: Springer, 2006, pp. 95-99.
29. Fanjul Moles ML, Cornelissen G, MirandaAnayaM, Prieto Sagredo J, Halberg F. Larger infradian vs. circadian prominence of locomotor activity in young vs. older crayfish. Abstract, 6° Convegno Nazionale de Cronobiologia, Chianciano, Italy, Nov 27-28, 1998. p. 65.
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30. Halberg F, Nelson W, Runge WJ, Schmitt OH, Pitts GC, Tremor J, Reynolds OE. Plans for orbital study of rat biorhythms. Results of interest beyond the Biosatellite program. Space Life Sei 1971; 2: 437-471.
31. Cornélissen G, Halberg F. Introduction to Chronobiology. Medtronic Chronobiology Seminar #7, April 1994, 52 pp. (Library of Congress Catalog Card #94-060580; URL http://www.msi.umn. edu/~halberg/)
32. Freund F. Pre-earthquake signals: underlying physical processes. Workshop on Validation of Earthquake Precursors by Satellite, Terrestrial and Other Observations (VESTO), Nishi-Chiba Campus, Chiba University, Japan, March 26-29, 2009.
33. Freund F. Toward a unified solid-state theory for pre-earthquake signals. Acta Geophysica 2010; 58 (5): 719-766.
34. Evstafyev V, Mikulecky M Sr. Recent biophysical researches explaining the mechanisms of lunar and solar links to the living matter. In: Proc. Man in His Terrestrial and Cosmic Environment. Upice, Czech Republic, May 18-20, 2010.
35. Halberg F, Cornélissen G, Ilyia E, Cegielski N, Hillman D, McCraty R, Finley J, Thomas F, Kino T, Chrousos GP, Mikulecky M, Strestik J. Half-yearly recurrent adynamia with loss of 24-hour synchronization: circasemiannual/circadian ecfrequentia. (Submitted).
36. Watanabe Y, Cornélissen G, Halberg F. Chronobiologically interpreted ABPM (C-ABPM) in delayed sleep phase syndrome. (In preparation).
37. Halberg F. Chronobiology: methodological problems. Acta Med Rom 1980; 18: 399-440.
38. Cornélissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T, eds. Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. pp. 796-812.
39. Refinetti R, Cornélissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692.
40. Halberg F, Siffre M, Engeli M, Hillman D, Reinberg A. Etude en libre-cours des rythmes circadiens du pouls de 1'alternance veille-sommeil et de l'estimation du temps pendant les deux mois de séjour souterrain ďun homme adulte jeune. CRAcad Sei (Paris) 1965; 260: 1259-1262.
41. Siffre M, Reinberg A, Halberg F, Ghata J, Perdriel G, Slind R. L'isolement souterrain prolongé. Etude de deux sujets adultes sains avant, pendant et apres cet isolement. Presse Méd 1966; 74: 915-919.
42. Reinberg A, Halberg F, Ghata J, Siffre M. Spectre thermique (rythmes de la temperature rectale) d'une femme adulte avant, pendant et apres son isolement souterrain de trois mois. CRAcad Sei (Paris) 1966; 262: 782-785.
43. Halberg F, Reinberg A, Haus E, Ghata J, Siffre M. Human biological rhythms during and after several months of isolation underground in natural caves. Nat Speleol Soc Bull 1970; 32: 89-115.
44. Cornélissen G, Halberg F, Siegelova J, Galvagno A. The moon's image in prolonged human isolation. (This volume).
45. Kripke DF, Elliott JA, Youngstedt SD, Rex KM. Circadian phase response curves to light in older and young women and men. J Circadian Rhythms 2007; 5: 4. doi: 10.1186/1740-3391-5-4.
46. Emens J, Lewy A, Kinzie JM, Arntz D, Rough J. Circadian misalignment in major depressive disorder. Psychiatry Res 2009; 168: 259-261.
47. Einstein A. On the method of theoretical physics. Philosophy of Science 1934; 1: 163-169.
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noninvasive methods in cardiology 2010
Table 1: Rhythm characteristics and their 95% confidence intervals (CI) for locomotor activity of a female crab (Uca minax) from Buzzards Bay, MA
Component Period (in hours) (CI) Amplitude (of „activity" hour) (CI)
1 12.47(12.46, 12.48) 1.46 (1.10, 1.83)
2 24.05 (23.95,24.15) 0.59 (0.22, 0.95)
3* 25.94 (25.79, 26.09) 0.44 (0.07,0.81)
*Beat frequency of components and 2 is 25.40 h; 25.95 h is the beat between component 1 and a
period of 24.00-h length.
Table 2: Recorded recurrent adynamia (A), overall self-rated vigor spectrum (B), lunar-cycle-related summaries (C) and endocrines during part of an adynamic episode (D)*
A. Start-end dates, lunar phase (f: date of full moon; n: date of new moon) and length (weeks) of spans of adynamia when recorded in winter (W) and summer (S)
2002 2003 2004 2005 2006 2007 2008 2009 2010
w - 01.18 f 02.17 f (4) 01.12 02.20 n (5) 01.05 02.15 (5) 12.25 n 02.14 n (7) 01.03 f 03.03 f (8) 01.08 n 02.21 f (6) 12.26 n 02.23 n (8) 01.02 f 02.28 f (8)
S 06.09 08.07 (8) 06.15 f 08.12 f (8) 06.17 n 08.18n (8) 06.20 f 08.09 (7) 06.04 08.28 (11) 05.31 f 08.12 n (10) ? 08.18 f (?) 06.09 f 08.08 f (8) Delayed*
*90 and 95% prediction intervals in 2010, computed from dates listed, are May 26-June 10 (90% PI) and May 22-June 29 (95% PI), respectively.
Table 3: Familial selenosensitivity in JF's family is supported by the moon's 24.8-hour image in circadian aspects of the circulation of a 3-year-old in the diastolic blood pressure on one of 3 spans (of hourly around-the-clock measurements for -15, ~9 and ~7 days) investigated#
Variable (unit) Period (hours) (CI*) Double amplitude, 2A (CI)
2009: 08/03 - 08/18
Diastolic blood pressure (mm Hg) 24.85 (24.04, 25.66) 13.50(6.00,21.09)
Systolic blood pressure (mm Hg) 24.40 (23.30, 25.51) 14.39(2.77, 26.01)
Heart rate (beats/min) 24.20 (23.14, 24.67) 27.92(18.08, 32.74)
2010: 05/07 - 05/16
Diastolic blood pressure (mm Hg) 23.99 (23.34, 24.64) 14.07 (7.94, 20.19)
Systolic blood pressure (mm Hg) 23.85 (23.19, 24.51) 17.94 (9.92, 25.96)
Heart rate (beats/min) 23.88 (23.57, 24.20) 30.19(23.71,36.67)
2010: 07/26 - 08/02
Diastolic blood pressure (mm Hg) 23.67 (21.89, 25.44) 4.20 (0.18, 8.21)
Systolic blood pressure (mm Hg) 23.94 (22.96, 24.93) 10.86 (5.57, 16.14)
Heart rate (beats/min) 24.01 (23.44, 24.58) 17.38 (12.63,22.13)
95% confidence interval
#Lunar period in diastolic blood pressure with no overlap of the 24-h period on one of three occasions investigated seems noteworthy in that LT was observed to be unusually energetic, talkative and somewhat resistant to parental guidance at new moons. The incidence rate of a point estimate corresponding to the double tidal period of 24.8 h was less than 1% of 270 -7/24 records of DBP of a 54-60-year-old woman and was also low in hundreds of 7/24 records obtained half-hourly around the clock in Urausu, Japan.
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noninvasive methods in cardiology 2010
Table 4: Free-running or pulled circadian cardiovascular and thermal rhythms in social isolation for >90 days*
Parameter MESOR Period (t) Amplitude
System Variable 95% confidence limits
Cardiovascular SBP 102.5 (101.6, 103.4) 24.57 (24.53, 24.60) 2.8(1.6,4.2)
MAP 78.5 (77.7, 79.2) 24.60 (24.59, 24.61) 2.4(1.3,3.5)
DBP 61.7 (61.0, 62.2) 24.56 (24.49, 24.62) 1.3 (0.5,2.2)
HR 60.6 (59.3, 61.7) 24.59 (24.56, 24.60) 6.9 (5.3, 8.7)
Thermal Sub 36.65 (36.58, 36.72) 24.56 (24.53, 24.59) 0.22 (0.14,0.33)
Axi 36.16 (36.10, 36.22) 24.60 (24.57, 24.62) 0.22 (0.13,0.31)
*27-year-old woman. SBP: systolic blooc pressure; MAP: mean arterial pressure; )BP: diastolic blood
pressure (all in mm Hg); HR: heart rate (beats/min). Sub: sublingual and Axi: axillary temperature (°C). Data analyzed by linear-nonlinear least squares rhythmometry. Period given in hours. The number of hourly means analyzed was 1632 for SBP, 1634 for MAP, 1635 for DBP and 1747 for HR; the corresponding total number of 26,403 original values stems from 6363 for SBP; 6295 for MAP; 6298 for DBP; 6777 for HR; and 335 for each Sub and Axi temperature. From ref. 5.
Table 5: Societal (24-h) and lunar asynchronization of circadian blood pressure (BP), heart rate (HR) and adrenocortical function (with possible lunar pull*), and lunar synchronization of vigor of JF during 41 days (of a longer span) of adynamia and unwellness for which Cortisol data are available (N: 236; 2010/01/18-2010/03/01)
Variable (unit) Period, t (CI) (hours) Amplitude, A (95% CI) t2 (days) A2 A2/A:
Vigor/wellness rating* 24.71 (24.10, 25.32) 2.01 (0.00, 5.66) 16.21 12.60 (8.98, 16.23) 6.27
Systolic BPf (mm Hg) 24.55 (24.44, 24.66) 10.83 (7.21, 14.45) 15.77 5.18 (1.43, 8.94) 0.48
Diastolic BPf (mm Hg) 24.63 (24.50, 24.77) 6.07 (3.63, 8.50) 14.06 2.05 (0.38, 4.47) 0.34
Heart ratef (beats/ min) 24.36 (24.24, 24.49) 4.08 (2.52, 5.65) 18.41 3.45 (1.82, 5.09) 0.85
Cortisol (nmol/L) 24.57 (24.44, 24.70) 2.97(1.82, 4.12) 14.73 0.23 (0.00, 1.35) 0.08
DHEA (ng/ml) 24.56 (24.46, 24.67) 3.21 (1.18, 5.25) 7.48 0.73 (0.09, 1.36) 0.23
*Note that only vigor's CI overlaps 24.84 (wherein the period was allowed to vary as a episodes.
i, the double tidal x, which x was found in an analysis parameter) of the first two of JF's investigated adynamic
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noninvasive methods in cardiology 2010
Table 6: Two distinct neighboring spectral components of JF's hormones may indicate a change in the period of just one*
Analysis Cortisol DH [EA
Period Amplitude Period Amplitude
Whole series 24.05 (23.95, 24.14) 2.29(1.71,2.87) 24.04 (23.97, 24.12) 0.97 (0.38, 1.55)
24.66 (24.55, 24.76) 2.06(1.40,3.72) 24.60 (24.52, 24.68) 1.02 (0.43, 1.61)
Part 1 24.69 (24.52, 24.86) 2.89 (0.65,5.12) 24.62 (24.47, 24.77) 1.69 (0.75,2.63)
— — 25.43** (25.13, 25.72) 0.96 (0.03, 1.89)
Part 2 12.02 (11.97, 12.07) 2.58 (0.48, 4.67) 12.04(11.99, 12.09) 0.59 (0.13, 1.05)
24.08 (23.96, 24.19) 4.54 (2.51,6.57) 24.10(24.02, 24.18) 1.54(1.08, 1.99)
*When a glocal analysis of a series c ealing with salivary determinations of two adrenocortical
hormones at 4-hour intervals around the clock covering 2 months was analyzed as a whole, it revealed, in each case, two circadian periods, x, one t1 with the CI (95% confidence interval) of x overlapping 24.0 h, the other x2 with a CI overlapping neither 24 h nor the CI of T1 as seen in the top row of the table for each Cortisol and dehydroepiandrosterone, in a global analysis. Chronobiologic serial section then revealed first desynchronization with a longer than 24-h period, with an oblique time course of acrophases, §, followed by 24-h synchronization with a horizontal sequence (not here shown), and delineated two different intervals of the time series for a local scrutiny. When the series were thus separated into two parts with the separation based on the change of the time course of <|)s in the serial sections and each part was analyzed separately, each of two endocrine data sets revealed only one or the other about 24-h circadian component (locally in time) rather than the 2 found globally (in the series as a whole).
**Probably another indication of a change in period that requires scrutiny in a serial section to find out whether separation needs to be done again, a task remaining, and if so where.
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noninvasive methods in cardiology 2010
AiEnfc Lnil Sqiirn SpKlr* atS*ltolk {5> aid DiaitdJic I Dl rYdssuru HIS1 iind
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td dl 1d i] 10 II IP J) ±ii ..•. *n:z±£ a>ii: clock, modi} M -WV-minute intervili (with short intcrn^liuns:- «iih jbi ainKiil.il. m k Hb (TM-Z*M i hm AAD (Tokyo. Japan I.
Figure 1. Prominent 24-h synchronized period and its harmonics in the circulation of GC, a clinically healthy woman 54-60 years of age, under conditions of life in society. © Halberg.
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noninvasive methods in cardiology 2010
CRAB (Uca mine*) LOCOMOTOR ACTIVITY
CHRQNOBlOLOGrC SERIAL SECTIONS (LEFT) 8, PLEXOGRAMS (RIGHT) Summary at iwo tnas penrxfs (t)
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Figure 3. Earliest life may well be characterized by a lunar (tidal, top), lengthening (middle) and solar (circadian, bottom) average period, which in their turn must be analyzed for changes as a function of time when given appropriately long time series (see Figure 4B). © Halberg.
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noninvasive methods in cardiology 2010
E.toli Growth Rite in Fluid Culture-
m m n f» i» *•* «
ihůui ifter stfal of colonyi
E.c[}li Growth Rate: Global Analysis Suggests F'ee-Running' ;Mjlb#rg ArdCofiiMr. 1*41]
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Figure 4A. Time plot of the 1930 data of Lore Alford Rogers and G.R. Greenbank, anoted bacteriologist described by a Cosmos Club (Washington, DC) Vignette of December 1967 as "the bright star in the [US Department of Agriculture] scientific horizon before World War II". In 1961,the data on growth rate (actually colony advance) of E. coli assessed at hourly intervals for slightly over 6 days were taken off the graph published by Rogers and Greenbank in 1930. Some regularity in the time series is apparent from the spikes in colony growth occurring at intervals shorter than 24 h, as seen by reference to the vertical dashed lines drawn at daily intervals, yet eyeballing can hardly serve for an estimate of a period and certainly forestalls any evaluation of uncertainties. Rogers and Greenbank wrote: "Fig. 1 [on top], which is representative of a number of experiments, shows that there is a considerable degree of periodicity to the alternation of rapid and slow growth." In considering this graph, it should be kept in mind that the curve represents not extent of growth, but rate of advance of growth for definite time periods. The number of bacteria in the different periods could not be determined. © Halberg.
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noninvasive methods in cardiology 2010
E.coM Growth Rale: Follow-up on 1SG1 Analyses*
J ? I! !: i 0 "5 '.Z
Time (dJVJ íHtr t>ríúlon/|
■Hrjl rsluf at 2 i ľiojrs after Vial U1 COlí^v. "94ur|5 tr sn? ruii niignrrf í= t dp^ni Ľť 2-oaY ir^rv^i mpjod p'ú9'c55ivt f bf hotŕi LhroijighrAJt. 1he iiecQrd
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E.coli Growth Rats: Follow-up on 1961 Analysts'
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2 E 4 0 u Time [days]
mFwiA valjn al 25 l-duí* ďtLer atari organy, rtlulti dí arulysns aaargrad 10 rn'dwin: í-J ľ--^ľ nlnrvnl movrd prDgreji'víly t>v 6 ho-jrr, tirQjgľoul lna rcocrd
Figure 4B. Periods and corresponding 95% CIs characterizing the data shown in Fig. 4A are here estimated for intervals of 2 days progressively moved throughout the time series by 6 h. An interval of 2 days was selected to have at least one replication to secure a more reliable estimate of the period while also allowing the investigation of any change in period length with time. Separate, non-overlapping 1-day intervals analyzed similarly yield acceptable similar estimates. The period is seen to lengthen as a function of time. As a first approximation, the dash-dotted line is in keeping with a linear increase. This increase is only of about 18 h at the beginning of the series, but approaches 24 h by the end of the first week of monitoring. With the qualification that consecutive estimates are not independent, the lengthening of the period has an ordering P < 0.001 (r = 0.90). The fit of a second-order polynomial (solid line) suggests that the period levels off. In this model, the quadratic term significantly reduces the residual variance (ordering P < 0.02) beyond the linear term. The results could be interpreted as an originally free-running circadian component that may be pulled by (if not become synchronized with) the 24-h day. © Halberg.
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noninvasive methods in cardiology 2010
B
Gir^Qta* tQinHi'tiH pi lpNgp4'<'4"<4i I'll
in fprntlr Ulf, -A.If, »b»jr fi. UfenHn A4*
f» Diir*r(iii l^iiuq Aifi>t«*
"M1 ........-j i iTi -mi. 1*
synchronised" Cifcadian Peanod Ol Cafe TafflpofQluro TcflorrtLitEirfnd Ifom Ambulatory S, U and E R;i1f; in Continuous Light of Lchu Intently
1
S30;.
U
Sotar
a
^1
Figure 5A and B. The double tidal period of telemetered core temperature of rats kept in continuous light of low intensity in the presence (A) but not in the absence (B) of the suprachiasmatic nuclei. © Halberg.
37
noninvasive methods in cardiology 2010
Predominantly 24-hunr rwlhtr thnn 24,S-hour Synchronization
Histograms nf Point Kslimatts of f'ircaJian Period of Si stuht ,S) Diastolic (D) Blood PresjMr* (IJPi and Hni-ailijiHi.ftiJilJHJ.p-J»'-Ir'jhihphi.htli + ltl
Figure 6. Periods encountered in mostly consecutive acceptable 270 ~7-day sections of vascular variables of GC, a clinically healthy woman. The incidence of a double tidal period varies from zero to less than 1% in the three variables investigated. © Halberg.
38
noninvasive methods in cardiology 2010
Delayed sleep phase syndrome (H5, male) associated with minor peaklets in both the double tidal and tidal spectral regions, each overshadowed by 24-h and 12-hour components'
1.M)
0-5 10 15 2.0
Frequency (cycles/day)
3 0
'Original data of Dr. YosNihiko Walanabe,
Figure 7. A 24.7-hour peaklet (encountered adjacent to a dominant 24-h synchronized circadian) and a 12.9-h peaklet (next to a dominant 12-h component) are minuscule in the spectrum of systolic blood pressure of a clinically healthy physician prior to an episode of delayed sleep phase syndrome (DSPS).OHalberg.
39
noninvasive methods in cardiology 2010
pflMl* |r4*|-W IhOOTl «i JF. ■ tt-W-tM Mtomttt*** "W*
I:
LI
f
r
-
DIClJtllHD. 1
h H
la
U
I
(mniHr-iriiil'jIr:
Figures 8A and B. Obj ective indications of the moon are mirrored in a case of a circadian and circasemidian dysfrequentia (circadian frequency desynchronization from the societal 24-h routine and possible lunar synchronization) of some of the variables investigated in a 62-year-old subjectively seleno-sensitive grandmother during the first month of an adynamic episode in the summer of 2010. © Halberg.
40
noninvasive methods in cardiology 2010
REPLICATED LUNAR SYNCHRONIZATION OF JF's VIGOR DURING FIRST MONTH (SHADED] OF (TWO-MONTH-LONG) ADYNAMIA EPISODES*
PERIOD
j i a n n .' n v id 11
7 ^ TIME [LUNAR CYCLES) 1
TwrnriwHtritw W mocni (JF n*wi*ncn* Domain
t ^ 24.0 hour*
t i i 1 * i 1 H u ** ii 4«
m m w in a* uc m ■• i» t*'ip'- /juiofl ■ C«»4p rtotkui few ifcaat 3 ■J— IdfrnflJ If} «Vr»jh#,rfi.ih»lM*i *ilh Jw .2 J-h« luubn. rainH bfr tfcwtwbctegWiJ iff^ mu IhmvilMHn >j uttiwlqih* of l*e pc*li in the ipwctnn (tnOn hfh^ Ntofcaf j^utpouaMt
(h*™ k-nj i« cm> ilw—iiy fi*i«p«Krt» «*h iwp tlifhh dirtW* |^na Aar^f fal (top M> ml wiwnHntkMk leltU*ir*4ihrnrm Tfuceita mplmnk iwfcle pe»L n MTU* k*>J ™*JiCml*rfatrti frtlipilteiU. Altai! priwnl i-*il> Jminp hatfc!* *pm Vcr> «nm£Uid*Aj*** icnk In mm mciuhtfftj h.ilTTii tix. rrVi. lifTKtf
Figure 12. Artificial two major peaks resulting from a change in period. © Halberg.
44
noninvasive methods in cardiology 2010
AeroTJliiisu t tun^c \ such as a Jump into Antiphase l Ki-sult* in Multiple SpcciraL K'aVi*
Time Domain Fmpienc} Dofniin
4-0
4 UfJirsL hjlO jtiJ* - almond h*\i-
VV/VV 1
* Iiif intlnc, ulirr return Irurti a M Jiivrm-iijuft fli^hr *ctmb> 7 or ■DM *Pte wm k.!in.>i*if>Aif.K-il *rt*l tcvi"*t
Ihrnxnitaf mn hj uvubtMHl of l»v fvA» in ita >r<\"trjm i bcrkm* ri(**) tinlti^ hwi sUition («'■ »mw<..'iJjl n»rii|»**|ili wilh t-ifiH1 pcm\l htA in anti]4uo« llcf aid ■■ilfli kill durmy JjU«ctn ipm (bctfcx* | tprcud tnwf».«m«j ii*jK#cnv i*K j Ji»cfrtti; in phaw or it ungk component Vcrj rail ujrlofrn rrwh irpm itifts ■ i1
■nun) Intfth Im **t nuih ipU- of cfcf cj ilc Ifnpt.
Figure 13. Artifical two major peaks resulting from a change in phase. © Halberg.
45
noninvasive methods in cardiology 2010
GENDER DIFFERENCES IN THE CHRONOME OF SUDDEN CARDIAC DEATH INCIDENCE IN THE ABSHERON PENINSULA, AZERBAIJAN
Germaine Cornelissen1, Elchin Babayev2, Franz Halberg1
1 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA 2 N. Tusi Shamakhy Astrophysical Observatory, Azerbaijan Nat Acad Sciences, Baku, Azerbaijan
Aim. To explore genetic and/or epigenetic associations of the sex chromosome with photic and non-photic cycles in the incidence patterns of sudden cardiac death in Baku and the Absheron Peninsula (Azerbaijan).
Materials and methods. The daily incidence (on most days) of sudden cardiac death (SCD WHO code ICD-10, classification 146.1) in the Absheron Peninsula, including the capital city Baku (Azerbaij an, > 3 million inhabitants) was obtained from 21 emergency and first medical aid call stations and a central station between 15 Nov 2002 and 30 Jun 2009. The date and time of occurrence was recorded together with gender and age (only cases in age range between 25 and 80 years were considered). There were 401 cases of SCD in women and 1,786 in men. For circadian analyses, the SCD incidences were stacked over an idealized 24-hour day and the number of cases per hour was counted separately for men and women. The data were analyzed by cosinor, involving the fit of cosine curves with periods of 24 hours and harmonic terms separately or jointly (1-3). Parameter tests (4) served to examine any gender difference in the circadian patterns of SCD. Daily incidences were also analyzed by least squares spectra to identify major spectral components, further resolved by nonlinear least squares to obtain point and 95% confidence intervals (CIs) for the period in addition to the MESOR, amplitude and acrophase, using Marquardt's algorithm (5).
Results. Overall, the circadian pattern of SCD incidence can be modeled by a two-component model consisting of cosine curves with periods of 24 and 12 hours (24-hour: PR=48%, PO.001; 12-hour: PR=28%, P=0.001; composite model: PR=76%, PO.001). In men, as expected, the fundamental amplitude is the largest (24-hour: PR=48%, P<0.001; 12-hour: PR=20%, P=0.011; composite model: PR=68%, PO.001). In women, however, the opposite is true (24-hour: PR=24%, P=0.003; 12-hour: PR=47%, PO.001; composite model: PR=71%, PO.001), Figure 1. The difference in circadian pattern between men and women is statistically significant and consists primarily of a larger 12-hour harmonic in women as compared to men, Figure 2.
Apart from long-term trends not assessable on the basis of the relatively short records, the daily incidence of SCD in women is characterized by a circannual component, Figure 3. Using as initial periods 1.0 and 0.5 year, nonlinear estimates of 1.016 [CI: 0.936, 1.095] and 0.517 [CI: 0.493, 0.541] year are obtained, overlapping the anticipated respective photic and geomagnetic environmental counterparts. Among others, a far-transyear with a period of 1.65 [1.43, 1.86] year is also detected, as is a cis-half-year with a period of 0.388 [0.377, 0.398] year, slightly shorter than the about 0.42-year component characterizing solar flares (6), also reflected in physiology (7). An about-yearly component of much smaller amplitude is also found for men, Figure 4. Among others, a cis-half-year with a period of 0.375 [0.363, 0.387] year, similar to that seen in women, is also detected, as is a relatively prominent cis-year with a period of 0.763 [0.736, 0.790] year not found in women.
46
noninvasive methods in cardiology 2010
Discussion and conclusion. Larger databases will be needed to investigate putative reasons underlying the larger prominence of the 12-hour versus 24-hour component characterizing the incidence of SCD in women, to determine whether the difference relates to no more than a difference in circadian waveform, or whether it may involve a separate mechanism more specifically related to the 12-hour component, as discussed elsewhere in this issue. Gender differences were also observed in the number of cases, with much fewer cases in women than in men. Gender differences observed in the time structure of SCD incidence have also been reported for the incidence patterns of suicide in Minnesota and in Australia (8, 9). Solar activity reportedly affects the gender ratio and modulates lifespan (10), among a host of other effects (11). Some critical environmental-biospheric associations occur primarily at non-photic para-annual and para-semiannual frequencies, including SCD which is further characterized by geographic differences (12, 13). Further systematic assessment of gender differences in spectral features and exploration of putative underlying physiological mechanisms may help understand how space weather exerts its influence on biota.
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH). REFERENCES
1. Halberg F. Chronobiology: methodological problems. Acta med rom 1980; 18: 399-440.
2. Cornelissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T (Eds.) Encyclopedia of Biostatistics, 2nd Ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
3. Refinetti R, Cornelissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692
4. Bingham C, Arbogast B, Cornelissen Guillaume G, Lee JK, Halberg F. Inferential statistical methods for estimating and comparing cosinor parameters. Chronobiologia 1982; 9: 397-439.
5. Marquardt DW. An algorithm for least-squares estimation of nonlinear parameters. J Soc Indust Appl Math 1963; 11: 431-441.
6. Rieger E, Share GH, Forrest DJ, Kanbach G, Reppin C, Chupp EL. A 154-day periodicity in the occurrence of hard solar flares? Nature 1984; 312: 623-625.
7. Cornelissen G, Tarquini R, Perfetto F, Otsuka K, Gigolashvili M, Halberg F. About 5-month cycle in human circulating melatonin: signature of weather in extraterrestrial space? Poster presentation, Fourth UN/ESA/NASA/JAXA Workshop on the International Heliophysical Year 2007 and Basic Space Science: "First Results from the International Heliophysical Year 2007", Sozopol, Bulgaria, June 2-6, 2008. (submitted to Sun and Geosphere, v.4, 2009).
8. Halberg F, Cornelissen G, Berk M, Dodd S, Henry M, Wetterberg L, Nolley E, Beaty L, Siegelova J, Fiser B, Wolff C, BIOCOS project. Solar signatures in Australian suicide incidence: gender differences in prominence of photic vs. nonphotic spectral components. In: Halberg F, Kenner T, Fiser B, Siege lova J (Eds.) Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, October 4-7, 2008. p. 44-62. http://web.fnusa.cz/files/kfdr2008/sbornik_2008.pdf
9. Cornelissen G, Halberg F, Babayev E. Solar wind overcomes seasons in incidence patterns of women's suicide. In preparation.
10. Davis GE, Lowell WE. Peaks of solar cycles affect the gender ratio. Medical Hypotheses 2008; 71: 829-838.
11. Halberg F, Cornelissen G, Sothern RB, Katinas GS, Schwartzkopff O, Otsuka K. Cycles tipping the scale between death and survival (= "life"). Progress of Theoretical Physics 2008; Suppl 173: 153-181.
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noninvasive methods in cardiology 2010
12. Halberg F, Cornelissen G, Katinas G, Tvildiani L, Gigolashvili M, Janashia K, TobaT, Revilla M, Regal P, Sothern RB, Wendt HW, Wang ZR, Zeman M, Jozsa R, Singh RB, Mitsutake G, Chibisov SM, Lee J, Holley D, Holte JE, Sonkowsky RP, Schwartzkopff O, Delmore P, Otsuka K, Bakken EE, Czaplicki J, International BIOCOS Group. Chronobiology's progress: season's appreciations 2004-2005. Time-, frequency-, phase-, variable-, individual-, age- and site-specific chronomics. J Applied Biomedicine 2006; 4: 1-38. http://www.zsf.jcu.cz/vyzkum/jab/4_l/halberg.pdf
13. Cornelissen G, Halberg F, Rostagno C, Otsuka K. A chronomic approach to cardiac arrhythmia and sudden cardiac death. The Autonomic Nervous System 2007; 44: 251-254.
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noninvasive methods in cardiology 2010
Circadian Rhythm of Sudden Cardiac Death (SCD) Incidence in Baku and Absheron Peninsula (16 Nov 2002 - 30 J un 2009)
Women: open diamonds, dotted curve Men: filled triangles, solid curve
04:00
08:00 12:00 16:00
Time (clock hours)
20:00
0
00:00
Figure 1
Gender Difference in Circadian Waveform* of Incidence Pattern of Sudden Cardiac Death in Baku and Absheron Peninsula (16-11-02 to 30-06-09)
40
35 -
S 30 £
o 25 -
< 20 "5 15
Q_
E 10 <
® Women (N=401) BMen (N=1786) F=0.01, P=0.99
mean + 1 SE
Test of equality of As* F=2.71, P=0.107 on residuals from 24h fit: >F=5.62. P=0.023
24-hour
Component
12-hour
Data * 12-
are hourly counts pooled over entire span, expressed as a percentage of the 24-hour mean (N=24) vs. 24-hour A ratio; ** Bingham C et al. Chronobiologia 1982; 9: 397-439.
Figure 2
49
noninvasive methods in cardiology 2010
0.07
0.06
0.05
5. 0.04
T3
~ 0.03
Q_
0.02
0.01
Sudden Cardiac Death in Baku and Absheron Peninsula (16-11-02 to 30-06-09): Women (N=401)
0.00
1.016y [0.936, 1.095]
0.0
1.0
2.0 3.0 Frequency (cycles/year)
4.0
5.0
Figure 3
Sudden Cardiac Death in Baku and Absheron Peninsula (16-11-02 to 30-06-09): Men (N=1786)
0.30 i-1-1-1-1—
0.25 -
0.0 1.0 2.0 3.0 4.0 5.0
Frequency (cycles/year)
Figure 4
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noninvasive methods in cardiology 2010
GROUNDING OR EARTHING: GLIMPSES AT PHYSIOLOGY AND PATHOLOGY
Germaine Cornelissen1, Franz Halberg1, Francis Guillaume1, Othild Schwartzkopff1, Judy Finley1, Ning Cegielski2, Paul Rosch3, Jarmila Siegelova4, Elias Ilyia2
1 University of Minnesota, Minneapolis, MN, USA;2 DiagnosTechs, Kent, WA, USA;3 American Institute of Stress, Yonkers, NY, USA;4 Masaryk University, Brno, Czech Republic
Support. GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
Aim. To assess whether "earthing" (connecting the body to the earth by grounding) affects physiology and pathology in selected volunteering investigators.
Background. Based primarily on anecdotal stories, a book on "earthing" advocates that connecting with the Earth can alleviate a number of symptoms, such as inflammation, sleep quality and energy/ vigor, presumably by neutralizing positive ions (free radicals) (1). One published study (2) reports an effect of "earthing" on circulating Cortisol from 12 subjects sampled at 4-hour intervals for 24 hours before and after sleeping on Earthing pads for up to 8 weeks, yet explicitly without detecting a statistical significance of the observation. Our re-analysis of the data by means of circadian parameter tests (3) also did not find any change in MESOR, circadian amplitude and/or acrophase (P>0.20), Figure 1. The authors' finding, however, related to a "normalization" of the circadian Cortisol rhythm (2), could be qualified by a comparison by paired t-test of inter-individual changes among circadian profiles (differences of individual time-specified values versus their corresponding timepoint means: t=3.169, P=0.025), Figure 2. "Normalization" may be no more than a regression to the mean, i.e., the observation that a variable that is extreme in a first series of measurements may be closer to the center of the distribution in follow-ups. The present investigation examined whether an effect of grounding could be documented for the individual rather than on a group basis.
Figure 1 (adapted from 2) Figure 2 Chrono-meta-analysis of (2) © Halberg
Subjects and Methods. Self-measurements of blood pressure (BP) and heart rate (HR) during waking, followed by automatic around-the-clock data at 1-hour intervals were available from JF (F, 62 years) for over one year. Effects of grounding focused on data from May 2010 when hormonal determinations in saliva (4 to 6 per day) had been obtained, including 9 days of grounding by night. For about 5 weeks, 4 other volunteering investigators automatically recorded their BP and HR around the clock at 30-minute intervals with an arm cuff (FH, M, 90 years MESOR-hypertensive when untreated but MESOR-normotensive thanks to current treatment; OS, F, 86 years; and GC, F, 60 years) or every 15 minutes during the night with a BP monitor on the wrist (FG, M, 62 years). The participants slept grounded during weeks 1, 3 and 5, unplugging the grounding sheet during weeks 2 and 4. The nightly data from FG were averaged daily. Daily data from the other 4 subjects were analyzed by cosinor (3)
51
noninvasive methods in cardiology 2010
to obtain daily estimates of the MESOR, 24-hour amplitude and acrophase. The daily endpoints were compared by Student t-test between days when each subject was or was not grounded.
Results. Table 1 summarizes results for the five investigators, each individual serving as his/her own control. No statistically significant differences in blood glucose concentration or in daily insulin requirements (P>0.15) were found for FG who has insulin-dependent diabetes mellitus. Nightly means of FG's systolic (S) BP were higher during grounding (110.6 vs. 104.9 mmHg, t=2.745, P=0.010), as were those of his pulse pressure (48.0 vs. 44.2 mmHg, t=2.716, P=0.011). By contrast, FH's pulse pressure was lower during grounding (58.1 vs. 61.6 mmHg, t=2.138, P=0.040). In the case of FH, grounding was also associated with a higher MESOR of HR (63.4 vs. 58.8 beats/min, t=4.413, P<0.001) and a larger circadian double amplitude (7.8 vs. 4.5 beats/min, t=3.136, P=0.004). In the case of GC, grounding was associated with a slight increase in body weight measured daily upon awakening (143.3 vs. 142.9 lbs, t=2.428, P=0.019) but it had no statistically significant effect on activity (P>0.10), assessed by step counts with a pedometer). Grounding was also associated with a lower MESOR of HR (72.9 vs. 76.1 beats/min, t=3.309, P=0.002) and with a decrease in the double circadian amplitude of diastolic (D) BP (17.9 vs. 21.7 mmHg, t=2.563, P=0.015), Figure 3. A similar decrease in the circadian double amplitude of DBPwas observed for OS (13.1 vs. 17.5 mmHg, t=2.143,P=0.045), Figure 4.
1-May 8-May 15-May 22-May 29-May 5-Jun 12-Jun 1-May 8-May 15-May 22-May 29-May 5-Jun 12-Jun
Time (calendar date in 2010) Time (calendar date in 2010)
Figure 3 © Halberg Figure 4 © Halberg
No effect of grounding was found on the BP and HR of JF (P>0.20). Grounding also had no statistically significant effect on JF's Cortisol (P>0.30). Grounding was associated, however, with an increased circadian amplitude of salivary testosterone (15.1 vs. 9.3 pg/ml, t=2.466, P=0.020), Figure 5, and a decrease in DHEA MESOR (4.0 vs. 4.6 ng/ml, t=2.958, P=0.006), Figure 6.
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noninvasive methods in cardiology 2010
Effect of Grounding on SalivaryTes tos te rone: JF (F, 62y)
35 30
I"
2 20
OJ
115"
3 10 -
5 -0
Grounding? -♦-Yes -o-No
Studentt = 2.466, P = 0.020
29-Apr 6-May 13-May 20-May 27-May Time (calendar date in 2010)
Effect of G rounding on Salivary DHE A: J F (F, 62y)
Student t = 2.958, P = 0.006
Grounding?
-^Yes -o-No
29-Apr 6-May 13-May 20-May 27-May 3-Jun Time (calendar date in 2010)
Figure 5 © Halberg Figure 6 © Halberg
An increase in vigor/wellness ratings of JF during grounding (72.5 vs. 60.7 AU, t=2.126, P=0.042), Figure 7, is noteworthy as JF has suffered for the past 20 years from adynamia episodes that can last 2-3 months and recurred twice yearly thus far, usually involving frequency desynchronization of her circadian system, a Vascular Variability Disorder (WD). Grounding seems to have been associated with a later onset of adynamia in the summer of 2010 and perhaps also with an episode of shorter duration, Figures 8 and 9, albeit results on the duration of the summer 2010 episode of adynamia remain uncertain at the time of this writing. Prediction intervals for the date of onset and for the duration of adynamia episodes were computed from records kept over the past 10 years. The onset of the summer 2010 episode occurred later than the upper 90% and even 95% prediction limit, and the duration was presumably less than the lower 90% (but not lower than the 95%) prediction limit, but the ending date of the episode is being debated as the recovery may have been followed by a return to adynamia.
Effect of G rounding on Vigor and Wellness: JF (F, 62y)
100 -i-
Student t = 2.126, P = 0.042
80
CD
c 40
01 20 V Grounding?
—♦—Yes -o- No
29-Apr 6-May 13-May 20-May 27-May 3-Jun Time (calendar date in 2010)
Figure 7 © Halberg
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noninvasive methods in cardiology 2010
Summer OnsetofUnwellness (JF, F, 62y in 2010)
Summer Duration of Unwellness (JF, F, 62y in 2010)
190
>-> 180
170
C 160
ro
E 150
o
i£ 140
D>
130
_1
120
Later J }
w
t90%PI
S5%pr
PI: Prediction Interval
2002 2003 2004 2005 2006 2007 2008 2009 2010 Time (calendar year)
S 60 c o
ra 40 ° 20
90% PI
95% PI
PI: Prediction Interval Shorter
2002 2003 2004 2005 2006 2007 2008 2009 2010 Time (calendar year)
Figure 8 © Halberg
Figure 9 © Halberg
Discussion and Conclusion. Whereas grounding was found to affect some BP and/or HR endpoints, the results are not consistent among the participants who differ in BP-MESOR when untreated. N-of-1 studies are complicated by the fact that a multitude of other factors may have contributed to the effects detected herein, beyond any effect of grounding. For instance, GC and FG had a head cold during this investigation, which may account in part for GC's lowered body weight in the absence of grounding. FH suffered a painful foot.
Interestingly, an observation made by the authors of the book (1) that earthing may be associated with an increase in the INR of patients treated with Coumadin was confirmed in the case of FH, Figure 10, albeit not (yet?) in that of OS (not shown). The range of variation of the INR was determined by computing 90% and 95% prediction limits based on data obtained before earthing started. An increase in the INR above the upper 95% prediction limit is found in association with earthing for FH, Figure 10. An increasing trend of borderline statistical significance (P=0.062) in the INR of FH after the initiation of earthing is also noteworthy, Figure 10.
5.0
4.0 -
3.0
2.0 -
1.0 -
0.0 H-
01/01/08
Using last 2-year span as reference
Grounding started May 4
Suggested reduction of Coumadin dose
'INR increase: r=0.995, P=0.062
PI: Prediction Interval
01/01/09 01/01/10 Time (calendar date)
01/01/11
Figure 10 ©Halberg
54
noninvasive methods in cardiology 2010
The design of this ongoing study will eventually allow the checking for consistent findings on an individual basis by examining whether differences observed within a 2- to 4-week span are reproducible over time. A placebo effect also needs to be considered and may require conducting double-blind studies.
REFERENCES
1. Ober C, Sinatra ST, Zucker M. Earthing. The most important health discovery ever? Basic Heath Publications, Inc., 260 pp. 2010.
2. Ghaly M, Teplitz D. The biologic effects of grounding the human body during sleep as measured by Cortisol levels and subjective reporting of sleep, pain and stress. J Alternative and Complementary Medicine 2004; 10: 767-776.
3. Bingham C, Arbogast B, Cornelissen Guillaume G, Lee JK, Halberg F. Inferential statistical methods for estimating and comparing cosinor parameters. Chronobiologia 1982; 9: 397-439.
55
Table 1. Sometimes opposite inter-individual variability of differences found in the presence versus absence of earthing in the
subjects investigated *
SBP-M SBP-2A DBP-M DBP-2A PP HR-M HR-2A HR-SD Glucose Insulin BW steps
FH (M, 91 y)
Grounding?
Yes (21days) 130.3 39.93 72.2 32.91 58.1 63.4 7.82 8.30
No (14 days) 133.6 38.83 72.0 29.19 61.6 58.8 4.49 6.85
Student t 1.412 0.324 0.121 1.505 2.138 4.413 3.136 1.486
P 0.167 0.748 0.905 0.142 0.040 <0.001 0.004 0.147
Deer NS NS Incr Deer Incr Incr Incr
,62y)
Grounding?
Yes (20/19days) 110.6 62.5 48.0 72.4 5.10 130.8 33.2
No (14/11 days) 104.9 60.6 44.2 72.3 4.44 141.0 30.5
Student t 2.745 1.971 2.716 0.083 1.074 1.325 0.748
P 0.010 0.057 0.011 0.934 0.291 0.196 0.461
Incr Incr Incr NS NS NS NS
OS (F, 86y)
Grounding?
Yes (11 days) 118.3 15.71 67.2 13.09 51.1 64.1 9.26 12.38
No (11 days) 122.1 21.71 69.1 17.50 52.9 62.4 10.04 11.50
Student t 1.283 1.946 1.700 2.143 0.711 1.420 0.344 0.719
P 0.214 0.066 0.105 0.045 0.485 0.171 0.734 0.481
NS Deer Deer Deer NS Incr NS NS
,60y)
Grounding?
Yes (21days) 117.9 29.12 69.4 17.90 48.6 72.9 21.98 11.22 143.3 10335
No (14 days) 118.0 32.85 69.1 21.74 48.9 76.1 21.91 11.33 142.9 10982
Student t 0.079 1.447 0.518 2.563 0.444 3.309 0.037 0.193 2.428 1.602
P 0.937 0.157 0.608 0.015 0.660 0.002 0.970 0.848 0.019 0.116
NS Deer NS Deer NS Deer NS NS Incr Deer
JF (F, 62y)
Grounding?
Yes (9 days) 113.5 32.56 63.9 17.79 49.6 62.4 14.51 8.71
No (22 days) 113.1 31.43 64.0 14.57 49.1 62.3 14.88 9.62
Student t 0.163 0.184 0.081 1.089 0.222 0.091 0.111 0.798
P 0.871 0.855 0.936 0.286 0.826 0.928 0.912 0.432
NS NS NS NS NS NS NS NS
Mood-M Mood-A Cort-M Cort-A DHEA-M DHEA-A Mel-M Mel-A Test-M Test-A Estr-M Estr-A Aldo-M Aldo-A
JF (F. 62y)
Grounding?
Yes (9 days) 72.5 3.96 5.83 4.16 3.97 1.55 40.5 55.8 39.7 15.14 15.55 5.69 54.8 16.62
No (22 days) 60.2 6.58 6.39 5.10 4.57 1.91 31.2 45.2 39.5 9.25 13.90 3.77 60.9 15.28
Studentt 2.126 1.448 0.832 0.924 2.958 1.320 1.986 1.674 0.105 2.466 1.834 1.377 1.250 0.382
P 0.042 0.158 0.412 0.363 0.006 0.197 0.057 0.105 0.917 0.020 0.077 0.179 0.221 0.705
Incr Deer NS NS Deer NS Incr Incr NS Incr Incr Incr NS NS
* SBP: Systolic Blood Pressure (mmHg); DBP: Diastolic Blood Pressure (mmHg); PP: Pulse Pressure (= SBP-M - DBP-M); HR: Heart Rate (beats/min); Glucose (mg/dl) by finger prick; Insulin (IU): daily requirement to treat IDDM; BW: Body Weight (lbs); steps (N): daily pedometer count; Mood: ratings (arbitrary units on 0-100 scale); Cort: Cortisol (uM); DHEA: Dehydroepiandrosterone (ng/ml); Mel: Melatonin (pg/ml); Test: Testosterone (pg/ml); Estr: Estradiol (pg/ml); Aldo: Aisosterone (pg/ml); all hormones determined in saliva; M: MESOR (Midline Estimating Statistic Of Rhythm, a rhythm-adjusted mean); A (or 2 A): 24-hour (or double) amplitude (half or full extent of predictable change within a day assessed by least squares fit of 24-hour cosine curve to data in 1-day intervals); Incr, Deer or NS: Earthing associated with Increase, Decrease or No (statistically Significant) effect.
noninvasive methods in cardiology 2010
AEOLIAN CHANGES AND GENDER IN THE INCIDENCE OF CARDIAC ARRESTS IN
MINNESOTA (1979-2008)
Germaine Cornelissen1, Judy Palermo2, Franz Halberg1
:Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA 2Minnesota Department of Health, St. Paul, MN, USA
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
Abstract
This paper updates earlier reports on the topic of solar wind cycles in the incidence patterns of diseases involving the heart and extends evidence concerning their aeolian nature with reference to both myocardial infarction (MI) and sudden cardiac death (SCD). It also summarizes physiological data that reflect their cosmos in some aspects of the human circulation in health. In addition to, or apart from, calendar-yearly components, blood pressure and heart rate can be characterized by a period, x, longer than a year (y) ~ the far-transyear, trans (beyond 1-y length) by several months (1.20 years [x - CI {95% confidence interval}] < [x + CI] < 1.90 years) ~ that have been distinguished from near-transyears (1.00 year < [x - CI< [x + CI] < 1.20 years). Both kinds of transyears can coexist for a while with a calendar-yearly component and, in some locations, can even transiently replace the latter.
Data base
The dates of deaths from cardiac arrest in Minnesota were obtained for the span from 1979 to 2008 (30 years). Additional information included date of birth and gender. From 1979 to 1998, cardiac arrest was diagnosed according to the ICD9 classification of diseases, whereas ICD10 was used for data collected starting in 1999. Cardiac arrest in a patient with an MI was an exclusion criterion in ICD10 while it was included under SCD in ICD9.
Time series were formed separately for males and females (ages at death spanned the range from early after birth to centenarians). Least squares spectra by cosinor (1-3) were performed for the series overall and for the shorter 10-year span of diagnoses made under the ICD 10 classification. In the latter case, the data were further subdivided according to codes 146.1 and 146.9. Chronobiologic serial sections were obtained at the trial period of I year and at periods corresponding to the spectral peak around the year for the 30-year series. Gliding spectra were obtained for both the overall 30-year series (all cardiac arrests, irrespective of gender) and for the last 10-year series (ICD 10146.1 and 146.9, irrespective of gender). Over 30 years, there were 11,302 deaths from cardiac arrest in Minnesota, equally distributed between males (N=5,905) and females (N=5,397). From 1979 to 1988, there was an increase in mortality from cardiac arrest, followed by an abrupt decline in 1989. From 1990 to 1996, the average daily incidence of cardiac arrests remained stable. It was also stable from 1999 to 2008, albeit slightly less than during the previous decade.
In view of the large trends in mortality, the least squares spectra had inflated low-frequency amplitudes. Overall, a spectral peak is centered on the year. An additional smaller peak is observed at a period of about 1.35 or 1.05 years for females and males, respectively. Least squares spectra of the last 10 years (ICD 10) show multiple peaklets that are not consistent between males and females, except for a weak about 0.32-year component. Least squares spectra of consecutive 5-year spans corroborated the earlier detection of a transyear with a period of about 1.4 years (4), contributed primarily by females, males having a peak
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noninvasive methods in cardiology 2010
around 1.04 years during the 1999-2003 span analyzed earlier. A cis-half-year is also corroborated for this particular 5-year span. The corresponding spectra for 2004-2008 are markedly different. Because earlier analyses were restricted to the incidence of sudden cardiac deaths (ICD 10 146.1), the cardiac arrests from 1999 to 2008 were further analyzed specifically for 146.1 and 146.9. Again, the about-1.4-year transyear observed earlier is contributed primarily by females and is not reproduced during the next 5 years when a calendar year component is prominent, albeit contributed by females. The about 1.4-year transyear detected during 1999-2003 for females characterizes both deaths classified as 146.1 or 146.9.
Chronobiologic serial sections at a trial period of 1.00 year reveal a relatively stable acrophase in winter, as anticipated. This is the case overall as well as for females or males considered separately. In the case of females, a disruption in the acrophase sequence is observed shortly after the transition from ICD9 to ICD10, during which span the yearly component cannot be detected with statistical significance. Thereafter, the acrophase seems to undergo a slight drift indicative of a period longer than 1 year, but it only reaches statistical significance at the end of the record when the acrophase seems to have stabilized, albeit around a slightly later time as compared to the timing at the beginning of the record. A similar situation applies to the results of males, but the disruption in the acrophase sequence occurs earlier, toward the middle of the record, and the acrophase drift during the last 10 years is more readily apparent. A trend toward stabilization of the acrophase at a slightly later time as compared to that observed at the beginning of the record is also observed in this case. Chronobiologic serial sections at periods of 1.15 years, 1.05 years, or 1.02 years, periods corresponding to spectral peaks for females, males, and overall incidence (irrespective of gender), show a relatively stable acrophase sequence during the last 10 years when the ICD 10 classification was used for both males and females. In the case of females, such a stable acrophase sequence is also observed during other earlier spans when the acrophase can assume a similar or a different value. No consistent drift in acrophase is seen. In the case of males, a drift in acrophase suggesting the presence of a component with a period shorter than the one used for analysis is seen during the first half of the record (before the disruption in acrophase sequence also observed when using 1 year as trial period). The fact that a period of 1.05 years was considered for males, closer to 1 year than the 1.15-year trial period used for females, may account for the visual acrophase drift seen for males but not for females. In the overall analysis, the drift in acrophase is milder as the trial period is even closer to 1 year. It also lasts longer, practically until the switch from ICD9 to ICD 10. A reversal from a shorter-than-1 year to a longer-than-1 year seems to occur in association with the ICD9 to ICD 10 switch.
Gliding spectra, Figure 2, corroborate the above impressions. A relatively strong yearly component is weakened already once the daily incidence of cardiac arrests starts declining, probably because the amplitude diminishes in keeping with the decreased average daily incidence. Of particular interest is the observation that a transyear is present intermittently, even before the institution of ICD 10. The same applies to cis-half-years that are particularly prominent during the first few years of the record. The transient presence of a transyear as well as of cis-half-years during the last 10 years is readily apparent, as is the more consistent detection of a circannual component. Whether the about 0.3-year component also detected during most of the last 10 years is an independent signal or the third harmonic of the year contributing to the circannual waveform remains to be elucidated. The bracketed section of Figure 3 shows the broad range of periods found in individual time series covering years or decades as well as some wide uncertainty estimates (CIs). This spread led to the very broad definition of the range of far-transyears (4-6) based on a similar span also encountered in the geographic variation of Table 1 (7; cf. 11), also reflected in Figure 4. While the proposition of transyears has been confirmed in other variables in our laboratory and elsewhere (8-11), their aeolian nature must be emphasized.
58
noninvasive methods in cardiology 2010
Conclusion
A number of pathological and physiological cycles drift in period and wax and wane in amplitude to the point of bifurcation, disappearance (or drawning in noise) and reappearing and requiring a global analysis of the series as a whole and in local analyses, the latter here initiated for SCD and MI as a follow-up on an earlier investigation (4, 12; cf. 5-11).
1. Halberg F. Chronobiology: methodological problems. Acta med rom 1980; 18: 399-440.
2. Cornélissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T, editors. Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
3. Refinetti R, Cornélissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692.
4. Halberg F, Cornélissen G, Katinas G, Tvildiani L, Gigolashvili M, Janashia K, Toba T, Revilla M, Regal P, Sothern RB, Wendt HW, Wang ZR, Zeman M, Jozsa R, Singh RB, Mitsutake G, Chibisov SM, Lee J, Holley D, Holte JE, Sonkowsky RP, Schwartzkopff O, Delmore P, Otsuka K, Bakken EE, Czaplicki J, International BIOCOS Group. Chronobiology's progress: season's appreciations 2004-2005. Time-, frequency-, phase-, variable-, individual-, age- and site-specific chronomics. J Applied Biomedicine 2006; 4: 1-38. http://www.zsf.jcu.cz/vyzkum/jab/4_l/halberg.pdf.
5. Cornélissen G, Masalov A, Halberg F, Richardson JD, Katinas GS, Sothern RB, Watanabe Y, Syutkina EV, Wendt HW, Bakken EE, Romanov Y. Multiple resonances among time structures, chronomes, around and in us. Is an about 1.3-year periodicity in solar wind built into the human cardiovascular chronome? Human Physiology 2004; 30 (2): 86-92.
6. Cornélissen G, Halberg F, Rostagno C, Otsuka K. A chronomic approach to cardiac arrhythmia and sudden cardiac death. The Autonomic Nervous System 2007; 44: 251-254.
7. Halberg F, Cornélissen G, Otsuka K, Fiser B, Mitsutake G, Wendt HW, Johnson P, Gigolashvili M, Breus T, Sonkowsky R, Chibisov SM, Katinas G, Siegelova J, Dusek J, Singh RB, Berri BL, Schwartzkopff O. Incidence of sudden cardiac death, myocardial infarction and far- and near-transyears. Biomedicine & Pharmacotherapy 2005; 59 (Suppl 1): S239-S261.
8. Mikulecky M, Florida PL. Daily birth numbers in Davao, Philippines, 1993-2003: Halberg's transyear stronger than year. Abstract, 26th Seminar, Man in His Terrestrial and Cosmic Environment, Upice, Czech Republic, May 17-19, 2005.
9. Mikulecky M. Reanalyza natality v jizni brazilii ~ opet dominuje Halbergova parasezonalita: International Conference on the Frontiers of Biomedical Science: Chronobiology, Chengdu, China, September 24-26, 2006, p. 188-193.
10. Kovac M, Mikulecky M. Time sequence of epileptic attacks from the point of view of possible lunisolar connections. International Conference on the Frontiers of Biomedical Science: Chronobiology, Chengdu, China, September 24-26, 2006, p. 175-179.
11. Kovac M, Mikulecky M. Secular rhythms and Halberg's paraseasonality in the time occurrence of cerebral stroke. Bratisl Lek Listy 2005; 106 (2): 423-427.
12. Halberg F, Breus TK, Cornélissen G, Bingham C, Hillman DC, Rigatuso J, Delmore P, Bakken E, International Womb-to-Tomb Chronome Initiative Group: Chronobiology in space. Keynote, 37th Ann. Mtg. Japan Soc. for Aerospace and Environmental Medicine, Nagoya, Japan, November 8-9, 1991. University of Minnesota/Medtronic Chronobiology Seminar Series, #1, December 1991, 21 pp. of text, 70 figures.
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noninvasive methods in cardiology 2010
Table 1: Geomagnetic/geographic differences among cycles with periods in the range of 0.8-2.0 years, characterizing the incidence of sudden cardiac death (SCD)1* and myocardial infarction (MI)
Sudden Cardiac Death (SCD)1
Site Span T, At, N SCD (N) Period (y) (95% CI) Amplitude (95% CI) A(% MESOR) P-value2
.....Transyear (TY) or Candidate Transyear (cTY) Detected.....
Minnesota 1999-2003 5y, 1d, 1826 343 1392 (TY) (1.173,1.611) 0.042 (0.00, 0.09) 22.0 0.014
Arkansas 1999-2003 5y, 1d, 1826 273 1.095 (0.939, 1.251) 0.032 (0.00, 0.07) 21.1 0.040
1686 (cTY) (1.293, 2.071) 0.031 (0.00, 0.07) 20.7 0.044
Czech Rep. 1999-2003 5y, 1d, 1826 1006 0.974 (0.856, 1.091) 0.078 (0.00, 0.16) 14.2 0.007
1759 (cTY) (1.408, 2.110) 0.077 (0.00,0.15) 13.9 0.01
1994-2003 10y, 1d, 3652 1792 1.726 (TY) (1.605,1.848) 0.074 (0.02,0.13) 15.1 <0.001
1 (0.944, 1.056) 0.052 (0.00,0.10) 10.6 0.01
.....Candidate Transyear Not Detected.....
North Carolina 1999-2003 5y, 1d, 1826 752 0.929 (0.834, 1.023) 0.069 (0.00, 0.14) 16.9 0.007
Tbilisi, Georgia Nov 99-2003 4.1y, 1d, 1505 130 0.988 (0.862, 1.114) 0.035 (0.00, 0.07) 40.7 0.007
Hong Kong 2001-2003 3y, 1 m, 36 52 0.843 (0.651, 1.036) (NS) 44.9 0.077
Myocardial Infarction (Ml)
Site Span T, At, N Ml (N) Period (y) (95% CI) Amplitude (95% CI) A(% MESOR) P-value2
.....Coexisting Year (Circannual) and Transyear (TY).....
Czech Rep. 1999-2003 5y, 1d, 1826 52598 1.014 (0.989, 1.038) 2.85 (2.22, 3.48) 9.88 <0.001
1.354 (TY) (1.252,1.456) 1.35 (0.69,2.02) 4.68 <0.001
1994-2003 10y, 1d, 3652 115520 0.998 (0.988, 1.009) 3.03 (2.47, 3.60) 9.58 <0.001
1.453 (TY) (1.417,1.489) 1.91 (1.34,2.49) 6.04 <0.001
115 (TY) (1.116,1.184) 1.23 (0.64,1.82) 3.88 <0.001
Minnesota 1968-1996 29y, 1d, 10593 129205 1.049 (1.035, 1.062) 0.30 (0.11,0.49) 2.46 <0.001
1.232 (1.207, 1.258) 0.18(0.02,0.35) 1.48 0.013
1.001 (0.998, 1.004) 1.04 (0.89,1.20) 8.53 <0.001
*With focus on transyears, with periods longer than 1.0 year (underlined; double underline for neartransyear). international Classification of Diseases (ICD10), Code 146.1, excluding Ml and sudden death of unknown or unspecified cause (except before 1999).
2From linear least-squares analyses, not corrected for multiple testing. Amplitude expressed in N/day. From Halberg F, Cornelissen G, Otsuka K, Fiser B, Mitsutake G, Wendt HW, Johnson P, Gigolashvili M, Breus T, Sonkowsky R, ChibisovSM, Katinas G, Siegelova J, Dusek J, Singh RB, Berri BL, Schwartzkopff O. Incidence of sudden cardiac death, myocardial infarction and far- and near-transyears. Biomedicine & Pharmacotherapy 2005; 59 (Suppl 1): S239-S261.
60
noninvasive methods in cardiology 2010
Pllf*3 Ol 1BÉF
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Figure 1. Cardiac arrest before and after a change in the International Classification of Diseases (ICD), indicated by a vertical line in females (top), males (middle) and a pool of both genders (bottom). © Halberg.
61
noninvasive methods in cardiology 2010
Figure 2. Gliding spectral windows in the range of periods from 0.25 years (y) to 4 y of cardiac arrest in Minnesota. © Halberg.
Tha Trans-year (an -1.3-yft»r component) In Ihe Cosmos Honor™*], Pathology (myocardial infarction, Ml), and Physiology (bottom n ruwnj*
1 0
10
1 1
1 2
Period (y&ara)
1.3
i .1
>
1.5 Physical
Vil-lilhlC!.!
16
20
Z 30
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Point and 9S"S confidence interval (CI)
" All di1fvrii>fl *>y rto-n-flwortappiiiB 9fi* cl1 ,rann 1h,e preenso calendar yvar and rmny lllrtartnfl **n010 #0*ti ottiar, ■ pubillvt hklt (if *rt*5fl*nk'tV, i,Hr,gt1; Ipnid For anclhor man rJrPYi*ng 3 addflidAl Mnfrd.
Figure 3. Transyears found in physics, in the incidence pattern of myocardial infarctions (MI), and in each physiological time series examined thus far. Note that broad 95 % confidence intervals of the period extend to shorter than 1.2-y estimates, violating this lower limit of a far-transyear. Hence, we refer to transyears in these cases, rather than coining another term. All limits remain tentative. © Halberg.
62
noninvasive methods in cardiology 2010
CB^,___J*^__^_________Jfr___-€
Geographic and time-varying differences in the spectrum of sudden cardiac death*
Figure 4. Geographic differences in the presence (and prominence) of a far-transyear (T) vs. that of a calendar year (Y) component during the span investigated. For the incidence in bracketing data, see Figure 2. Table 1 cannot be generalized. © Halberg.
63
noninvasive methods in cardiology 2010
FEASIBLE AMBULATORY BLOOD PRESSURE AND HEART RATE MONITORING IN AMERICAN SECONDARY SCHOOLS TO ASSESS CHRONOMES IN CLINICALLY
HEALTHY ADOLESCENTS
William Huynh1, Germaine Cornélissen1, Richie Huynh1, Ryan Huynh1, Franz Halberg1
1 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
Aims. To demonstrate the feasibility of prolonged monitoring of blood pressure (BP) and heart rate (HR) in high school students and to illustrate how it can address some interesting physiological questions while also providing reference values for the time structure of BP and HR at an important stage of life.
Background. Teaching how to measure BP and HR in secondary education (1 -4) has a long history in the context of chronobiology education (1 -7). Before ambulatory monitors became available, students had to be taught how to listen to Korotkoff sounds to measure systolic (S) and diastolic (D) BP and how to take their pulse. Despite great limitations related to this approach, notably in young children, these early school proj ects were first to reveal a difference in the circadian amplitude between students with a positive versus negative family history of high BP and related cardiovascular problems (8-11). BP and HR monitoring in schools, even with ambulatory monitors, as a rule has been limited to 24 or at most 48 hours (8). The data collected around-the-clock for up to 5 weeks from 14 adolescents in this award-winning school project (12) are reanalyzed herein to assess the time structure (chronome) of BP and HR.
Subjects and Methods. As part of a secondary school project focusing on effects of exercise on BP and HR (12), 14 clinically healthy adolescents measured their BP and HR around-the-clock at 30-minute intervals for up to 5 weeks, with few and short interruptions. They used the TM-2421 ambulatory monitor from A&D (Tokyo, Japan). The students (7 girls and 7 boys) were between 15 and 17 years of age. The data were edited prior to analysis to remove obvious outliers and bad data. Criteria for data editing were values for the pulse pressure (SBP- DBP) less than 10 or greater than 100 mmHg. Least squares spectra (13-15) were computed for each edited data series in the frequency range of one cycle in 35 days (5 weeks) and three cycles per day. Amplitudes at each trial period were averaged over the 14 students to obtain an average least squares spectrum for each variable. Population-mean cosinor spectra (13-15) were also computed to test the zero-amplitude (no rhythm) assumption of anticipated components with periods of 24, 12 and 8 hours (circadian rhythm and harmonic terms) and of 168 and 84 hours (week and half-week components). Their amplitudes and the MESOR were compared between boys and girls by means of the two-tailed Student t-test assuming equal variances.
Results. Twelve of the 14 students mostly completed the scheduled monitoring. Since shorter records might yield spuriously elevated amplitudes of the low-frequency components, average least squares spectra were computed on the basis of these 12 students only, Figure 1. The average amplitude with its standard error (SE) is shown for each trial period (between 5 weeks and 8 hours). The two major spectral peaks have periods of 24 and 12 hours, as expected since the circadian system is usually very prominent and ubiquitous. As the circadian variation of BP and HR is not necessarily sinusoidal, being characterized by a steeper fall of shorter-than 12 hours duration during the night, a relatively sharp rise in the morning and a slower decrease in the evening hours, it is likely that the 12-hour peak reflects the second harmonic of the circadian rhythm, accounting for the non-sinusoidal waveform.
64
NONINVASIVE METHODS IN CARDIOLOGY 2010
The 24-hour and 12-hour components are invariably statistically significant by population-mean cosinor (P<0.001) for all three variables. In addition, the 7-day and 3.5-day components of HR are also statistically significant (P<0.05), as are harmonic terms of the circadian variation with periods of 6.0 and 4.8 hours, Figure 2.
Population-mean CosinorSpectrum: Heart Rate
0.0 1.0 2.0 3.0 4.0 5.0 6.0 7.0 8.0
Frequency (cycles/day)
Figure 2. Population-mean cosinor of HR. In addition to the prominent 24-hour and 12-hour components, statistically significant harmonics of 6.0 and 4.8 hours also contribute to the circadian waveform of HR, and the week and half-week components are detected with statistical significance.
On an individual basis, the circadian component is invariably statistically significant for all three variables (P<0.001). The second harmonic with a period of 12 hours is also invariable statistically significant for DBP, and it is statistically significant in 13 of the 14 students for SBP and HR, while reaching borderline statistical significance (P<0.10) for the other student in the case of SBP. In the case of SBP, the circaseptan component reaches statistical significance for 2 girls and 5 boys, and borderline statistical significance for 3 girls and 1 boy. The half-week is statistically significant for 5 girls and 3 boys and reaches borderline statistical significance for 2 boys. In the case of DBP, the circaseptan component is statistically significant for 3 girls and 3 boys and reaches borderline statistical significance for 1 girl and 1 boy. The circasemiseptan component is detected with statistical significance for 3 girls and 4 boys and with borderline statistical significance for 1 girl and 1 boy. In the case of HR, statistical significance of the circaseptan component is reached for 4 girls and 5 boys and that of the circasemiseptan component for 6 of the 7 boys but for none of the girls. As seen from Table 1, boys have a slightly higher MESOR of SBP as compared to girls (P=0.086)„ in keeping with earlier studies. The two genders do not differ in terms of their circadian or circaseptan systems of SBP, however (P>0.20). No gender difference is found for the MESOR of DBP or for the double amplitudes of components with a period of 7 days, 3.5 days or 24 hours in the spectrum of this variable, but boys show a larger double amplitude of the 12-hour component than girls (P=0.030), Table 1. As expected, girls have a higher MESOR of HR than boys (P=0.035). Whereas the two genders do not differ in terms of their circadian system of HR, boys are found to have a more prominent half-weekly component than girls (P=0.005), Table 1.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Table 1
Systolic Blood Pressure Diastolic Blood Pressure Heart Rate
Girls MESOR 168h-2A 84h-2A 24h-2A 12h-2A MESOR 168h-2A 84h-2A 24h-2A 12h-2A MESOR 168h-2A 84h-2A 24h-2A 12h-2A
02_ 110.8 5.38 19.67 27.65 12.35 66.9 1.89 14.03 21.87 8.73 77.2 3.77 3.28 11.05 3.79
05_ 118.4 14.00 9.99 36.67 22.19 68.8 2.69 1.13 14.61 7.69 79.0 11.84 4.24 28.79 12.27
07_ 111.2 0.29 1.45 27.95 3.28 64.8 2.79 2.19 22.07 5.37 73.7 1.57 1.61 9.97 3.22
08_ 113.4 9.32 0.68 13.56 7.56 60.9 7.73 1.45 14.84 7.82 73.5 2.04 1.97 10.55 5.55
10_ 114.2 1.92 3.02 12.86 8.30 61.1 0.54 3.04 10.57 6.71 73.6 2.41 1.78 9.90 5.24
11_ 121.0 3.47 3.91 18.02 9.72 66.9 4.70 2.59 19.92 9.44 73.3 6.34 1.21 10.13 4.25
14__109.9 1.16 3.16 25.41 9.10 64.0 2.16 2.64 18.11 8.69 74.4 2.83 0.73 11.19 5.86
Mean 114.1 5.08 5.98 23.16 10.36 64.8 3.21 3.87 17.43 7.78 75.0 4.40 2.12 13.08 5.74
_SE_1.7 2.03 2.75 3.56 2.40 1.2 0.96 1.85 1.74 0.56 0.9 1.49 0.50 2.84 1.24
Boys
01_ 120.7 4.38 9.68 20.43 7.27 71.9 2.71 7.20 17.62 9.28 77.1 2.06 6.42 15.22 5.93
04_ 119.4 2.12 0.52 9.94 3.86 67.1 0.49 1.52 13.06 8.19 70.3 3.78 1.95 18.94 7.22
06_ 108.5 3.68 2.65 20.47 11.09 59.2 2.12 1.89 16.22 11.93 72.3 5.60 3.72 20.64 10.57
09_ 118.5 9.34 7.04 29.53 12.88 62.1 8.00 7.79 19.67 11.75 70.8 9.15 5.26 18.40 9.86
12_ 116.2 4.05 2.35 10.98 8.40 65.3 4.70 3.05 11.06 8.55 72.1 3.45 4.18 10.94 6.83
13_ 127.1 6.99 2.92 21.95 12.55 72.2 4.67 3.25 13.57 10.87 71.3 4.00 5.31 21.64 7.88
15__135.4 4.46 2.21 14.41 5.50 66.6 2.47 1.27 14.34 8.06 70.7 1.56 5.09 8.43 7.95
Mean 120.8 5.00 3.91 18.25 8.79 66.4 3.59 3.71 15.08 9.81 72.1 4.23 4.56 16.32 8.03
SE_3.5 0.98 1.32 2.82 1.43 1.9 1.00 1.10 1.20 0.69 0.9 1.04 0.59 2.05 0.67
Student t -1.871 0.036 0.734 1.169 0.604 -0.745 -0.298 0.078 1.198 -2.468 2.376 0.102 -3.422 -0.999 -1.758
P 0.086 0.972 0.477 0.265 0.557 0.471 0.771 0.939 0.254 0.030 0.035 0.920 0.005 0.338 0.104
MESOR: Midline Estimating Statistic Of Rhythm; 2A: double amplitude, a measure of the extent of predictable change within one cycle. SE: standard Error. Systolic and Diastolic MESORs and 2As in mmHg, Heart Rate MESOR and 2As in beats/min.
Discussion and Conclusion. This study clearly demonstrates the feasibility of ambulatory monitoring of BP and HR in adolescents as part of a school project, not only for just a day or two but for a prolonged span of up to 5 weeks. It shows that students can be motivated to learn about themselves while also having an opportunity to experience first-hand how their physiology is affected by a variety of factors such as exercise, the original topic of the project (12, 16). The data thereby collected are amenable to checking for a number of physiological results, such as important gender differences documented herein. They also provide a valuable reference standard in the light of which future monitoring can be interpreted for an individual assessment of change. Such an assessment was obtained by sphygmochron (17) for consecutive weeks of monitoring for all study participants. This analysis compares each subject's circadian (parametric and non-parametric) endpoints with time-specified reference values that are qualified by gender and age, by contrast with current practice that relies on the same threshold for all adults 18 years and older. The results herein clearly indicate the need to account for the prominent circadian variation and for gender differences in interpreting BP and HR data, even though the age range of the participants did not allow for an examination of changes as a function of age.
REFERENCES
1. Ahlgren A, Halberg F. Cycles of Nature: An Introduction to Biological Rhythms. Washington, DC: National Science Teachers Association; 1990. 87 pp.
2. Halberg F, Haus E, Ahlgren A, Halberg E, Strobel H, Angellar A, Kühl JFW Lucas R, Gedgaudas E, Leong J. Blood pressure self-measurement for computer-monitored health assessment and the teaching of chronobiology in high schools. In: Scheving LE, Halberg F, Pauly JE eds. Chronobiology, Proc. Int. Soc. for the Study of Biological Rhythms, Little Rock, Ark. Stuttgart: Georg Thieme Publishers/Tokyo: Igaku Shoin Ltd.; 1974. p. 372-378.
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3. Scheving LA, Scheving LE, Halberg E Establishing reference standards by autorhythmometry in high school for subsequent evaluation of health status. In: Scheving LE, Halberg F, Pauly JE eds. Chronobiology, Proc. Int. Soc. for the Study of Biological Rhythms, Little Rock, Ark. Stuttgart: Georg Thieme Publishers/Tokyo: Igaku Shoin Ltd.; 1974. p. 386-393.
4. Reeker F. Autorhythmometry, anxiety and the delabeling process. In: Scheving LE, Halberg F, Pauly JE eds. Chronobiology, Proc. Int. Soc. for the Study of Biological Rhythms, Little Rock, Ark. Stuttgart: Georg Thieme Publishers/Tokyo: Igaku Shoin Ltd.; 1974. p. 394-398.
5. Stroebel CF. Autorhythmometry methods for longitudinal evaluation of daily life events and mood: psychophysiologic chronotography. In: Scheving LE, Halberg F, Pauly JE eds. Chronobiology, Proc. Int. Soc. for the Study of Biological Rhythms, Little Rock, Ark. Stuttgart: Georg Thieme Publishers/Tokyo: Igaku Shoin Ltd.; 1974. p. 379-385.
6. Halberg F, Halberg J, Halberg Francine, Halberg E. Reading, ,riting, ,rithmetic—and rhythms: a new „relevant" „R" in the educative process. Perspect Biol Med 1973; 17: 128-141.
7. Halberg F, Smith HN, Cornelissen G, Delmore P, Schwartzkopff O, International BIOCOS Group. Hurdles to asepsis, universal literacy, and chronobiology—all to be overcome. Neuroendocrinol Lett 2000; 21: 145-160.
8. Halberg F, Cornelissen G, Carandente A, Bakken E, Young E. Chronobiologic perspectives of international health care reform for the future of children. Chronobiologia 1993; 20: 269-275.
9. Halberg F, Cornelissen G, Bingham C, Tarquini B, Mainardi G, Cagnoni M, Panero C, Scarpelli P, Romano S, März W, Hellbrügge T, Shinoda M, Kawabata Y. Neonatal monitoring to assess risk for hypertension. Postgrad Med 1986; 79: 44-46.
10. Syutkina EV, Cornelissen G, Halberg F, Johnson D, Grigoriev AE, Mitish MD, Turti T, Abramian AS, Yatsyk GV, Syutkin V, Tarquini B, Mainardi G, Breus T, Pimenov K, Wendt HW. Could the blood pressure of newborns track the solar cycle? Abstract, 4° Convegno Nazionale, Societä Italiana di Cronobiologia, Gubbio (Perugia), Italy, June 1-2, 1996. p. 62-63.
11. Halberg F, Cornelissen G, Halberg E, Halberg J, Delmore P, Shinoda M, Bakken E. Chronobiology of human blood pressure. Medtronic Continuing Medical Education Seminars, 4th ed. Minneapolis: Medtronic Inc.; 1988. 242 pp.
12. Huynh Ryan, Huynh Richie. Orcadian stage-dependent effects of exercising on the time structure of blood pressure. Fourth place award, Intel Science and Engineering Fair, Phoenix, AZ, 13 May 2005.
13. Halberg F. Chronobiology: methodological problems. Acta med rom 1980; 18: 399-440.
14. Cornelissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T, editors. Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
15. Refinetti R, Cornelissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692.
16. Huynh Richie, Huynh Ryan, Cornelissen G, Huynh W, Borer K, Halberg F. Circadian timing of exercise or flying blind figuratively? J Applied Biomedicine, submitted.
17. Cornelissen G, Halberg F, Bakken EE, Singh RB, Otsuka K, Tomlinson B, Delcourt A, Toussaint G, Bathina S, Schwartzkopff O, Wang ZR, Tarquini R, Perfetto F, Pantaleoni GC, Jozsa R, Delmore PA, Nolley E. 100 or 30 years after Janeway or Bartter, Healthwatch helps avoid "flying blind". Biomedicine & Pharmacotherapy 2004; 58 (Suppl 1): S69-S86.
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THE MOON'S IMAGE IN PROLONGED HUMAN ISOLATION
Germaine Cornelissen1, Franz Halberg1, Jarmila Siegelova2, Andrea Galvagno3
1 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN 55455, USA; 2 Masaryk University, Brno, Czech Republic;3 Underlab Project, Ancona, Italy.
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
Abstract: An alternative hypothesis to the usual assumption of mere circadian desynchronization merits consideration in interpreting data collected during isolation from society, whether in buildings at or near the earth's surface or in caves underground (1,2). Around-the-clock blood pressure (BP) and heart rate (HR) data collected during 267 days of isolation in a special habitat (like Lunar Base) known as Underlab in the Frasassi caves near Ancona, Italy, by a 28-year old woman show a stable and robust about 24.8-hour "lunar" component with a residual weaker near 24.0-hour synchronized cycle. Before as well as after isolation, only a strong 24.0-hour synchronized circadian rhythm is detected. Aim: To assess the time structure of BP and HR in a clinically healthy woman under conditions of prolonged isolation, with focus on the circadian system and a possible lunar pull. Background: Circadian was coined to account for a partly endogenous circadian system, when the period was found to differ slightly but statistically significantly from 24 hours in the absence of environmental synchronizers such as the alternation of light and darkness (3). The "circa" in "circadian" also implies that there is an inherent uncertainty in the determination of the period, due to measurement errors and primarily to the finite duration of the span during which a given variable is observed, not accounting for the added possibility that the period itself may not necessarily remain constant over time (1). The demonstration of free-running in the experimental laboratory relied on telemetry over prolonged spans on large numbers of animals. Lessons learned therefrom included a measure of the extent of inter-individual variability in the free-running period as well as inter-species differences in the average free-running period. In rats kept in continuous light of low intensity, the desynchronized circadian period of core temperature telemetered from ambulatory sham-operated animals averaged 24.8 hours, close to the lunar period (4). By contrast, the average period of animals after bilateral lesioning of the suprachiasmatic nuclei was close to 24 hours, albeit with a much larger inter-individual variation in period length. Unilaterally-lesioned animals, like sham-operated rats, also had an average period close to 24.8 hours (4). Human studies conducted in caves and in bunkers, while also documenting circadian desynchronization in the absence of major environmental clues, had to rely at first on self-measurements rather than automatic monitoring. Many studies in isolation also tended to be of shorter duration. Against this background, we analyze the about 1-year record of BP and HR measured automatically around-the-clock by a clinically healthy woman who spent 267 days in isolation. Subject and Methods: K is a 28-year old clinically healthy woman. She used an ambulatory monitor (ABPM-630) from Colin Medical Instruments (Komaki, Japan) to automatically measure systolic (S), mean arterial (MA) and diastolic (D) BP and HR, mostly at 20-min intervals around-the-clock with few interruptions. She spent 267 days in the isolation of a laboratory near Ancona, Italy, from 26 July 1994 to 20 April 1995. Monitoring started 24 days prior to isolation and proceeded for another 69 days after completion of the isolation span. The original analysis of these data had revealed the presence of a circadian period longer than 24 hours but slightly shorter than 24.9 hours by chronobiologic serial sections. The circasemiseptan component (half-week) of heart rate was also found to be congruent with that of the geomagnetic disturbance index Kp (5).
The recent finding of desynchronized circadian rhythms assuming a period close to 24.8 hours discussed elsewhere in this volume prompted a re-analysis of these data to determine whether the free-
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running rhythm of K also was close to the lunar period of 24.8 hours. The data were averaged over consecutive 3-hour intervals for association with environmental variables (local K, Kp, and cosmic rays) and analyzed by least squares spectra, separately before, during ad after isolation. The data collected during the first week of isolation were omitted to reduce any artifacts related to the transition from society to isolation. Spectra were computed in the frequency range from one cycle in 24, 252, or 69 days (before, during and after isolation, respectively) to slightly more than two cycles per day. The periods of components corresponding to spectral peaks were further assessed by nonlinear least squares according to Marquardt's algorithm (6). In order to examine whether the desynchronized circadian period varied with time, nonlinear analyses were also carried out in 8-week intervals displaced by 1 week during the isolation span, using a two-component model consisting of cosine curves with initial periods of 24.8 and 24.0 hours.
Time (calendar da1
Time (calendar da1
Figure 1. Time plots of systolic blood pressure, mean arterial pressure, diastolic blood pressure and heart rate of K (F, 28y) before, during and after isolation.
24.0 hours -> Before Isolation
(24 days)
12.0 hours—■
o -I-1-1-1-1-1-1-1-1-1--
0.0 1.0 2.0
Frequency (cycles/day)
0.0 1.0 2.0
Frequency (cycles/day)
Figure 2. Least squares spectra of systolic blood pressure before and after isolation reveal the prominence of a 24.0-hour synchronized component as well as the presence of its second harmonic.
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Results: The 3-hourly mean data for SBP, MAP, DBP and HR are plotted as a function of time in Figure 1. Except for an overall decrease in HR during isolation, the naked eye cannot discern the underlying time structure of these variables.
As expected, least squares spectra before and after isolation indicate the prominence of a 24-hour synchronized circadian component, as illustrated in Figure 2 for SBP. By contrast, during isolation the major spectral peak corresponds to a period of about 24.8 hours, as shown in Figure 3 for SBP. Amuch smaller spectral peak is also observed at 24.0 hours. Another spectral peak corresponding to a period of 12.32 hours is validated nonlinearly for BP but not for HR. Its period has a narrow 95% confidence interval (CI) extending from 12.31 to 12.33 hours.
E 2 -
1 I
24.8 hours-
During Isolation (252 days) -24.0 hours
12.0 hours-»
12.32 hours
0.0
1.0
Frequency (cycles/day)
2.0
Figure 3. Least squares spectrum of systolic blood pressure during isolation (omitting data collected during the first week of isolation) reveal an about 24.8-hour component.
A model consisting of two cosine curves with trial periods of 24.8 and 24.0 hours was fitted nonlinearly to each variable during isolation. As seen from Table 1, both components are detected with statistical significance as the CIs of their respective amplitudes do not overlap zero, with the exception of the 24.0-hour component of DBP. The nonlinearly estimated period is invariably 24.80 hours for BP and 24.82 hours for HR, its 95% CI covering 24.8 hours. The period of the second component is invariably close to 24.0 hours, albeit the 95% CI does not cover 24.0 hours for SBP and MAP, Table 1.
Table 1 SBP MAP DBP HR
M 103.4 77.9 59.5 70.90
95% CI [102.7 | 104.1] [77.23 | 78.60] [58.9 | 60.1] [70.0
24.8h 24.80 24.80 24.80 24.82
95% CI [24.77 | 24.821 [24.77 | 24.821 [24.77 | 24.821 [24.8 | :
A1 2.45 2.42 2.02 3.05
95% CI [1.44 | 3.45] [1.45 | 3.39] [1.18 | 2.85] [1.79
24. Oh 23.93 23.92 24.01 23.96
95% CI [23.88 | 23.98] [23.88 | 23.97] [23.94 | 24.09] [23.92 | :
A2 1.13 1.08 0.58 1.51
95% CI [0.13 2.121 [0.11 2.041 [-0.26 11.411 [.25
1
This global two-component model remains applicable throughout most of the isolation span, as seen from local nonlinear analyses carried out over an 8-week interval progressively displaced by
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1 week. The desynchronized circadian component assumes a period close to 24.8 hours most of the time, except for the first interval that may still be influenced by the transition from society. The 95% CI that does not cover 24.0 hours, as illustrated in Figure 4A for SBP. Similar results are obtained for MAP, DBP and HR (not shown). Despite the much shorter (8-week) spans, the 24.8-hour component is detected with statistical significance most of the time, as seen from the non-overlap of zero by the 95% CI of the about 24.8-hour amplitude, shown in Figure 4B for SBP.
Nonlinear Estimate of the "Lunar" Period: SBP
25.8
20-Oct-94 8-Dec-94 26-Jan-95
Time (calendar date)
16-Mar-95
Figure 4A. The desynchronized circadian period of SBP remains close to 24.8 hours throughout isolation, its 95% confidence interval not covering 24.0 hours.
Nonlinear Estimate of the "Lunar" Amplitude: SBP
Figure 4B. Time course of the about 24.8-hour amplitude of systolic blood pressure, assessed nonlinearly, indicates the statistical significance of this component most of the time during isolation. Similar results are obtained for the three other variables (not shown).
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Whereas the about 24.0-hour component also has a relatively stable period that remains close to 24.0 hours during isolation, as seen in Figure 4C for SBP, it is only detected with statistical significance in a few but not in the majority of the intervals considered, illustrated for SBP in Figure 4D. Similar results apply to MAP, DBP and HR (not shown).
Nonlinear Estimate of the "Solar" Period: SBP
22.8 -I-■-■-■-■-■-■-1-■-■-■-■-■-■-1-■-■-■-■-■-■-1-■-■-■-■-■-■-1
1-Sep-94 20-Oct-94 8-Dec-94 26-Jan-95 16-Mar-95
Time (calendar date)
Figure 4C. Time course ofthe about 24.0-hourperiod of systolic blood pressure, assessed concomitantly with the about 24.8-hour component by nonlinear least squares during isolation, indicates relative stability over time, the 95% CI remaining shorter than 24.8 hours, except for the first interval likely influenced by the transition from society.
Nonlinear Estimate ofthe "Solar" Amplitude: SBP
Figure 4D. Time course of the about 24.0-hour amplitude of systolic blood pressure during isolation only shows occasional statistical significance by the non-overlap of zero by the 95% CI.
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Discussion and Conclusion: For the entire 267 days of social isolation, the BP and HR of K were characterized by a strong and stable about 24.8-hour component, whereas a much weaker about 24.0-hour rhythm remained demonstrable overall but only in a few of the 29 8-week intervals examined. Desynchronization from 24.0 hours in human isolation studies is not new, but this thoroughly examined case raises the question whether deviation from 24.0 hours preferentially assumed a period of 24.8 hours, close to twice the tidal period. Evidence reviewed elsewhere in this issue suggests that it may not necessarily be only a chance event. The possibility of a pull by the moon in the absence of strong 24.0-hour synchronizers deserves further investigation. For this purpose, the dense and automatically collected data of K represent a great asset amenable to additional analyses from a fresh new perspective.
REFERENCES
1. Haus E. Biologic aspects of a chronopathology. PhD Thesis, University of Minnesota, 1970. 361 pp.
2. Wever RA. The Orcadian System of Man: Results of Experiments under Temporal Isolation. New York: Springer-Verlag; 1979. 276 pp.
3. Halberg F, Cornelissen G, Katinas G, SyutkinaEV, Sothern RB, ZaslavskayaR, Halberg Francine, Watanabe Y, Schwartzkopff O, Otsuka K, Tarquini R, Perfetto P, Siegelova J. Transdisciplinary unifying implications of circadian findings in the 1950s. J Circad Rhy 2003; 1: 2. 61 pp.
4. Cornelissen G, Halberg F. Introduction to Chronobiology. Medtronic Chronobiology Seminar #7, April 1994, 52 pp. (Library of Congress Catalog Card #94-060580; http://www.msi.umn. edu/~halberg/)
5. Halberg F, Cornelissen G, Sonkowsky RP, Lanzoni C, Galvagno A, Montalbini M, Schwartzkopff O. Chrononursing (chronutrics), psychiatry and language. New Trends in Experimental and Clinical Psychiatry 1998; 14: 15-26.
6. Marquardt DW. An algorithm for least-squares estimation of nonlinear parameters. J Soc Indust ApplMath 1963; 11: 431-441.
Dedicated to the memory of Maurizio Montalbini (1953-2009) who had "hoped it [the study chrono-meta-analyzed herein] would provide valuable insight into the natural cycles of the body". Indeed, he achieved more; he demonstrated natural solar and lunar cyclicities and their continued response (resonance with) geomagnetism through which the lunar effect might be mediated.
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URINARY OUTPUT AND GEOMAGNETISM REVISITED
Germaine Cornelissen1, Franz Halberg1, Judy Finley1, Faithe Thomas1, Jarmila Siegelova2, Jiri Dusek2, Bohumil Fiser2
1 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA 2 St. Anna Teaching Hospital, Masaryk University, Brno, Czech Republic
In 1989, Payne et al. (1) concluded that urinary metabolite retention is periodic in nature insofar as in 815 patients presenting as emergency admissions in two hospitals in Great Britain, a higher incidence of urinary retention was observed during the new moon in comparison with the other phases of the lunar cycle, a finding prompting our chrono-meta-analysis herein. No association was found by the original authors between urinary retention and circadian, monthly and seasonal periodicity. We confirm Payne et al.'s (1) negative finding only when we test for a circannual component separately. When in turn we use a combined linear-nonlinear approach to concomitantly fit a year and a half-year by the nonlinearly extended cosinor (2-4), we find, Figure 1, that the combined model is statistically significant (P<0.02). Both tested components are present, and with this model, the geomagnetic half-year matches the contribution of the seasons.
The half-year has been associated with geomagnetism by Chapman (5) as reviewed (6) with biospheric associations (7). That it may influence human water metabolism is suggested by a study of nocturia of a 54-year-old man with benign prostatic hypertrophy, who recorded for about 4 years the number of times he awoke each night to urinate (8). These data have been reanalyzed by the methodology of chronomics, the mapping of time structures (chronomes), involving the computation of least squares spectra of the urinary record and of environmental variables recorded during the same 4-year span. In addition to the previously reported monthly variation (8), other periodicities have been documented, including two separate components with periods of one week and of a near-week, Figure 2 (9). The precise 7-day component may be a mainly exogenous resonance with external influences such as a weekly social schedule, whereas the near-week may be a resonance with natural changes in geomagnetics, reflecting in part changes in other non-photic natural environmental factors. Table 1 shows congruent periods in nocturia and geomagnetic activity (9), and Figure 3 congruence between geomagnetics and heart rate of a woman isolated from society in a cave specially designed for studies of natural periods in and around us (10). Congruence is also apparent for nocturia in Figure 4, all extending the scope of Figure 1.
1. Payne SR, Deardon DJ, Abercrombie BF, Carlson GL. Urinary retention and the lunisolar cycle: is it a lunatic phenomenon? BMJ 1989; 299: 1560-1562.
2. Halberg F. Chronobiology: methodological problems. Actamed rom 1980; 18: 399-440.
3. Cornelissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T (Eds.) Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
4. Refinetti R, Cornelissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692
5. Chapman S. The solar and lunar diurnal variations of terrestrial magnetism. Phil Trans Roy Soc Lond Series A 1919; 218: 1-118.
6. Chapman S, Bartels J. Geomagnetism. 3rd ed. Oxford: Clarendon Press; 1962. 1049 pp.
7. Cornelissen G, Halberg F, Pollmann L, Pollman B, Katinas GS, Minne H, Breus T, Sothern RB, Watanabe Y, Tarquini R, Perfetto F, Maggioni C, Wilson D, Gubin D, Otsuka K, Bakken
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EE. Circasemiannual chronomics: half-yearly biospheric changes in their own right and as a circannual waveform. Biomed & Pharmacother 2003; 57 (Suppl. 1): 45s-54s.
8. Axelrod DE. Amonthly period of symptoms associated with benign prostatic hyperplasia. Urology 2000; 55: 436iv-436vi.
9. Cornélissen G, Axelrod DE, Halberg F. About-weekly variations in nocturia. Biomed & Pharmacother 2004; 58 (Suppl. 1): S140-S144.
10. Halberg F, Cornélissen G, Sonkowsky RP, Lanzoni C, Galvagno A, Montalbini M, Schwartzkopff O. Chrononursing (chronutrics), psychiatry and language. New Trends in Experimental and Clinical Psychiatry 1998; 14: 15-26.
11. Halberg F, Breus TK, Cornélissen G, Bingham C, Hillman DC, Rigatuso J, Delmore P, Bakken E, International Womb-to-Tomb Chronome Initiative Group: Chronobiology in space. Keynote, 37th Ann. Mtg. Japan Soc. for Aerospace and Environmental Medicine, Nagoya, Japan, November 8-9, 1991. University of Minnesota/Medtronic Chronobiology Seminar Series, #1, December 1991, 21 pp. of text, 70 figures.
12. Vladimirskii BM, Narmanskii VYa, Temuriantz NA. Global rhythmics of the solar system in the terrestrial habitat. Biophysics 1995; 40: 731-736.
Support. GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
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Table 1. Major periods of nocturia and geomagnetic activity*
octuri
h a Kp
Trial Period Period Amplitude Period Amplitude
(days) (95% CI) (95% CI)
Different Behavior
365 349.8 0.15 432.2 0.11
(320.7; 378.9) (0.05; 0.25) (363.3; 501.2) (0.0; 0.23)
182.5 181.8 0.3
(177.3; 186.3) (0.19; 0.42)
Similar Behavior
26 26.22 0.13 26.42 0.17
(26.03;26.40) (0.03; 0.23) (26.24; 26.59) (0.05; 0.28)
7 7.007 0.14 7.021 0.15
(6.992; 7.022) (0.02; 0.27) (7.004; 7.038) (0.00; 0.29)
6.85 ** 6.87 0.11 6.879 0.14
(6.849; 6.889) (0.00; 0.22) (6.862; 6.895) (0.00; 0.29)
"Assessed concomittantly
I I
* CI: Confidence Interval. Although the 95% CIs of the circannual periods of nocturia and Kp partly overlap, the behavior of the two variables differs in that for nocturia, the period is not statistically significantly different from one year, but for Kp it is statistically significantly longer than one year (when series longer than 4 years are analyzed). The difference in behavior also related to the fact that nocturia is characterized primarily by an about-yearly variation, whereas Kp has a much more prominent half-yearly variation, which is not detected for nocturia.
Chrono-meta-analysis revealing that in a population of 685 patients, resonance with the geomagnetic half-year more than matches resonance with the seasons, as gauged by the
0.5-year/1.0-year amplitude ratio
Yearly and Half-yearly Changes in Urinary Retention *
15 -i-1
8/1/1985 8/1/1986 8/1/1987 8/1/1988
Time (calendar date)
* Payne SR, Deardon DJ, Abercrombie GF, Carlson GL. BMJ 1989; 29: 1560-1562.
Figure 1. Chrono-meta-analysis of Table II from (1) on the number of patients per month presenting with acute urinary retention in Portsmouth. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Least Squares S pectrum of Nocturia in 54-year old Man Diagnosed with Benign Prostatic Hyperplasia
0.16
0.14
0.12
_C
"c
CD 0.10
CO
S
03 M— 0.08
O
z
Ol 0.06
TJ
"q. 0.04
e
< 0.02
0.00
Circannual
Circaseptan (7 days and .87 days)
20 40 60 80
Frequency (cycles in 52 weeks)
100
120
Figure 2. Anticipated spectral peaks resolved with their uncertainties by linear-nonlinear rhythmometry (2-4). In particular, two separate components in the circaseptan range deserve further study. Their relative prominence, gauged by the amplitude difference in nocturia, may be aligned with a similar difference in geomagnetic activity. The 6.87-day period is similar to the natural geomagnetic activity and the 7-day period is probably anthropogenic, yet in each case there is only a frequency and no phase synchronization, pointing to resonance without phase lock-in. By contrast to Figure 1, a half-year could not be demonstrated for nocturia in this patient. © Halberg.
DO GEOMAGNETIC DISTURBANCES AFFECT HUMAN PHYSIOLOGY?
Heart Rate
Geomagnetic Index (Kp)
95% Confidence Interval from Nonlinear Analyses
79.5 80.0 80.5 81.0 81.5 82.0
Circasemiseptan Period (Hours)
82.5
* 28-year old woman (K) during 267 days of isolation from society (26 July 1994 to 20 April 1995).
Figure 3. Even if temporal relations are not necessarily causal, a possible influence of geomagnetics on human HR is suggested by closeness of circasemiseptan period reached nonlinearly for HR (monitored automatically around the clock for 267 days of isolation from society) and Kp, a global geomagnetic disturbance index (recorded every 3 hours during the same span) (10). © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Figure 4. Similarity in the circaseptan range of spectra on nocturia and the planetary geomagnetic index Kp, both with more than a single about 7-day component. One component in nocturia corresponds to the social week. It is almost certainly societal, of anthropogenic origin. It is close to a spectral peak for the geomagnetic index Kp, which in this record happens to be characterized by a period slightly but statistically significantly longer than precisely 7 days (52 cycles in 52 weeks, vertical line), as gauged by its 95% confidence interval. The next peak to the right corresponds to a component with a period of 6.87 (nocturia) or 6.88 (Kp) days, also resolved by nonlinear least squares. The about 6.88-day component in Kp, albeit wobbly, is almost certainly natural environmental, as reported earlier (11, 12), and may pull, if not synchronize, a built-in component of similar period length in nocturia. © Halberg.
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CIRCASEMIDIAN AND CIRCASEMISEPTAN GAUGES OF VASCULAR AD JUSTMENT AFTER TRANSMERIDIAN CROSSING OF THREE TIME ZONES
Othild Schwartzkopff1, Dewayne Hillman1, Franz Halberg1, Germaine Cornelissen1, Mark Engebretson2, George S. Katinas1, Sergei M. Chibisov3, Jarmila Siegelova4,
Rajesh Agarwal3, Rollin McCraty5
1 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA 2 Department of Physics, Augsburg College, Minneapolis, MN, USA 3 People's Friendship University of Russia, Moscow, Russia 4 Masaryk University, Brno, Czech Republic 5 Institute of HeartMath, Boulder Creek, CA, USA
A temporal microscopy (microchronometry, a term suggested by the senior author, or perhaps microbiochronometry) applied by the cosinor (1-3) to consecutive intervals of a time series is the counterpart of serial sections used in histology. It serves to reveal rhythms as the counterpart of cells, with the anticipation that some rhythm alterations may precede cellular change and could thus provide useful harbingers for preventive action. This approach can be used for analyses revolving around the abundant literature dealing with transmeridian dyschronism (jet lag) and related problems (4-15) by considering mainly the 24-hour component, usually without parameter estimation after prior hypothesis testing, with only exceptional concern with circaseptans (16-19), circasemiseptans (19,20) and circannuals (21), and without consideration of other non-photic (22) components. It seems the more important to include an assessment of second harmonics of both the circadian and circaseptan components (with periods of 12 and 84 hours, respectively). We herein consider circasemidians and circasemiseptans with circadians and circaseptans, the former two components considered in their own right and as second harmonics accounting for non-sinusoidality. With certain interval lengths chosen for analysis by chronobiologic serial sections on data involving flights across only a few (here three) time zones and a return trip by ship rather than air, these harmonic terms happen to be sensitive and the only gauges of adaptation.
Systolic (S) and diastolic (D) blood pressure (BP) and heart rate (HR) were automatically measured with a TM-2421 monitor (A&D, Tokyo, Japan) at half-hour intervals before, during and after an arctic tour from 20 July to 4 August 2005. Serial sections on these and bracketing data, extending until 22 August 2005 were performed by the separate fit of cosine curves with trial periods (xs) of 168, 84, 24 and 12 hours. Departure from the USA was on July 18 to Anchorage, Alaska, USA, and from there to Anadyr, Russia (64°44'N, 177°20'W). Return was from Resolute, Nunavut, Canada, 74°42'N, 95° 10'W, on August 4, 2005. Intervals were chosen to cover by their length 4 to 8 cycles in the case of circadian and circasemidian analyses, or 2 to 4 cycles in the case of circaseptan and circasemiseptan analyses. They were displaced by increments of 12 or 24 hours for the case of circadian-circasemidian and circaseptan-circasemiseptan analyses, respectively. The circadian and circaseptan rhythms remain environmentally synchronized, as apparent from the horizontal time course of their acrophases, Figures 1-3. By contrast, their second harmonics show the major phase adjustments for each of the variables examined. Whether we deal with changes in the waveform of the circadian system or with an ~ 12-hour oscillation in its own right (23) remains to be determined and cannot be inferred from their different behavior during adjustments.
Analyses by sphygmochron (24) of 7-day/24-hour records of BP and HR routinely consist of the concomitant fit of cosine curves with xs of 24 and 12 hours to account for the traditional
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NONINVASIVE METHODS IN CARDIOLOGY 2010
approximation of the usually non-sinusoidal circadian waveform of these variables. Determining the time of maximum of such a composite model (orthophase) with an estimate of uncertainty (95% confidence interval) was achieved in the context of cancer chronotherapy with adriamycin (25, 26). The addition of harmonic terms to describe the circadian waveform was illustrated for the case of inter-beat intervals (27). Analyses of such R-R intervals to derive the correlation dimension as a measure of fractal scaling indicated the critical role of the 12-hour component to separate healthy men from patients with coronary artery disease (28). Harmonic terms indeed may be more sensitive gauges, notably for adjustments after flights over a few time zones: a 3-hour shift as in the case here reported corresponds to a 90° change in phase by the 12-hour component, but only to a 45° change in phase by the 24-hour component. The 12-hour and 24-hour components could be routinely included in the study by 24- and 168-hour cosinor analyses of transmeridian or shiftwork-related adjustments. Conclusion. Harmonic terms could be routinely used to study adjustments to changes in schedule, provided they contribute with statistical significance to the waveform of the fundamental rhythm(s) of interest and, much more generally, for studies in health and disease.
REFERENCES
1. Halberg F. Chronobiology. Annu Rev Physiol 1969; 31: 675-725.
2. Cornelissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T (Eds.) Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
3. Refinetti R, Cornelissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692
4. Hildebrandt G. Phase manipulation, shift work, and jet lag: an overview. Progress in Clinical and Biological Research 1987; 227B: 377-390.
5. Vigh B, Manzano MJ, Zadori A, Frank CL, Lukats A, Rohlich P, Szel A, David C. Nonvisual photoreceptors of the deep brain, pineal organs and retina. Histol Histopathol 2002; 17: 555-590.
6. Moser M, Penter R, Fruehwirth M, Kenner T. Why life oscillates: biological rhythms and health. Conference proceedings. Annual International Conference of the IEEE Engineering in Medicine and Biology Society. IEEE Engineering in Medicine and Biology Society. Conference. 01/02/2006; 1: 424-428.
7. Atkinson G, Edwards B, Reilly T, Waterhouse J. Exercise as a synchronizer of human circadian rhythms: an update and discussion of the methodological problems. Eur J Appl Physiol 2007; 99: 331-341.
8. Paquet J, Kawinska A, Carrier J. Wake detection capacity of actigraphy during sleep. Sleep 2007; 30: 1362-1369.
9. Ptacek LJ, Jones CR, Fu YH. Novel insights from genetic and molecular distribution of the human clock. Cold Spr Harb Symp quant Biol 2007; 273-277.
10. MartinoTA, OuditGY, HerzenbergAM, TataN, KoletarMM, KabirGM, Belsham DD, BackxPH, Ralph MR, Sole MJ. Circadian rhythm disorganization produces profound cardiovascular and renal disease in hamsters. Am J Physiol Regul Integr Comp Physiol 2008; 294 (5): R1675-R1683.
11. Scheer FA, Shea TJ, Hilton MD, Shea SA. An endogenous circadian rhythm in sleep inertia results in greatest cognitive impairment upon awakening during the biological night. J Biol Rhythms 2008; 23:353-361.
12. Arendt J. Managing jet lag: some of the problems and possible new solutions. Sleep Med Rev 2009; 13: 249-256.
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13. Minami Y, Kasukawa T, Kakazu Y, Iigo M, Sugimoto M, Ikeda S, Yasui A, van der Horst GT, Soga T, Ueda HR. Measurement of internal body time by blood metabolomics. Proc Nat Acad Sei USA 2009; 106: 9890-9895.
14. Scheer FA, Hilton MF, Mantzoros CS, Shea SA. Adverse metabolic and cardiovascular consequences of circadian misalignment. Proc Nat Acad Sei USA 2009; 106: 4453-4458.
15. Waterhouse J, Reilly T. Managing jet lag (comment). Sleep Med Rev 2009; 13: 247-248.
16. Halberg F, Hillman D, Halberg E. Spectral approach to schedule shifts by circadian and infradian cardiovascular marker rhythm assessment. Chronobiologia 1988; 15: 274.
17. Halberg F, Hillman D, Halberg E. Circaseptan (about 7-day) cardiovascular adjustment after transmeridian round-trip (west-east-west vs. east-west-east) flights. Chronobiologia 1988; 15: 247-249.
18. Hillman D, Halberg E, Halberg F. More on about-weekly (circaseptan) cardiovascular variation after transmeridian (7-h shift of schedule) east-west-east flights. Chronobiologia 1988; 15: 249-250.
19. Cornelissen G, Halberg J, Halberg F, Sanchez de la Pena S, Nelson W, Schwartzkopff O, Stoynev A, Haus E. Schedule shifts, cancer and longevity: good, bad or indifferent? J Experimental Therapeutics Oncol 2008; 7 (4): 263-274.
20. Schweiger H-G, Berger S, KretschmerH, MörlerH, Halberg E, Sothern RB, Halberg F. Evidence for a circaseptan and a circasemiseptan growth response to light/dark cycle shifts in nucleated and enucleated Acetabularia cells, respectively. Proc Natl Acad Sei USA 1986; 83: 8619-8623.
21. Marques N, Marques MD, Marques RD, Marques LD, März W, Halberg F. Delayed adjustment after transequatorial flight of circannual blood pressure variation in 4 family members. II Policlinico, SezMedica 1995; 102: 209-214.
22. Halberg F, Cornelissen G, Sothern RB, Katinas GS, Schwartzkopff O, Otsuka K. Cycles tipping the scale between death and survival (= "life"). Progress of Theoretical Physics 2008; Suppl. 173: 153-181.
23. Katinas G. Adjustment after schedule shifts, notably jet lag, assessed by multiple 12- and 24-hour and 84- and 168-hour cosine fits and complementary methods. This issue.
24. Cornelissen G, Halberg F, Bakken EE, Singh RB, Otsuka K, Tomlinson B, Delcourt A, Toussaint G, Bathina S, Schwartzkopff O, Wang ZR, Tarquini R, Perfetto F, Pantaleoni GC, Jozsa R, Delmore PA, Nolley E. 100 or 30 years after Janeway or Bartter, Healthwatch helps avoid "flying blind". Biomed & Pharmacother 2004; 58 (Suppl 1): S69-S86.
25. Tong YL, Nelson WL, Sothern RB, Halberg F. Estimation of the orthophase (timing of high values) on a non-sinusoidal rhythm, illustrated by the best timing for experimental cancer chronotherapy. In: Halberg F (Ed.) Proc. XII Int. Conf. Int. Soc. for Chronobiology, Washington, D.C., 1975. Milan: II Ponte; 1977. p. 765-769.
26. Tong YL. Interval estimation of the critical value in a general linear model. Ann Inst Statist Math 1987; 39 (Part A): 289-297.
27. Cornelissen G, Bakken E, Delmore P, Orth-Gomer K, Äkerstedt T, Carandente O, Carandente F, Halberg F. From various kinds of heart rate variability to chronocardiology. Am J Cardiol 1990; 66: 863-868.
28. Otsuka K, Cornelissen G, Halberg F. Circadian rhythmic fractal scaling of heart rate variability in health and coronary artery disease. Clinical Cardiology 1997; 20: 631-638.
Support. GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
82
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'OS, F, 83, £005, lour 07(20-12:00 (1) -DfflM-12:00{2), SBP (N=1780). Numbers or acrophsse charts between horizontal dashed lines (left) are the perbd Med (=360") and in (), the, ir-jerval analyzed and ihe increment by which this interval was displaced for consecutive analyses, all in hours (hi: vertical c'ashec'lires are 1. departure from Minnesota for a flight to Anadir. Russia, followed bya Northwest Passage cruise from west to east and 2. return flight from Resolute. Nunavut, Canada. Phases are doubly ptotied when nearO' or MO'. SEs ir raw 2 (topi are dis'iar-ces Jon the dot shown by a tiny circled bracket,to ihe lower or upper [M+AI curves.
Figure 1. For systolic blood pressure (SBP), with the intervals chosen for analyses, the major adjustment along the 24-hour scale is gauged by the 12-hour cosine fit (bottom left). The 84-hour component suggests, but does not validate, a jump in phase since it is statistically significant too briefly before the return home and thereafter. © Halberg.
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'"OS. F, S3. 2005, ■our07/2rj'12:0rj (1). 00/M'12:M (2), HR(N=170C). NumwrE on acrophase chars between horizontal dashetilirws (left) arc the pe rim faec (aSWlarc in (), the interval analyzed and'he increment by which this internal was eisplacco for ccflsec-iive analyses, all in hours (h): vertical cashed lines are 1, deparure from Minnesota for a fiigh: lo Anadir, FLssia. Fo owed by a Mcrhwcst -assace cruise from v.est to east, anc 2. return fiigh: from -lesa-jle, NunaA,t Canada rrvi5cs are doubly poitc-d when nearC" or360'. SEs In ro*2 anccis:unc£3frcm:hccoLshottnbya tiny circled rvackeL. ;othe lower (W)cr upper (I.UA) curves.
Figure 3. For heart rate (HR), noise clouds acrophase behavior and the acrophases of components that are not statistically significant cannot rigorously distinguish a gradual shift from a sudden jump. © Halberg.
NONINVASIVE METHODS IN CARDIOLOGY 2010
A FAR-TRANSYEAR IN THE BLOOD PRESSURE OF A 17-YEAR-OLD MALE
Fumihiko Watanabe*, Germaine Cornélissen*, Yoshihiko Watanabe*, Franz Halberg*
*Department of Medicine, Tokyo Women's Medical University, Tokyo, Japan •Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
While a father (YW) self-monitored blood pressure (BP) and heart rate (HR) automatically half-hourly for decades, FW, his clinically healthy boy, has self-measured these variables as a follow-up on dense neonatal monitoring (1-14). This paper updates an earlier report on a far-transyear, a spectral component with a period, X, longer than a year by several months (11). With Figure 1, we here document again, with added data, that in both systolic (S) and diastolic (D) BP FW has, during ages 8-17, a far-transyear, defined broadly as a spectral component with a x longer than a year (y) ~ trans = beyond (1 year length) ~ by several months (1.2 years < [x - CI {95% confidence interval}] < [x + CI] < 1.9 years), to be distinguished from a near-transyear (1.00 year < [x - CI {95% confidence interval}] < [x + CI] < 1.20 years) (15). The far-transyear is the major peak in the para-annual region for both SBP and DBP, even when a peaklet is present at a trial period of precisely 1 year, notably for DBP By contrast for HR, Figure 1 shows a peak at the calendar year that is numerically slightly larger in amplitude than that of the also-present far-transyear.
Discussion. Atransyear (T) characterizes decades-long series of blood pressure and heart rate from 13 adults, mimicking, by the range of CIs (95% confidence intervals) of its periods, x, the range of CIs of xs of several physical variables, and further the incidence pattern of myocardial infarctions (Mis) (15, 16). Atransyear can coexist for a while with a calendar-year component (Y) in the same and/or in different geographic locations in sudden cardiac death (16,17), and is found in terrorism (18), natality (19,20), epilepsy (21) and stroke (22), among other conditions. A selective assortment of biospheric-environmental congruences in period is often encountered in the infradian spectral range as already noted in this case (11) and others (23).
REFERENCES
1. Watanabe Y, Katinas G, Watanabe F, Watanabe M, Cornélissen G, Otsuka K, Halberg F. Cardiochronomics for astrobiology: infradian prominence in heart rate of a healthy boy born at term. Abstract 20, 2nd International Symposium: Workshop on Chronoastrobiology & Chronotherapy, Tokyo Kasei University, Tokyo, Japan, November 17, 2001, unpaginated (2 pp).
2. Watanabe Y, Cornélissen G, Hellbriigge T, Watanabe F, Otsuka K, Schwartzkopff O, Halberg F. Partial spectral element in the chronome of a human neonatal heart rate at term. Biomedicine & Pharmacotherapy 2002; 56 (Suppl 2): 374s-378s.
3. Watanabe Y, Sothern RB, Katinas G, Cornélissen G, Watanabe M, Watanabe F, Otsuka K, Halberg F. Replication of anticipated circadecadal solar cycle modulation of cardiovascular circannual variation: Part III. Abstract 6, Proceedings, 3rd International Symposium: Workshop on Chronoastrobiology and Chronotherapy, Eriguchi M, ed, Research Center for Advanced Science and Technology, University of Tokyo, Nov. 9, 2002.
4. Watanabe Y, Cornélissen G, Katinas G, Sothern RB, Halberg F, Watanabe M, Watanabe F, Otsuka K. Non-photic, non-thermic circadecadal solar cycle interaction with cardiovascular circannual and circasemiannual variation in heated air-conditioned habitat. Biomedicine & Pharmacotherapy
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2003; 57 (Suppl 1): 55s-57s.
5. Watanabe Y, Cornélissen G, Watanabe F, Siegelova J, Dusek J, Halberg F. The trans- (-1.3) year in the blood pressure of a 10-year-old boy. Abstract 17, MEFA, Brno, Czech Republic, 04-07 Nov 2003. p. 22.
6. Watanabe Y, Cornélissen G, Watanabe M, Watanabe F, Otsuka K, Ohkawa S-i, Kikuchi T, Halberg F. Effects of autogenic training and antihypertensive agents on circadian and circaseptan variation of blood pressure. Clin Exp Hypertens 2003; 25: 405-412.
7. Watanabe Y, Watanabe F, Cornélissen G, Halberg F. Infradian aspects of the blood pressure (BP) and heart rate (HR) chronomes during adolescence. Abstract S8-12, 3rd Int Congress on Cardiovascular Disease, Taipei, Taiwan, 26-28 Nov 2004. Int J Cardiol 2004; 97 (Suppl 2): S15.
8. Watanabe Y, Halberg F, Cornélissen G, Katinas G, Watanabe F, Otsuka K, Bakken E, Sothern RB, Sothern SB. Differing modulations by seasons, Halberg's paraseasonality, and geomagnetics found at different circadian stages. In: Proceedings, 59th Annual Meeting, Japan Society of Neurovegetative Research, Tokyo, November 1-3, 2006. p. 61-63.
9. Watanabe Y, Halberg F, Cornélissen G, Katinas G, Watanabe F, Otsuka K, Bakken EE, Sothern RB, Sothern SB. Various modulations by the seasons and by paraseasonality at different circadian stages. The Autonomic Nervous System 2007; 44: 255-258.
10. Watanabe Y, Watanabe F, Cornélissen G, Halberg F. About-weekly changes in heart rate at birth and at 14 years of age in the presence of anxiety. PS-055, Proceedings, 2nd World Congress of Chronobiology, November 4-6, 2007, Tokyo, Japan, p. 89.
11. Watanabe F, Cornélissen G, Watanabe Y, Siegelova J, Czaplicki J, Halberg F, BIOCOS project. Differing far-transyear/calendar year amplitude ratios in blood pressure vs. heart rate in adolescence. In: Halberg F, Kenner T, Fiser B, Siegelova J, eds. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, October 4-7, 2008. p. 177-183. http://web.fnusa. cz/files/kfdr2008/sbornik_2008 .pdf
12. Watanabe Y, Cornélissen G, Katinas GS, Watanabe F, Fiser B, Siegelova J, Schwartzkopff O, Halberg F. Chronomics: Anxiety disorder in adolescence and heart rate asynchronized with weekly schedule. In: Halberg F, Kenner T, Fiser B, Siegelova J, eds. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, October 4-7, 2008. p. 189-203. http://web.fnusa. cz/files/kfdr2008/sbornik_2008 .pdf
13. Watanabe Y, Cornélissen G, Watanabe F, Tarquini R, Perfetto F, Siegelova J, Fiser B, Dusek J, Homolka P, Halberg F. Solar signatures in a boy's blood pressure and heart rate. In: Halberg F, Kenner T, Fiser B, Siegelova J, eds. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, July 7-10, 2009. (Dedicated to the 90th Anniversary of Prof. Franz Halberg.) p. 211-225. http://web.fnusa.cz/files/kfdr2009/sbornik_2009.pdf
14. Watanabe Y, Nintcheu-Fata S, Kaunas G, Cornélissen G, Otsuka K, Hellbrügge T, Schwartzkopff O, Bakken E, Halberg F. Methodology: partial moving spectra of postnatal heart rate chronome. Neuroendocrinol Lett 2003; 24 (Suppl 1): 139-144.
15. Cornélissen G, Masalov A, Halberg F, Richardson JD, Katinas GS, Sothern RB, Watanabe Y, Syutkina EV, Wendt HW, Bakken EE, Romanov Y. Multiple resonances among time structures, chronomes, around and in us. Is an about 1.3-year periodicity in solar wind built into the human cardiovascular chronome? Human Physiology 2004; 30 (2): 86-92.
16. Cornélissen G, Halberg F, Rostagno C, Otsuka K. A chronomic approach to cardiac arrhythmia and sudden cardiac death. The Autonomic Nervous System 2007; 44: 251-254.
17. Halberg F, Cornélissen G, Katinas G, Tvildiani L, Gigolashvili M, Janashia K, Toba T, Revilla M, Regal P, Sothern RB, Wendt HW, Wang ZR, Zeman M, Jozsa R, Singh RB, Mitsutake G, Chibisov SM, Lee J, Holley D, Holte JE, Sonkowsky RP, Schwartzkopff O, Delmore P, Otsuka K, Bakken
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EE, Czaplicki J, International BIOCOS Group. Chronobiology's progress: season's appreciations 2004-2005. Time-, frequency-, phase-, variable-, individual-, age- and site-specific chronomics. J Applied Biomedicine 2006; 4: 1-38. http://www.zsf.jcu.cz/vyzkum/jab/4_l/halberg.pdf.
18. Halberg F, Cornelissen G, Sothern RB, Katinas GS, Schwartzkopff O, Otsuka K. Cycles tipping the scale between death and survival (= "life"). Invited presentation, Nishinomiya-Yukawa International & Interdisciplinary Symposium 2007, What is Life? The Next 100 Years of Yukawa's Dream, Yukawa Institute for Theoretical Physics, Kyoto University, October 15-20, 2007. Progress of Theoretical Physics 2008; Suppl. 173: 153-181.
19. Mikulecky M, Florida PL. Daily birth numbers in Davao, Philippines, 1993-2003: Halberg's transyear stronger than year. Abstract, 26th Seminar, Man in His Terrestrial and Cosmic Environment, Upice, Czech Republic, May 17-19, 2005.
20. Mikulecky M. Reanalyza natality v jizni brazilii ~ opet dominuje Halbergova parasezonalita: International Conference on the Frontiers of Biomedical Science: Chronobiology, Chengdu, China, September 24-26, 2006, p. 188-193.
21. Kovac M, Mikulecky M. Time sequence of epileptic attacks from the point of view of possible lunisolar connections. International Conference on the Frontiers of Biomedical Science: Chronobiology, Chengdu, China, September 24-26, 2006, p. 175-179.
22. Kovac M, Mikulecky M. Secular rhythms and Halberg's paraseasonality in the time occurrence of cerebral stroke. Bratisl Lek Listy 2005; 106 (2): 423-427.
23. Halberg F, Cornelissen G, Wilson D, Singh RB, De Meester F, Watanabe Y, Otsuka K, Khalilov E. Chronobiology and chronomics: detecting and applying the cycles of nature. Biologist 2009; 56 (4): 209-214.
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Systolic Diastolic (D) Blood Pressure (BP) and Henri Hütt lEIH) ScIT-Measurements on Awakening during nearly years by a boy (FW) 8-17 years of arc Hevtal Far-Transycar *
• Nonlirwwly esii mated periods und Lheir 95% confidence intervals are 1.40 11,36, 1.43], 1,42 [1.37, L Ati[, jnd ] JS 11,32H 1.44J yon for SBP. DBF. aid HR. respectively. CotresponJLnjs amplitudes and their 95% cwifidcnw intervals arc 12,7, 4.S] and ] .8 [1.2. 2J1 mmHg ft* SBP and DBPh rcspcu'tivvlv, mJ 16 |OS. 2.3] beaLi/min CorHR.
Figure 1. Prominence of 1.38-year far-transyear, gauged by amplitude, A, exceeds the A estimate at the trial period of a calendar year in systolic and diastolic blood pressure. Heart rate has a slightly more prominent calendar-yearly component. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
CHRONOBIOLOGICALLY INTERPRETED ABPM (C-ABPM) IN DELAYED SLEEP
PHASE SYNDROME
Yoshihiko Watanabe*, Germaine Cornélissen*, Franz Halberg*, Jarmila SiegelovaJ
Tokyo Women's Medical University, Tokyo, Japan •University of Minnesota, Minneapolis, MN, USA {Masaryk University, Brno, Czech Republic
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH).
We here introduce chronobiologically interpreted blood pressure (BP) and heart rate (HR) monitoring with analyses of the time series as a whole (globally) and/or in sections of the data (locally), i.e., glocally, to study a delay in the timing of the habitual sleep span usually uninterpreted for biospheric and environmental interactions, the topic of chronomics. A chronomic analysis aligning physiological data with environmental ones remains to be carried out.
Case reports
HS. Suddenly, patient HS (M, 41 y) could not go back early in the morning to work at his company, where he made drawings. He came to our hospital with a relatively severe to absolute inability to advance his sleep time (phase) to earlier hours by enforcing conventional sleep-wake times. He was diagnosed with a delayed sleep phase syndrome (DSPS) because of his sleep-wake logs, kept for 3 prior weeks, documenting a consistent habitual pattern of sleep onset, later than 3 am, and lengthy sleeps. He monitored his BP and HR around the clock at 30-minute intervals before and after bright light (5000 lux for 2 hours [h]/day) therapy administered first in the afternoon, then progressively earlier in the day, with the rate of advance being 1 h/week. Monitoring started on 26 Feb 1998 and lasted until 10 Jul 1998. Treatment started on 2 Apr 1998 and succeeded in allowing the patient to sleep and work on the regular societal activity schedule. YW. For a while, patient YW (M, 35 y) could not go to his office early in the morning because his sleep phase was delayed toward early morning. He could not go to bed before 3 am. He understood that something was happening in his body. Every day when he got up, he felt general fatigue. Some days, he did not retire until nearly 4:30 am. In spite of this unacceptable condition, he had worked hard in his office from morning to midnight. One day, he did not leave his office until the sun was rising. As a physician, he realized that he had a sleep disorder and knew about treatment methods that claimed to adjust the time of retiring. He tried to do a sort of chronotherapy by will power, not a chronotherapy by bright light. Forcing himself to go to bed before 1 am was very difficult on his ordinary routine, but he eventually succeeded in advancing his bedtime to that of his society.
Method
The data were analyzed by chronobiologic serial sections. In this approach, a cosine curve with a given period is fitted by cosinor to data in a given interval progressively displaced in increments throughout the time series. Least squares spectra were also obtained to provide an overall assessment of the time structure of BP and HR during specified spans. Periods corresponding to spectral peaks were used as initial values in nonlinear analyses that estimate the period as well as the MESOR, amplitude and acrophase, each parameter with its CI (95% confidence interval). The extended cosinor (1-3) with Marquardt's algorithm was used, with several models that allowed all periods to vary, or
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only some of them, with or without harmonic constraints. Results
In the case of HS, chronobiologic serial sections, obtained using a 7-day interval displaced with 1-day increments, indicate that treatment (starting at the vertical dashed line) was associated with a gradual advance of the 24-h acrophase in systolic (S) and diastolic (D) BP, Figures 1 and 2, as well as HR, Figure 3. The circadian rhythm was invariably the most prominent component in the least squares spectra in all data, Figure 4, in the section before treatment, Figure 5, and in that summarizing data after the start of light therapy, Figure 6. A summary at a trial period of 24 h confirms that for all three variables, the CIs of the acrophase after start of treatment did not overlap the corresponding CIs before treatment (Table 1). For SBP and DBP but not for HR, the 24-h amplitude increased on treatment. A two-component model consisting of cosine curves with trial periods of 24 and 12 h (with no constraint of harmonicity) was fitted by nonlinear least squares to data in each of the 5 spans (before treatment and to 4 separate spans after start of treatment). In each case, the model was found to be statistically significant, each component contributing to the overall variability in the data with statistical significance (Table 2). In all instances, estimated periods were close to 24 and 12 h and their CIs covered 24 and 12 h, respectively.
Least squares spectra, computed over the entire about 4-month span, over the about 1-month span before treatment, and over the entire about 3-month span on treatment, all had the two major spectral peaks corresponding to frequencies of one and two cycles per day (Figures 4-6). Only before treatment had the circasemidian component a period slightly longer than 12 h in the case of SBP and DBP but not HR (Figure 5). The period of 12.3 h is very close to the tidal period. In the case of all three variables, there was then another smaller spectral peak in the circadian region corresponding to a period of about 26.4 h (Figure 5), no longer detected after the start of treatment (Figure 6). Accordingly, a model consisting of a cosine function with a fixed 24.0-h period and of cosine functions with trial periods of 26.4 and 12.3 h was fitted to data before the start of bright light therapy. All components are found to contribute with statistical significance to the model, except for the about
12.3- h component of HR (Table 3), in keeping with the results of least squares spectra. When a slightly different model was used in which the trial period of 24.0 h was allowed to vary, similar results were obtained, the estimated circadian period being very close to 24.0 h with a CI overlapping 24 h. These results indicate that for patient HS, DSPS was associated with the presence of a second circadian component that had a period longer than 24 h, albeit of lesser prominence than the concomitantly present 24.0-h synchronized component. DSPS was also associated with a desynchronization of the 12-h component of BP but not of HR. Bright light therapy restored a 12-h synchronized circasemidian component and amplified the 24-h synchronized circadian amplitude of BP but not that of HR. The secondary circadian component with a period of about 26.4 h was no longer detected with statistical significance after the start of bright light therapy.
Figure 7 shows acrophases before, during and after YW's DSPS. Non-overlapping CIs of acrophases indicate the statistical significance of the phase delay in all three variables investigated (not shown). Figure 8 shows the very great prominence of the 24- and 12-h components. Therefore, these two components were fixed for follow-up extended cosinors, to prevent them from interfering with the estimation of any 24.8- and 12.4-h components. These data were fitted by four models in all of which the periods of the two dominant components (24 and 12 h) were fixed. In model 1, the 24.8- and
12.4- hour components were allowed to vary without constraint; in models 2 and 3, only the 24.8 h or the 12.4 h component was added to the fixed 24-h and 12-h cosine curves; and in model 4, both were allowed to vary, but constrained to be harmonically related. Model 2, fixing the 24.0 and 12.0 components and allowing the 24.8-h period to vary, was found to fit the data well before and during
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DSPS. Before the span with DSPS (1 Jan-12 Mar 1988), the period of SBP was estimated as 24.70 h [CI: 24.59, 24.82] and its double circadian amplitude was 4.88 [2.06, 7.70] mmHg by comparison with double amplitudes of 20.62 and 14.16 mmHg forthe 24.0 h and 12.0 h components, respectively. The DBP period was 24.65 h [24.53, 24.76] with a double amplitude of 4.04 [1.82, 6.28] mmHg by comparison with double amplitudes of 16.14 and 11.38 mmHg forthe 24.0 h and 12.0 h components, respectively. In the case of HR, the period was 24.69 h [24.55, 24.83] with a double amplitude of 3.50 beats/min [1.16, 5.86] by comparison with double amplitudes of 14.56 and 9.94 beats/min for the 24.0 h and 12.0 h components, respectively. During DSPS (13 Mar-25 Aug 1988), the SBP period was 24.75 h [24.66, 27.84] with a double amplitude of 1.74 mmHg and a CI slightly overlapping zero [-.04, 1.77]. The period of DBP was 24.72 h [24.66, 24.78] and its amplitude 2.10 mmHg [0.62, 3.58]. For HR, the period was 24.76 h [24.68, 24.83] with an amplitude of 1.84 beats/min [0.20, 3.50]. After the DSPS (18 Sep-31 Dec 1988), the more complete model 4 allowed the demonstration of both -24.8 h and -12.4 h components for BP but not HR. The estimated fundamental periods were 24.75 h [24.69, 24.80] and 24.75 h [24.70, 24.80] for SBP and DBP, respectively, with corresponding double amplitudes of the -24.8 h component of 1.88 [-.04, 3.78] and 1.36 [-.04, 2.78] mmHg and of the second harmonic of 2.16 [0.24, 4.08] and 1.70 [0.28, 3.10] mmHg, respectively. The decimals in all of these results are given only to indicate, in the case of periods, the presence or absence of overlap by CIs of 24.8 and 24.0 hours and in the case of double amplitude, the absence or presence, and in the latter case the extent of an overlap of zero. No quantitative importance beyond the foregoing considerations is attached to the decimals.
Discussion
Elsewhere, we show that an actual frequency change in a time series results in multiple peaks, as does a phase change. Therefore, a glocal analysis is recommended in dealing with any ecfrequentia that has been found in blind individuals by Emens et al. (5), who have reviewed the literature on circadian clocks and free-running, terms and concepts coined by analogy to a free-running oscillator in the early 1950s (6, 7). The finding of a 26.4-h period could be simply a free-running desynchronized period with the 24-h period masking it (5). An earlier finding of a 24.7h period (only) in the SBP and reported without a confidence interval in 1973 (in a blind boy for, one year after a bilateral retinoblastomectomy during 14 days at home), was not analyzed in the circasemidian region of the spectrum (8; cf. 9).
The finding of a near-tidal period of 12.3 h in BP but not in HR of HS during DSPS and in YW only after DSPS lets us question the pertinence of a tidal period (10) to the DSPS. More generally, tidal components deserve consideration since the double tidal 24.8-h period was found in a selenosensitive woman (9); it certainly cannot be generalized, but it provides an objective basis for lunar effects when the double tidal period (10) appears in her self-ratings of vigor in two untreated adynamic episodes and the 24.8 h period is also found in SBP and HR (and a 24.75-h period in DBP in the third desynchronized episode as the dominant components with the largest amplitudes). Whether a lunar cycle occurs in some others is a possibility with a precedent in the longest study in isolation from society for 267 days in a cave (11, 12).
In the circaseptan spectral region, a selective pull of geomagnetics is documented for a physiological variable, HR, but not for BP which remained societally 7-day synchronized (13). A selective assortment characterizes environmental-biospheric congruences of periods (14). Gravity may act by inducing currents piezoelectrically (15) or via positive holes (16) that reach the earth-air interface. From this viewpoint, the presence of a longer-than-12-h semidian component in HS and after DSPS in YW deserve attention. Whether we deal with free-running, also from the moon in the case of
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24.8-h periods, is also at variance with data on rats that show an average 24.8-h period in continuous light of low intensity, in keeping with lunar synchronization (17). A second circadian component in subjects with and without DSPS with a period longer than 24 h and the presence of a trans-semidian (trans = beyond, i.e., longer than a 12-h) component remain to be investigated on added subjects. If the methodologic aspect of this paper introduces a glocal approach, i.e., the analysis of time series as a whole, globally and in sections, it will have served its purpose, but any effects of the moon remain a challenge.
REFERENCES
1. Halberg F. Chronobiology: methodological problems. Acta med rom 1980; 18: 399-440.
2. Cornelissen G, Halberg F. Chronomedicine. In: Armitage P, Colton T, editors. Encyclopedia of Biostatistics, 2nd ed. Chichester, UK: John Wiley & Sons Ltd; 2005. p. 796-812.
3. Refinetti R, Cornelissen G, Halberg F. Procedures for numerical analysis of circadian rhythms. Biological Rhythm Research 2007; 38 (4): 275-325. http://dx.doi. org/10.1080/09291010600903692.
4. Marquardt DW. An algorithm for least-squares estimation of nonlinear parameters. J Soc Indust Appl Math 1963; 11: 431-441.
5. Emens JS, Lewy AJ, Lefler BJ, Sack RL. Relative coordination to unknown "weak Zeitgebers" in free-running blind individuals. J Biol Rhythms 2005; 20: 159-167.
6. Halberg Franz, Cornelissen G, Katinas G, Syutkina EV, Sothern RB, Zaslavskaya R, Halberg Francine, Watanabe Y, Schwartzkopff O, Otsuka K, Tarquini R, Perfetto P, Siegelova J. Transdisciplinary unifying implications of circadian findings in the 1950s. J Circadian Rhythms 2003; 1: 2. 61 pp. www.JCircadianRhythms.com/content/pdf/1740-3391-2-3.pdf
7. Halberg F, Cornelissen G, Otsuka K, Katinas G, Schwartzkopff O. Essays on chronomics spawned by transdisciplinary chronobiology: Witness in time: Earl Elmer Bakken. Neuroendocrinol Lett 2001; 22: 359-384.
8. Levine H, Halberg F, Taylor D. Circadian rhythms before and after removal of both eyes for bilateral retinoblastoma. Graefes Arch Ophthalmol 1973; 188: 263-280.
9. Halberg F, Cornelissen G, Ilyia E, Cegielski N, Hillman D, Finley J, Thomas F, Kino T, Chrousos GP, McCraty R. Selenosensitivity: half-yearly recurrent adynamia and loss of adrenocortical and vascular synchronization with society. Submitted.
10. Doodson AT. The harmonic development of the tide-generating potential. Proc Roy Soc Lond A 1921; 100: 305-329. See also http://en.wikipedia.org/wiki/Arthur_Thomas_Doodson
11. Halberg F, Cornelissen G, Sonkowsky RP, Lanzoni C, Galvagno A, Montalbini M, Schwartzkopff O. Chrononursing (chronutrics), psychiatry and language. New Trends in Experimental and Clinical Psychiatry 1998; 14: 15-26.
12. Cornelissen G, Halberg F, Siegelova J, Galvagno A. The moon's image in prolonged human isolation. This volume.
13. Halberg F, Cornelissen G, Schwartzkopff O, Bakken EE. Cycles in the biosphere in the service of solar-terrestrial physics? In: Schröder W, ed. Case studies in physics and geophysics. Bremen: Wilfried Schröder/Science Edition, 2006, p. 39-87. [Beiträge zur Geophysik und Kosmischen Physik/Journal for the History of Geophysics and Cosmical Physics, Special issue, 2006/2. ISSN 1615-2824]
14. Halberg F, Cornelissen G, Wilson D, Singh RB, De Meester F, Watanabe Y, Otsuka K, Khalilov E. Chronobiology and chronomics: detecting and applying the cycles of nature. Biologist 2009; 56 (4): 209-214.
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15. Evstafyev V, Mikulecky M Sr. Recent biophysical researches explaining the mechanisms of lunar and solar links to the living matter. Proceedings, Man in his terrestrial and cosmic environment, Upice, Czech Republic, May 18-20, 2010 (abstract).
16. Freund F. Pre-earthquake signals: underlying physical processes. Workshop on Validation of Earthquake Precursors by Satellite, Terrestrial and Other Observations (VESTO), Nishi-Chiba Campus, Chiba University, Japan, March 26-29, 2009.
17. Halberg F, Nelson W, Runge WJ, Schmitt OH, Pitts GC, Tremor J, Reynolds OE. Plans for orbital study of rat biorhythms. Results of interest beyond the Biosatellite program. Space Life Sci 1971; 2: 437-471.
18. Halberg F, Cornelissen G, Sothern RB, Cegielski N, Ilyia E, Siegelova J. Tides and double tides pulling the biosphere. This volume.
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r.HRnHrjSIDLG&Y LFIBDRRT0RIE5 - UN [VERS ITY OF MINNESOTA
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ijnt. l DPirSJ
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Figure 1. Chronobiologic serial section of systolic blood pressure (SBP) in a patient (HS) with delayed sleep phase syndrome (DSPS). © Halberg.
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CHRONOBtOLOGY LABORATORIES - UNIVERSITY OF MINNESOTA
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Figure 2. Chronobiologic serial section of diastolic blood pressure (DBP) in a patient (HS) with delayed sleep phase syndrome (DSPS). © Halberg.
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CHRQNQBIQLQGY LABORATORIES - UNIVERSITY OF HINNFSOTfl
PHASE REF. 1997 1221 ODOO PERI00 24.O0HR INTERVflL 168-00HR START TIME 1S96 0226 0000 N OF DflTR 4576 INCREMENT £4.00Hft END TIME 1999 0710 0000
TIME (DAYSI
AMBULATORY CPfiDlOVASCULAR hCNlTOR]M*i HS (Mr 41TJ HR (BPM1
+5.0CI
Figure 3. Chronobiologic serial section of heart rate (HR) in a patient (HS) with delayed sleep phase syndrome (DSPS). © Halberg.
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11
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Figure 4. Least squares spectrum: all data of systolic (S) and diastolic (D) blood pressure (BP) and heart rate (HR) in a patient (HS) with delayed sleep phase syndrome (DSPS). © Halberg.
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HS (diitji before Imitiucnl)
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Figure 5. Least squares spectrum of HS: pre-treatment data of systolic (S) and diastolic (D) blood pressure (BP) and heart rate (HR). © Halberg.
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US (data after start of light therapy)
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Figure 6. Least squares spectrum of HS: data after start of treatment of systolic (S) and diastolic (D) blood pressure (BP) and heart rate (HR). © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Course of aero phases in a cardiologist (YW) treating his delayed sleep phase syndrome by sheer willpower
Systolic (5) (top) and diastolic (D) (middle] blood pressure (BP) and heart
rate (HR) (bottom]
4H.-1
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Figure 7. Acrophase of YW before, during and after delayed sleep phase syndrome. © Halberg.
101
Delayed sleep phase syndrome (DSPS): YW, 35 y of age in 1988
Before
During
After
14 1,4 ?»
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Figure 8. Dominant 24-h and 12-h components in YW with added 24.7- and 12.9-h components. © Halberg.
NONINVASIVE METHODS IN CARDIOLOGY 2010
Bright l.iRhi Therapy ndromc (US. M, 41 y) *
Span PF<%r A(mrriHt) Pk(%) imp A i rrnnUc.1 1 IK Afbpm} + {95WCI)
:-k:i-n- H\ 14 9.5 5.1 -ZH 26 1&.4 -271
(-2B7.-3Q2) <-!**.-»+) (-2T£-2*3)
Rx (span 1) 20 II I -2*8 ICi 7 1 22 9.4 -257
(.2Sn..3ftS) (.254,-271) (-251,-2*4)
34 114 It "Si -264 ?.u im -2J7
(-25S.-270) (-»7,-271) (-252.J62I
FjfJfanJ) zl ||4 -IS! |4 <+ ■255 J5 L2.7 ■235
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(-226.-J44) RJ1.-255) (-207,-2211)
1 SBP: Syilolii- BP. DHH I Ji.i>.24.l>-[kn^acmpriaie (meajuee of the liming of
overall hi>2i»ulwrs tCVutnng d»y, expeeued in negative degree*, with J6u*i24 noun and 0*- Local rnidru'gtrl); CI: Confidence
Table 2
NanJincaj Estimate of Cincadian md tircawmidian Period? of Blood PrciiUft (BP) and Hean Raw |HR) in Paitmr. with Sletp-Delaytd Phase Syndrome (HS. M, 41 y) Receiving nrijrJii Therapy (H.x)*
Span Systolic BP Disiwlk BP I1R
24h Trial Period [95% Clj 12b rrisl Period 244i Trial Period 195% Ct| I2h Trial Period ['X^l 1) 2Ah Trial Perkd [9S14CI] 12h Trial Period [95% CI|
Retort ft* M.DO [23.M24.l3] 12 OS rn.aiiiti 2J.*v> 03.79,14121 1141 |LI.W,L2J04] 13.98 12.05 [11.99.12.10]
Rx (mui l> 23» I23.S 5.24.051 11.17 rn.93,12.411 IJ.* [».«$.24,071 11.96 111.93, LJjUI] [25.KJ4.LBJ 11.97 [11.9J.L2J02J
kx (tpm2t 123.9424.121 L2.A2 111 tt.12.WI ?4 115 ESJ-WJi-iji lui |l 1.97,12.0!] 24.03 [23.95J4.lll 12.» 111 94.LI.061
Rx (qui 3) 23.94 11.* [IL.M,I3.0E| 23.94 IZ3.7JJ4.iaj 11.47 [1 ] .B9.l2.tHJ 24J03 I23.UJ4.E4I 11.9« [11.92.12*4]
RX' by Monlinew Lewi Square foe Blood Pressure (BP) and Heart Ra*e {HR) of PaiicHi with Sleep-DeJnyed Phase Syndrome (HS, M. 4ly) licfnrr Hrceivine Bright Light Therapy'
r'ix*424|iC Ijte^TttlirrHUJBd - 2i.4h C DcsMKrhroaiied -123 C
A.|4*%cl| period [«%cq
Syndic Bf (mnaHi) 9.28 ■6s.i:.o:j 26.14 l25.Tfl-J6.i9l 3.3« Ifl.WJio)! 12 ?4 [15.24,15.43] J.J3 (QLtU^.251
l>juralLc BP(mmS|g) [Jjoa.ft.97] pSjiSJoJSJ i.22 [U.3i.-1 12.JS [12.25.12.441 2.51 I0M.4.44I
11H i Ik-.ii-. in-iii [s.^j.12 :-■ ;,. 44 124*1.26441 2f; [0.59>jSJ| 12,4] [I3JT,32.54] ^>
C: COflipoKnc; Period (ifihoun); CI: {coBscrvalin) CcafideiKC lnlcrval: NS: NvlSulnlictlly Sik^iriOrK
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NONINVASIVE METHODS IN CARDIOLOGY 2010
INFRADIAN MODULATION OF THE DEVELOPMENT OF HUMAN TRUE WHITE-COAT MESOR-HYPERTENSION
Yoshihiko Watanabe1, Germaine Cornélissen2, Franz Halberg2, Dewayne Hillman2, Bohumil Fiser3, Jiri Dusek3, Pavel Homolka3, Jarmila Siegelova3
^okyo Women's Medical University, Medical Center East, Tokyo, Japan 2Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA 3Masaryk University, Brno, Czech Republic, Corresponding author: Franz Halberg, M.D., Professor of Laboratory Medicine and Pathology, Physiology, Biology, Bioengineering and Oral Medicine, Co-director, Halberg Chronobiology Center, University of Minnesota - Campus Mail Code 8609, 420 Delaware St. S.E. Minneapolis, MN 55455, USA, PHONE +1 (612) 624.6976, FAX +1 (612) 624.9989 E-MAIL halbe001@umn.edu, URL http://www.msi.umn.edu/~halberg/
Running title: MESOR-hypertension: strain test,
Support: GM-13981 (FH) and University of Minnesota Supercomputing Institute (GC, FH). Abstract
Objective. To explore any changes in blood pressure (BP) and heart rate (HR) with age by chronobiologically interpreted (C-) ambulatory blood pressure monitoring (ABPM) for a continuous electronically implemented self-surveillance. C-ABPM is now a cost-effective alternative to spotcheck BP measurements in office visits and to spotchecks (sic, because of day-to-day variability) by 24-hour ABPM; the latter is not only limited to a single circadian cycle but also only to a minuscule fraction of infradian cycles, with periods in months, years and decades as well as days, an endeavor comparable to taking the pulse for a minuscule fraction of a second.
Design. Data from automatic ambulatory instruments collected for 23 years at 30-minute intervals are subjected to a cosine model-based and a complementary stacking-based assessment of results from inferential statistical approaches by the linear-nonlinear cosinor and gliding spectral windows and/or chronobiologic serial sections.
Setting. Everyday clinical practice by a cardiologist (YW).
Results. Circadian and infradian rhythms characterize a busy cardiologist's (YW) systolic (S) and diastolic (D) BP and HR, and infradians are mapped tentatively including components with a period length exceeding the limits of the series' length.
Main findings. The rare opportunity of following the development of human as yet transient insofar as professional work-related MESOR-hypertension, MH, shows that it can differ in three different, each several months-long consecutive records of the same individual. Hence, continued self-surveillance should become routine, unless people who should be treated are not and vice versa, and should be implemented in the population as a whole. Such dense and long around-the-clock records along the age scale covered by YW allow the detection of decadal and tentatively even of transtridecadal and other infradian spectral components. In the development of human MH, a recurrent increase in A with infradian periods preceded the increase in M, as it does only once, with a shorter lag, in laboratory models of MH, in the stroke-prone spontaneously hypertensive Okamoto rat and with a lag of only a few days in the rat's salt and DOCA-induced hypertension.
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Conclusion. A spotcheck evidence-based health care awaits replacement by one based on continued inferential statistical surveillance of the individual. The P-values and 95% confidence intervals that are currently indispensable in publications of research are applicable to the individual, in whose care they are equally indispensable. Moreover, with automatic analyses of data required by self-surveillance, this approach is cost-effectively practical, providing much more information at a much lesser cost.
Introduction
Half-hourly around-the-clock BP and HR values, surveilled over 7 days or preferably over longer spans, are 24-hour synchronized in most time series. Hence, one can fit a 24-hour cosine curve to the data, preferably with the 12.0-hour harmonic, to obtain model-based estimates of the midline-estimating statistic of rhythm, i.e., the MESOR, M; the amplitude, A, and acrophase, cp, measures of the extent of rhythmic change and of its timing, respectively. The data can also be stacked along the 24-hour scale without model-fitting for comparison with time-specified reference values from clinically healthy peers matched by gender and age. Measures of the extent of abnormality, if any, are thus obtained by the hyperbaric (or hypobaric) indices, summarizing BP excess (or deficit). These indices consist of the integrated area between the time-varying prediction limits and any part of the BP curve where the latter lies outside the limit. All endpoints of a given subject can be compared with those of clinically healthy peers of the same gender and age group for a circadian and any broader infradian as well as ultradian (in dense data) chronobiologic assessment, separately of systolic (S) and diastolic (D) BP and of HR. YW, a clinically healthy chrono-cardiologist/scientist, 57 years of age, is in the 23rd year of continued chronobiologically-interpreted automatic half-hourly around-the-clock, ambulatory as well as resting monitoring (C-ABPM) (with relatively few interruptions) of his BP and HR. His father died of renal failure with malignant hypertension associated with a pheochromocytoma at the age of 47 years. At the age of 55 years in an about (~) 7.5-month section of his record, YW had by cosine fitting (of a 2- component model, consisting of cosine curves with periods of 24 and 12 hours) and by stacking, both compared with reference standards of clinically healthy peers matched by gender and age, a complete (model-based and non-model-based) SBP-MESOR (M)-hypertension (S-MH) and an incomplete (model-based, but not stacking-derived) DBPM-hypertension, D-MH. In an immediately following ~5-month record at the age of 56 years, he has incomplete (only model-based) S-MH and DBP MESOR-normotension, MN (D-MN) (1).
Months-long records in everyday life can differ as a function of professional and other loads. For YW, this assumption is in keeping with the finding that, during 4 days of vacation at home away from work, there is complete S-MN and D-MN, due to a statistically significant lowering of the BP-M and only a slight numeric increase in the hyperbaric index of DBP. Thus, the monitoring during as well as before and after a vacation constituted a professional strain test. His varying complete vs. incomplete (both model-based and stacking-derived vs. only model-based) S-MH or his incomplete (only model-based) vs. absent D-MH can be interpreted as an occupational MESOR-hypertension. We are dealing with a reversible D-MH that can be readily "treated", e.g., that is eliminated by a change in routine.
Method
YW wears an automatic monitor from A&D (Tokyo) around the clock with few interruptions. His summary a year ago (1) serves as a reference standard for the data accumulated in the interim of ~7 months. YW's chronobiologic reference summaries at ages 55 and 56 years include a sphygmochron carried out with both a model-based approach, from the fit of a two-component model (consisting of
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cosine curves with periods of 24 and 12 hours) and one by stacking, both interpreted by comparison with clinically healthy peers matched by gender and age, Figure 1, as done routinely in the project on The Biosphere and the Cosmos, BIOCOS (2).
Results
Figure 1 shows the original data, that involve gaps, a change in the instrumentation used for monitoring, an episode of a delayed sleep phase disorder and trips, among other "noise" (not here identified). Figure 2 stacks the data along an idealized 24-hour scale from the span summarized by the sphygmochron in Figure 3. Thus, the first of the 48 dots in the top row of Figure 2 is the average of all values collected between 00:00-00:30 during ~7 months; the next dot summarizes all data collected between 00:30-01:00, etc. The ~7-month recordings caught a glimpse of an interesting time span when many SBP clock-time mean values are slightly above the time-specified limit of peers matched by gender and age, while, with no exception from 48 clocktime mean values, the DBPs are near but just below or at the upper 95% prediction limit, but none exceeds that limit.
The diagnosis made 2 years earlier at age 55 differed from that in the sphygmochron in Figure 3 at age 57, inferentially statistically but hardly clinically. At age 55, it was a complete (model- and stacking -based) systolic MH (S-MH) and an incomplete (model- but not stacking-based) diastolic MH (D-MH). All abnormality of BP or HR had been absent during 4 vacation days, summarized in Table 1. Moreover, the blood pressure M on Sundays had been lower than on other days of the week, as seen in Figure 4 (cf. summary in Table 2). No diastolic abnormality was found in the last sphygmochron in Figure 3. A stacking excess during 24 hours above 50 mm Hg x h, as found for SBP, is not acceptable. Thus, the diagnosis of 2008 changed by early 2009 to an incomplete model-based but not stacking-based S-MH and (complete) DBP MESOR-normotension, while in 2010, it is now a complete S-MH with complete diastolic MESOR-normotension.
In this case at this time a systolic abnormality occurred in the absence of the previous but not lasting diastolic MESOR-hypertension. Thus, parameters of consecutive spans, each of at least 5 months, reveal statistically significant differences. The desirability to assess and compare diagnoses with their uncertainties in inferential statistical terms cannot be overemphasized, yet a statistically significant difference in itself does not imply clinical or scientific signification (3, 4), notably if we realize that we are modulated by our cosmos.
The main findings on infradians can account for the foregoing differences; they are summarized in the variabilities of over 231,277 measurements/variable analyzed in two preliminary steps by serial sections, involving the fit of a 24-hour period in Figure 5 and that of a 7-day (168-hour) cosine in Figure 6. Infradians are apparent to the naked eye, which, however, is unable to assess the periods involved (and their uncertainties) or the extent to which they may contribute to the changing diagnoses in the development of MH and in its course. The data are dense with few gaps as seen in Figure 1. In the top rows of Figures 5 and 6, for each variable the lower curve is the MESOR, M, a midline-estimating statistic of rhythm, and the distance from this to a dot below is the standard error (SE) of M. The distance between the two curves in the top row is the amplitude, A, and the distance from the upper curve to the dot above it is the SE of A. The second rows show acrophases, §, of the cosine curve best fitting the data; dots above and below the <|) bracket 95% confidence intervals of §, which is doubly plotted whenever it approaches midnight, i.e., 0° or 360°. The acrophases are reasonably consistent for both the circadian and the circaseptan component.
The bottom rows of each section of Figures 5 and 6 are the results of the tests of the "no-rhythm", i.e., zero (circadian or circaseptan) amplitude assumption, and are overwhelmingly below the dashed horizontal line representing the 5% level of significance. The rhythms can be demonstrated, most of the
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NONINVASIVE METHODS IN CARDIOLOGY 2010
time at or below the 1% level, but with the weekly intervals used in Figure 5 only with interruptions, with fewer interruptions when much longer intervals are used, as in Figure 6 for the fit of the 1-week cosine. Figures 5 and 6 suffice to discern modulations of both M and A but for an estimate of the periods involved, and certainly for the uncertainty of the periods. Figures 5 and 6 are imputations leading to Table 3 and Figures 7 and 8.
Figures 7 and 8 and Table 3 show some of the infradian modulations of the M and the A for systolic and diastolic blood pressure. The M is modulated for both blood pressures by a circadecadal component and, in addition, tentatively, in the case of diastolic blood pressure, by a transtridecadal component, the latter qualified by the relative brevity of the series. The A of each variable shows a circaseptennian modulation and, in addition, a didecadal component for systolic and atentative transtridecadal component for diastolic blood pressure with the uncertainties and double amplitudes of some of the periodic components given in Table 3. Both Figures 7 and 8 reveal more than one circadian double amplitude increase in a clinically healthy subject with a positive family history of vascular disease. Whether these amplitude increases are harbingers of a vascular variability disorder, WD, or are physiological will eventually have to be clarified with the study of other longitudinally investigated subjects and in the light of long-term outcomes. YW has tried non-drug approaches, but no drug therapy.
Discussion
From studies consisting of 24-hour spotchecks in the stroke-prone spontaneously MESOR-hypertensive Okamoto rat, it was learned that a circadian A-increase precedes an M-increase (5). This finding was extended to humans with a cross-sectional design (6) with an A-increase preceding an M-increase around an M of -140 mm Hg along a scale of the left ventricular mass index. Cugini et al. (7) found a higher A & M around an M of-120 mm Hg in patients with minimal change retinopathy vs. those without this condition. Table 3 shows that the double amplitude of about (~) 5.34 mm Hg, associated with an ~ 10-year periodicity, is small, yet other periodic components may add to that difference. For diastolic BP, a tentative transtridecadal period has a double A of 11.32 mm Hg, sufficient to account for the difference between the diagnosis of an acceptable double amplitude vs. CHAT, circadian hyper-amplitude-tension (8). Likewise, the infradian modulation of the diastolic blood pressure MESOR can, at critical MESORs, account for the difference between MH and MESOR-normotension. There is an opportunity in YWs data and in other longitudinal records to account for both circadian and infradian variability in following the development of MH or CHAT, lessons learned in Figures 7 and 8 and Table 3.
Further analyses in others'time series, covering decades, may answer the question about the degree of generality with which a deviation (e.g., an elevation) in A alone or concomitantly with M (7) or in M alone leads to MH or CHAT (8). Consecutive sphygmochrons to pursue in more detail the development of a VVD remain to be computed. In the laboratory, the sequence of a 2A elevation preceding an elevation of M also occurs for BP and other telemetered variables, albeit with a lag of only a very few days, in the saline and desoxycorticosterone-induced hypertension of the rat (unpublished studies by John Osborn), mimicking findings in the spontaneously-hypertensive stroke-prone rat (SHR-SP)
(5) . Likewise, a higher BP-A is associated with intermediate values of the left ventricular mass index (ĽVMI), whereas a higher BP-M (above 140 mmHg) is seen only for larger LVMI values in humans
(6) . This chronobiologic pre-hypertension around an M of 140 mm Hg and the finding of an increase in both 2A and M around a SBP-M of 120 mmHg associated with minimal change retinopathy, discovered by Pietro Cugini and interpreted by him as constituting a pre-hypertension (7, 8) can be reconciled by the operation of genetically anchored infradians. Similarly, pre-diabetes has been documented by focus upon the detection of circadian VVDs (9, 10). More than single subjects will
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have to be longitudinally investigated by systematic monitoring as newborns (2, 3) and at school age to explore any sequences in the development of incomplete to complete S-MH and D-MH, started in adulthood, now in the perspective of decades in YW.
The removal of the load of professional activity can normalize BP in certain individuals: this should be explored further with replications in YW's vacations and work-free Sundays as contrasted to workdays in YW and other individuals. We here present evidence that an ~30-40-year Briickner-Egeson-Lockyer (BEL) transtridecadal cycle (11) and a ~21-year Hale cycle in the bipolarity of sunspots are mirrored in YW's circulation as noted earlier for 3 of 3 others examined (11), one MESOR-normotensive, the other two MESOR-hypertensive, one of them with complicating CHAT. There is also evidence in YW's son FW of an ~5-month cycle in his SBP, putatively related to solar flares, as he aged from 8 to 17 years (12).
The frequency and sequence of alternations between incomplete or complete D-MH and/or S-MH probably also depend on factors like pain (JF has a history of lumbago), grief or conflict during the daily routine, problems to be explored with diaries in decades-long time series like that ofYW. It will be interesting to find out from the entire 23-year and still accumulating record whether professional loads are associated with differences not only in circadian summaries but also in certain infradian cycles'A and/or cp (e.g., by comparing infradian characteristics at certain frequencies from data collected only during weekdays vs. only from weekends and holidays). Also to be further explored is the sequence, if any, in which SBP vs. DBP stacking-based endpoints, such as the hyperbaric index (HBI), change, by comparison to changes in their A, cp and M, if they do not alter concomitantly, as seems to have been the case for YW. The exploration of sequences in which the foregoing changes occur in any longitudinal records of others collected systematically with diaries depends on the development of affordable, unobtrusive instrumentation for continuous automatic BP and HR monitoring.
Conclusion
In current practice, under the assumption of homeostasis, it may appear that diagnoses based on monitoring spans of 5 or more months are superfluous and the 24-hour profile is the platinum standard. Pre-hypertension is conventionally defined as a systolic pressure of 120 mm Hg or higher. As earlier (5-8), others and we here describe pre-hypertension as increases in circadian double amplitude that can (and do in YW) undergo infradian variations in their own right, for years, before an increase in M occurs. We must not fly blind (13) to a cosmically influenced physiology when "seeing" may enter the state of the art in terms of both affordable, unobtrusive hardware and software on a website for automatic analysis (14, 15). Support: GM-13981 (FH), University of Minnesota Supercomputing Institute (GC, FH), MSM0021622402
REFERENCES
1. Watanabe Y, Cornélissen G, Beaty L, Fiser B, Dusek J, Homolka P, Halberg F. White-coat hypertension in a cardiologist: decades of monitoring lead to transient occupational MESOR-hypertension absent during vacation: strain test. In: Halberg F, Kenner T, Fiser B, Siegelova J, eds. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, July 7-10, 2009. (Dedicated to the 90th Anniversary of Prof. Franz Halberg.) p. 226-246. http://web.fnusa.cz/files/ kfdr2009/sbornik_2009.pdf
2. Halberg F, Cornélissen G, Otsuka K, Watanabe Y, Katinas GS, Burioka N, Delyukov A, Gorgo Y, Zhao ZY, Weydahl A, Sothern RB, Siegelova J, Fiser B, Dusek J, Syutkina EV, Perfetto F, Tarquini R, Singh RB, Rhees B, Lofstrom D, Lofstrom P, Johnson PWC, Schwartzkopff O, International
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BIOCOS Study Group. Cross-spectrally coherent -10.5- and 21-year biological and physical cycles, magnetic storms and myocardial infarctions. Neuroendocrinol Lett 2000; 21: 233-258.
3. Halberg F, Cornelissen G, Bakken E. Caregiving merged with chronobiologic outcome assessment, research and education in health maintenance organizations (HMOs). Progress in Clinical and Biological Research 1990; 341B: 491-549.
4. Cornelissen G, Bingham C, Siegelova J, Fiser B, Dusek J, Prikryl P, Sonkowsky RP, Halberg F. Cardiovascular disease risk monitoring in the light of chronobioethics. Chronobiologia 1994; 21: 321-325.
5. Halberg J, Halberg E, Hayes DK, Smith RD, Halberg F, Delea CS, Danielson RS, Bartter FC. Schedule shifts, life quality and quantity modeled by murine blood pressure elevation and arthropod lifespan. Int J Chronobiol 1980; 7: 17-64.
6. Kumagai Y, Shiga T, Sunaga K, Cornelissen G, Ebihara A, Halberg F. Usefulness of circadian amplitude of blood pressure in predicting hypertensive cardiac involvement. Chronobiologia 1992; 19: 43-58.
7. Cugini P, Cruciani F, Turri M, Regine F, Gherardi F, Petrangeli CM, Gabrieli CB. 'Minimal-change hypertensive retinopathy' and 'arterial pre-hypertension', illustrated via ambulatory blood-pressure monitoring in putatively normotensive subjects. International Ophthalmology 1999; 22(3): 145-149.
8. Cornelissen G, Halberg F, Beaty L, Kumagai Y, Halberg E, Halberg J, Lee J, Schwartzkopff O, Otsuka K. Cugini's syndrome in statu nascendi: Oratio contra morem prevalentem et pro chronobiologica ratione ad pressione sanguinis curandam. La Clinica Terapeutica 2009; 160 (2): el3-e24.
9. Sanchez de la Pena S, Gonzalez C, Cornelissen G, Halberg F. Blood pressure (BP), heart rate (HR) and non-insulin-dependent diabetes mellitus (NIDDM) chronobiology. Abstract S8-06, 3rd Int Congress on Cardiovascular Disease, Taipei, Taiwan, 26-28 Nov 2004. Int J Cardiol 2004; 97 (Suppl 2): S14.
10. Gupta AK, Greenway FL, Cornelissen G, Pan W, Halberg F. Prediabetes is associated with abnormal circadian blood pressure variability. J Human Hypertension 2008; 22: 627-633. doi:10:1038/jhh.2008.32.
11. Halberg F, Cornelissen G, Sothern RB, Czaplicki J, Schwartzkopff O. 35-year climate cycle in heliogeophysics, psychophysiology, military politics, and economics. Geophysical Processes and Biosphere 2009; 8 (2): 13-42. [In Russian with English summary; English translation of paper forthcoming.]
12. Watanabe F, Cornelissen G, Watanabe Y, Halberg F. A far-transyear in the blood pressure of a 17-year-old male. Proceedings, Noninvasive Methods in Cardiology, Brno, Czech Republic, 2010, in preparation.
13. Fossel M. Editor's Note (to Halberg F et al. Circadian Hyper-Amplitude-Tension, CHAT: a disease risk syndrome of anti-aging medicine. J Anti-Aging Med 1998; 1: 239-259.) J Anti-Aging Med 1998; 1: 239.
14. Halberg F, Cornelissen G, Otsuka K, Siegelova J, Fiser B, Dusek J, Homolka P, Sanchez de la Pena S, Singh RB, BIOCOS project. Extended consensus on means and need to detect vascular variability disorders (VVDs) and vascular variability syndromes (VVSs). Leibniz-Online Nr. 5, 2009 (http://www2.hu-berlin.de/leibniz-sozietaet/journal/archiv_5_09.html). 35 pp.
15. Halberg F, Cornelissen G, Otsuka K, Siegelova J, Fiser B, Dusek J, Homolka P, Sanchez de la Pena S, Singh RB, BIOCOS project. Extended consensus on need and means to detect vascular variability disorders (VVDs) and vascular variability syndromes (VVSs). Geronto-Geriatrics: Int J Gerontology-ChronomeGeriatrics 2008; 11 (14): 119-146.
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Table 1: Comparison of 3 vascular profiles: 1 and 2 based on months of monitoring; 3 based on weekends and holidays
Systolic Blood Pressure (mm Hg)
i Span MESOR 24h-A 2411-0 (A4)
j 1. Jan-Aug 2008 142.6 11.76 -246
1 2. Aug 08-Jan 09 140.1 13.56 -251
! 3. Holiday (2008-09) 132.1 12.54 -226
I 1 vs. 2 vs. 3
1 F 32.174 0.440 4.598 2.501
I P <0.001 0.645 0.012 0.045
1 1 vs. 2
! F 4.247 1.029 0.392 0.708
i P 0.042 0.313 0.533 0.495
1 2 vs. 3
i F 29.504 0.246 7.073 3.886
! P <0.001 0.621 0.009 0.024
Diastolic Blood Pressure (mm Hg)
I Span MESOR 24h-A 2411-0 (A.O)
j 1. Jan-Aug 2008 87.3 5.94 -236
i 2. Aug 08-Jan 09 86.9 8.11 -242
1 3. Holiday (2008-09) 81.9 9.08 -226
i 1 vs. 2 vs. 3
! F 13.248 1.896 1.129 1.457
i P <0.001 0.154 0.327 0.219
! lvs. 2
! F 0.324 5.029 0.618 2.827
! P 0.571 0.027 0.434 0.065
! 2 vs. 3
! F 13.581 0.254 1.740 0.949
1 P 0.001 0.616 0.192 0.391
Heart Rate (beats/min)
i Span MESOR 24h-A 2411-0 (A4)
j 1. Jan-Aug 2008 74.9 4.92 -246
1 2. Aug 08-Jan 09 75.8 5.28 -253
! 3. Holiday (2008-09) 69.6 7.95 -253
I 1 vs. 2 vs. 3
1 F 21.029 2.543 0.146 1.355
1 P <0.001 0.082 0.865 0.253
1 lvs. 2
i F 0.785 0.053 0.187 0.120
! P 0.378 0.819 0.667 0.887
1 2 vs. 3
i F 37.279 3.392 0.001 1.697
! P <0.001 0.069 0.975 0.189
A: Amplitude; <\>: Acrophase, expressed in (negative) degrees, with 360° = 24 hours, 0° = 00:00. Results from parameter tests (Bingham C, Arbogast B, Cornelissen Guillaume G, Lee JK, Halberg F. Inferential statistical methods for estimating and comparing cosinor parameters. Chronobiologia 1982; 9: 397-439). For this time-microscopic assessment, the data during the 4 days of vacation in span 3 were removed from span 2 prior to analysis.
no
Table 2: Comparison of vascular endpoints on Sundays with weekdays reveals acceptability of blood pressure (BP) on Sundays by contrast to weekdays in YW, a physician-scientist
Sphygmos SBP-M DBP-M HR-M SBP-2A DBP-2A HR-2A S-HBI D-HBI TCI
1. Sun 132.9 83.0 72.2 20.03 9.10 10.30 5 1 0
2. Mon 138.8 86.9 74.2 28.15 19.86 11.25 53 11 0
3. Tue 140.9 88.2 76.2 29.58 18.05 14.23 70 12 0
4. Wed 138.6 86.2 75.0 28.33 18.33 10.46 51 9 0
5.Thu 141.4 88.3 75.2 22.85 10.78 8.07 80 6 0
6. Fri 143.0 88.4 77.0 27.52 17.70 8.84 80 5 0
7. Sat 141.0 85.6 78.5 30.86 19.30 16.17 57 5 0
*S: systolic; D: diastolic; BP: blood pressure; M: MESOR, a midline-estimating statistic of rhythm; 2A: double circadian amplitude, HR: heart rate; HBI: hyperbaric index; TCI: tachycardic index. A lower value on Sundays for BP was also found for 30 series from 25 individuals, when the data of each subject were expressed as a percentage of their mean values, examined as a group by a one-way analysis of variance: the lower MESOR was statistically significant for DBP below the 5% and for SBP below the 10% level. In the same 30 series, the 2A of HR was higher on Sundays and Saturdays than on other days of the week (P<0.05).
NONINVASIVE METHODS IN CARDIOLOGY 2010
Figure 1. Plot of original measurements of YW, M, 57 years of age. Data between + and -2 standard deviations from the mean are plotted linearly within the proximal horizontal lines. Beyond these lines, in lesser intervals between the proximal and distal upper and lower borders, data are compressed for an exponential approximation of the upper and lower extremes representing + or - infinity. Location: 3 SD at -5/8, and 4 SD at -7/8 of strip width. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Circad^art patterns of YW. M. 57 /ears of age. from January IG-August 15. Z01D: Hatf-hourly averages slacked along an Idealized 24-h scale
C.Tjrt4.r.Ptri-ySBP e*t«**h haw* at »p Cit**"'inr"*i'Hn
Figure 2. Summary by stacking of half-hourly around-the-clock means along an idealized 24-hour day at age 57 years for blood pressure (BP) and heart rate (HR) during regular professional life. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
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Figure 3. Sphygmochron of mostly half-hourly around-the-clock data, stacked and averaged for 48 consecutive (half-hourly) bins of an idealized 24-hour day, for a man (YW) in everyday professional life as a cardiologist at age 57 years. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Sundays1 Systolic (5) and Diastolic (D) MESOR-Normotension (NM); Occupational S-MESOR-Hypertension (MH) on Workdays1
SBP (mmHg) DBP (mmHg) HR (beats/min)
Time (clock hours)
' YYV iW *>) rnormwod S and 0 bbod pressure (BP) and hearl rate |HR| ai 30mm itmpr.* Aug ZD08 - Jtn »09 (rl*4.11Sr.
Figure 4. Weekend blood pressures and heart rates differ from those on weekdays. See also Tables 1 and 2. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Orcadian rhythm characteristics of systolic (5) and diastolic (D) blood pressure [BP} and heart rate (HR) of YW, M, 57 years of age, during 23
years*
01
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Figure 5. Chronobiologic serial sections of YW's systolic (A) and diastolic (B) blood pressure and heart rate with the fit of a 24-h cosine curve to consecutive intervals of 1 week, displaced in 48-hour intervals. © Halberg.
116
86
Chronobiologic serial sections resolve about-weekly rhythm of YW, M,
August 26,1987-August 15, 2010*
Blood pressure
Heart rate
Systolic
Diastolic
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'Period fitted: 1 week; interval: 40 weeks; increment: 1 week. Phase reference: 19870101.
Figure 6. Chronobiologic serial sections of YW's systolic (A) and diastolic (B) blood pressure and heart rate with the fit of a 1-week cosine curve to 280-day intervals displaced in 1-week increments. © Halberg.
DEVELOPMENT OF TRUE "WHITE COAT HYPERTENSION" *, MODULATED BY COSMOS, IN THE SYSTOLIC BLOOD PRESSURE OF YW, PHYSICIAN, 57 YEARS OF AGE
o
Joint Nonlinear Fit of a 10.25 year Cosine added to a Cubic Curve
Joint Nonlinear Fit of Cosine Curves of 19.36 and 7.61 year Periods
1987/8/26
1993/5/23 1999/2/19 TIME (Calendar Date)
2004/11/16 2010/8/15
'WHILE SEEING PATIENTS
Figure 7. Infradian fit by linear-nonlinear cosinor of MESOR (top curve) and circadian amplitude (bottom curve) of systolic blood pressure of YW. A decadal modulation of the MESOR (top curve) coexists with a didecadal and circaseptennian modulation of the double circadian amplitude (bottom curve). © Halberg.
DEVELOPMENT OF TRUE "WHITE COAT HYPERTENSION" *, MODULATED BY COSMOS, IN THE DIASTOLIC BLOOD PRESSURE OF YW, 57 YEARS OF AGE
Joint Nonlinear Fit of Cosine » Curves of 34.8 and 9.4 year \ A(Sj^^^
Joint Nonlinear Fit of Cosine Curves of 31.8 and 7.9 yea
' \> sriods
1987/8 26
1993/5/23 1999/2/19 2004/11/16 2010/8/15
TIME (Calendar Date) *while seeing patients
Figure 8. Infradian fit by linear-nonlinear cosinor of MESOR (top curve) and circadian amplitude (bottom curve) of diastolic blood pressure of YW. A transtridecadal component modulates both the MESOR and the double amplitude in addition to a decadal component in the case of the MESOR and a circaseptennian component for the double circadian amplitude. © Halberg.
NONINVASIVE METHODS IN CARDIOLOGY 2010
COMPLEMENTARY YET DIFFERING RHYTHMIC ASPECTS OF A MAN'S MOOD AND VIGOR IN VARIOUS SPECTRAL REGIONS
Robert B. Sothern12, Franz Halberg2, Germaine Cornelissen2, Dewayne Hillman2, George Katinas2, Jarmila Siegelova3
1 The Rhythmometry Lab, Dept of Plant Biology, University of Minnesota, St. Paul, MN, USA 2 Halberg Chronobiology Center, University of Minnesota, Minneapolis, MN, USA. 3 Masaryk University, Brno, Czech Republic
Abstract. Using the most recent subspan of 8 months from a more than 4-decade-long self-measurement project, we report a statistically significant difference in the circadian phase of mood (M) and vigor (V) self-rated by a clinically healthy man (RBS, age 62y) about 6 times a day, mostly between awakening and bedtime. Analyses involving 24-hour cosine fitting confirm statistically significant circadian rhythms in each variable and quantify the subject's awareness that his vigor peaked during mid-activity (acrophase, <|) = 15:42), while his mood peaked late in the evening = 00:16). Oral temperature (OT) measured simultaneously verified synchronization to his sleep-wake schedule (<|) = 16:34). Chronobiologic serial sections confirmed the stability of each variable's circadian acrophase over the 8-month span. Additional cosinor analyses for periods up to 30 days revealed statistically significant periodicities between 12 and 16 days in V, but no circaseptan rhythm, while M showed periodicities between 11.5 and 19.0 days, plus a 27.5-day cycle and a possible free-running circaseptan component with a period of 6.5 days. Gliding spectral windows between 0.7 and 2.5 years showed further infradian differences between M and V that can be compared with the infradian time course of OT during the entire four decades of monitoring. Differences in circadian timing, and changing amplitudes and drifting infradian frequencies in M and V describe diverse rhythmic patterns in subjective assessments of what superficially seem to be interdigitated aspects of psychology.
Background. By separating positive from negative affect with their PANAS scale (1), Watson, Clark and Tellegen enabled the demonstration of a prominent about 7-day (circaseptan) cycle in negative affect (NA) versus a 24-hour (circadian) prominence in positive affect (PA) in 196 clinically healthy subjects (2). The circaseptan amplitude was larger than the circadian amplitude for NA, whereas the circadian amplitude was larger for PA. The broader spectrum of rhythms includes a circadecadal modulation, i.e., an about 11.5-year variation (3) in a 30-year-long record of M and V self-ratings carried out on average about 5 to 6 times a day with only a few interruptions by the same subject (RBS) of this current report. Information on the time structure of M provides endpoints to be considered in any attempt to optimize psychological well-being by making sleeping, dietary, and/or other lifestyle adjustments. The 8-month series of M and V self-ratings examined herein by chronobiologic analyses served as clinically healthy control data for a magneto-labile family who self-monitored over the same time span that covered 8 lunar cycles.
Subject. A healthy male biomedical scientist (RBS), age 62y at the start of the current 8-month self-ratings span, used a slightly modified version of 7-point scales proposed in 1972 (4) for M and V (summarized in Table 1), although in actuality he only rated V between 1-5. Self-rating on each M and V rating scale separately (3) has its justification, as documented herein, in assessing different aspects of psychology.
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Table 1: Mood and Vigor Ratings modified from (4) used by RBS
Mood Physical Vigor
Very depressed, „blue" 1 Very tired, very sleepy, no energy
Somewhat depressed, „down" 2 Somewhat tired, sleepy, inactive
Slightly less cheerful than usual 3 Slightly less active than usual
Usual state, „average mood" 4 Usual state, „average vigor"
Slightly more cheerful than usual 5 Slightly more active than usual
Quite cheerful, feel good 6 Quite active, full of pep
Super cheerful, happy 7 Super active, „hyper"
The subject performed 1,450 self-measurements between Mar 7 and Nov 4, 2009. After removal of 84 values during 2 weeks with an upper respiratory infection in March, the remaining „healthy" M, V and OT data (N = 1,366) were analyzed for rhythm characteristics by the least-squares fit of cosines between 24 hours and 30 days, which included a precise 7-day (168-hour) fit (4). Serial sections (4) with 7-day intervals were then used for the fit of a 24-hour cosine, and intervals covering 6 or 12 weeks for the fit of a 168-hour cosine. The intervals used for analysis were advanced through the time series to derive moving estimates of amplitudes, acrophases, statistical significance and percentage rhythm (coefficient of determination) of the components investigated.
Results. A highly significant circadian rhythm (P<0.001) was found in each variable measured by RBS, with acrophases (0) located at night for M (00:16) and during the day for V (15:42) and OT (16:34) (Figure 1). The fit of a 7-day cosine did not reach statistical significance for M (P = 0.160), V (P = 0.136) or OT (P = 0.541). When looking at rhythm stability over the 8-month time span, chronobiologic serial sections show a particularly tight circadian acrophase in the early afternoon for V (row 3 of Figure 2), in keeping with a consistent statistically highly significant rejection of the zero-amplitude assumption in row 4 in which all P-values are well below the dashed horizontal line marking P=0.05 (arrow). In row 2 of Figure 2, the lower curve represents the rhythm-adjusted mean (MESOR) and dots below it its standard error, while the distance between the two curves represents the amplitude and dots above the upper curve represent its standard error. The 95% confidence intervals of the acrophase bracket the dark row of acrophases and show a more or less horizontal (stable) circadian timing even though the MESOR and amplitude exhibit infradian modulations. The fit of a 168-hour cosine curve to the same data set for V (not shown) do not allow the consistent demonstration of circaseptan rhythmicity.
In turning to Figure 3, a 24-hour-synchronized circadian rhythm is demonstrated more often than not in M, as apparent from the fourth row of P-values (P<0.05 mostly). Row 2 of Figure 3 shows that the infradian modulation of both the circadian MESOR and amplitude of M is much more pronounced than that of V, and its acrophases hovering around midnight are clearly different from the time course in early afternoon of the acrophases for V. From the fit of a 7-day cosine (Figure 3, rows 5 and 6), for parts of its time course, the circaseptan phase for M (row 6), at the start and particularly at the end of the record, is outwardly advancing, and thus not synchronized with the societal week, suggesting a shorter than 7-day period. Indeed, the period of the best-fitting cosine in the circaseptan region was 6.5 days (PO.001) compared with P = 0.160 for a 7-day cosine. RBS, the subject uniquely self-investigated, apparently can show a 24-hour-synchronized cycle in M in the presence of a 7-day socially-desynchronized cycle in M. The circaseptan component, however, was the third most prominent in a list of several candidate infradian periods up to 30 days that were detected for M, which includes (in order of prominence): 16.5, 19.0, 6.5, 27.5, 11.5 and 14.0 days, all of which were significant at P<0.001 (P-values not corrected for multiple testing). No infradian components were found in OT, but several candidate periods were found for V, including 14.0 days (P=0.005), 16.0
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days (P=0.023) and 12.0 days (P=0.046). Of note, results from 7 months of data collected in 1971 by this same subject when he was 24 years of age found a statistically significant 16.0-day component in M and a 7.0-day periodicity in V, but no infradians in OT (5).
Using previously published findings, further differences between M and V, also versus OT, in the spectral region extending from 0.7 to 2.5 years can be seen in a gliding spectrum (6) in Figure 4 for the same subject, in whom, among others (7), an about 33-year transtridecadal cycle was also demonstrated for his heart rate (8) and in data collected at certain times of day for his estimation of 1 minute (9).
Discussion. Without extrapolating beyond the scope of a single subject, the extensive data herein analyzed in the circadian and infradian regions, covering 8 months and nearly 8 lunar cycles, each from one full moon to the next full moon as indicated by vertical dashed lines in Figures 1 and 2, are presented as control information for other data from subjects presumably sensitive to the moon. The data in the para-annual region of the spectrum of 3 variables studied in Figure 4 over 4 decades also show differences in time structure. In the case of M, all results in Figures 1-4 could possibly benefit further from a separation of positive from negative affect (1,2).
Conclusion. The inclusion of a simple-to-perform and fast mood and vigor self-rating separately throughout the day is recommended for the study of individuals' and groups' behavior over time, whereby circadian and other rhythm characteristics can be consistently assessed by cosinor, including chronobiologic serial sections (4) and gliding spectra (5). The data in hand warrant the construction of a device in which all self-ratings could be recorded in a form electronically downloadable to a computer.
REFERENCES
1. Watson D, Clark LA, Tellegen A. Development and validation of brief measures of positive and negative affect: the PANAS scales. J Person Soc Psychol 1988; 54: 1063-1070.
2. Cornelissen G, Watson D, Mitsutake G, Fiser B, Siegelova J, Dusek J, Vohlidalova L, Svacinova H, Halberg F. Mapping of circaseptan and circadian changes in mood. Scripta Medica 2005; 78: 89-98.
3. Halberg F, Cornelissen G, Otsuka K, Watanabe Y, Katinas GS, Burioka N, Delyukov A, Gorgo Y, Zhao ZY, Weydahl A, Sothern RB, Siegelova J, Fiser B, Dusek J, Syutkina EV, Perfetto F, Tarquini R, Singh RB, Rhees B, Lofstrom D, Lofstrom P, Johnson PWC, Schwartzkopff O, International BIOCOS Study Group. Cross-spectrally coherent -10.5- and 21-year biological and physical cycles, magnetic storms and myocardial infarctions. Neuroendocrinol Lett 2000; 21: 233-258.
4. Halberg F, Johnson EA, Nelson W, Runge W, Sothern R. Autorhythmometry ~ procedures for physiologic self-measurements and their analysis. Physiol Teach 1972; 1: 1-11.
5. Sothern RB. Low frequency rhythms in the beard growth of a man. In: Chronobiology. Scheving LE, Halberg F, Pauly JE (Eds.) Tokyo: Igaku Shoin Ltd, 1974, pp. 241-244.
6. Nintcheu-Fata S, Katinas G, Halberg F, Cornelissen G, Tolstykh V, Michael HN, Otsuka K, Schwartzkopff O, Bakken E. Chronomics of tree rings for chronoastrobiology and beyond. Biomed Pharmacother 2003; 57 (Suppl 1): 24s-30s.
7. Sothern RB, Halberg F. Longitudinal human multifrequency structure of blood pressure self-measured for over 2 decades. Proc 2nd Ann IEEE Symp Computer-Based Medical Systems, Mpls, MN, June 26-27, 1989. Wash DC: Computer Soc Press, 1989, pp. 288-294.
8. Sothern RB, Katinas GS, Fiser B, Siegelova J, Cornelissen G, Halberg F. A transtridecadal cycle in human heart rate: Selective infradian, notably multidecadal solar-physiologic BEL congruences. In: Halberg F, Kenner T, Fiser B, Siegelova J (Eds.) Proc Noninvasive Methods
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in Cardiology, Brno, Czech Republic, Oct 4-7, 2008, pp. 204-213. http://web.fnusa.cz/files/ kfdr2008/sbornik_2008.pdf 9. Halberg F, Sothern RB, Cornelissen G, Czaplicki J. Chronomics, human time estimation, and aging. Clin Interv Aging 2008; 3 (4): 749-760.
Support. GM-13981 (FFT) and University of Minnesota Supercomputing Institute (GC, FIT).
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arcadian Patterns In 3 Variables Self-Measured 5-7 times/day over 8 Months by a Healthy Man (RBS. age 62-3y) *
00 04 08 I2 16 20 00 00 04 08 12 16 20 00 00 04 08 12 16 20 CO
Time (Local dock Hour)
'Data span ■ March 7 - Nov 4,2009; N * 1366; maona oomputad ovar2h apana; Dark bar m avmsge aloapliyg ap&iy
Figure 1. Orcadian patterns show peaks in the afternoon for vigor and oral temperature and in the evening for mood in self-measured data by a clinically-healthy man, Two-hourly means±SE (assigned to midpoint) shown with best-fitting 24-hour cosine. N data per 2 hours, P-value from zero-amplitude (no-rhythm) test and rhythm parameters are listed.
NONINVASIVE METHODS IN CARDIOLOGY 2010
CMKCNOBItlLtMif LAUQtUTClfllbH ' U NEVE: tih MINNHKHTA
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Figure 2. Serial section of 8 months of vigor ratings by RBS showing results from the fit of a 24-hour cosine. Acrophase units: 0° and -360° = 00:00, -90° = 06:00, -180° = 12:00, -270° = 18:00. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
FMIJlHr' KhF. IfUIIU U I II I 1343
1 ,h*. ,1 ,avi.|
Figure 3. Serial section of 8 months of mood ratings by RBS showing results from the fit of a 24-hour cosine in rows 2-4 (see Fig 2 legend for acrophase units) and of a 7-day cosine in rows 5 and 6 (acrophase reference: 0° = Thur, Jan 1 00:00). © Halberg.
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TIME COURSE IN ABOUT 4 DECADES OF FREQUENCY STRUCTURE OH VICTOR .M\ti
KIjv I i i m h- : l 11 v in.: ill hi.' mnn, 21 y old at slitrf uf Mf|f-rahn}j; v un-H M jhuL jm'UMirinK I 5 " times per J^j-r
{■hding sptctrd. computed with inlcn-jkl = 10 y L mcncmcnl ~ 4 months, h-urmn-nic i ei ltl1 in lani M.MS; iirilL-riiiK I'-idlut irzuu ivxi of lepo^amplttudt a»um prion ar li(ihlvst ^hi*di«-g. j» < OrOI, darker *.ha-dinp; forrpspnn^is In larger antplirudt.
Figure 4. Gliding spectral window showing frequency structure of mood (M), vigor (V) and oral temperature (T) investigated in RBS over 40 years. © Halberg.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
NIGHT-TO-DAY BLOOD PRESSURE RATIO DURING SEVEN-DAY AMBULATORY
BLOOD PRESSURE MONITORING
Fišer B., Havelkova A., Siegelová J., Dušek J., Pohanka M., Cornélissen G.*, Halberg F.*
Department of Physiology, Department of Physiotherapy, Department of Functional Diagnostics and Rehabilitation, Faculty of Medicine, Masaryk University, St. Anna Teaching Hospital, Brno, CZ,
*University of Minnesota, USA
Support by grant MSM 0021622402.
From 1988, when O'Brien and colleagues reported that an abnormal circadian blood pressure profile with a less marked decrease in night-time blood pressure led to an increased risk for stroke, the clinical significance of night-to-day blood pressure ratio is known (1). Subsequent studies confirmed the prognostic significance of night-to-day blood pressure ratio for prediction of a higher rate of cardiovascular complications (2-8). One of large-scale studies based on International Database on Ambulatory blood pressure monitoring in relation to Cardiovascular Outcomes was published in 2007 (9). The investigators did 24-hour blood pressure monitoring in 7458 people (mean age 56.8 years) from Denmark, Belgium, Japan, Sweden, Uruguay and China. Median follow-up was 9.6 years. They found that night-to-day ratio of systolic and diastolic blood pressure adjusted for cohort, sex, age, body-mass index, smoking and drinking, serum cholesterol, history of cardiovascular disease, diabetes mellitus, and antihypertensive drug treatment predicted total mortality, non-cardiovascular mortality and cardiovascular mortality. In fully adjusted models night-to-day ratio was additionally adjusted for 24-hour blood pressure. The results for fully adjusted night-to-day ratio were similar except systolic blood pressure and cardiovascular mortality where the hazard ratio 1.08 (0.99- 1.17) was not statistically significant. After the patients were, according the night-to-day ratio, divided in 4 categories with night-to-day ratio >1.0 (reverse dippers), 0.9-1.0 (non-dippers), 0.9-0.8 (dippers) and <0.8 (ultra-dippers), the total mortality was increased in non-dippers and reverse-dippers in comparison to dippers. Cardiovascular mortality was significantly increased in reverse dippers, as well as incidence of all cardiovascular events.
Although the prognostic significance of night-to-day blood pressure ratio was proved in a large group of patients, the clinical significance of this value depends on variation of repeated measurement in individual patients.
The evaluation of night-to-day blood pressure variability during 7 days of ambulatory blood pressure measurement was the aim of the present study.
Methods
Thirty subjects (18 males, 12 females), twenty one years to seventy three years old, were recruited for seven-day blood pressure monitoring. Colin Medical Instruments (Komaki, Japan) were used for ambulatory blood pressure monitoring (oscillation method, 30-minute interval between measurements) (10). One-hour means of systolic and diastolic blood pressure were evaluated, when night-time was considered from midnight to 0600 h and day time from 1000 to 2200 h, avoiding the transitional periods. Mean day-time and mean night-time systolic and diastolic pressures were evaluated every day (11). Dipper status was evaluated every day. Dippers were defined as those individuals with a 10-20 % fall in nocturnal blood pressure. Non-dipping was defined as a less than 10 % nocturnal fall, and those with no fall in blood pressure were defined as reverse-dippers (12).
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Results
The patients were ordered according mean 7-day SBP (patient No 1: 107 mmHg, patient No 30: 131 mmHg; median value: 123 mmHg).
Variability of night-to-day ratio during 7-day monitoring is seen in Fig. 1 for SBP and in Fig. 2 for DBP
Only 4 subjects (13 %) were found which could be classified as SBP dippers or ultra-dippers every day. Most of the subjects were classified on various days differently, even 8 subjects (27 %) were one day classified as ultra-dippers and the other day as reverse-dippers.
Similarly no subject classified as DBP dipper or ultra-dipper every day was found. Four subjects (13 %) were one day classified as ultra-dippers and the other day as reverse-dippers. The day-to-day variability of night-to-day ratio is large. The dipping status classification in individual patient is not reliable.
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Variability of night-to-day SBP ratio during 7-day monitoring. Patients were put to order according mean 7-day SBP (patient No 1: 107 mmHg, patient No 30: 131 mmHg; median value: 123 mmHg). One-day mean values (point) and 7-day mean values (dash) are indicated.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Seven days monitoring DBP night-to-day
1.2 n
Fig. 2
Variability of night-to-day DBP ratio during 7-day monitoring. Patients were ordered according mean 7-day SBP (patient No 1: 107 mmHg, patient No 30: 131 mmHg; median value: 123 mmHg). One-day mean values (point) and 7-day mean values (dash) are indicated.
Discussion
Our finding of large night-day ratio variability in individual subjects corresponds to the results of other studies. The night-to-day blood pressure ratio is subject to regression-to-the mean (13). Dipping status has also a low reproducibility, with up to 40 % of individuals from Europe (14) and Asia (15) changing status between repeat recordings.
In our former study we demonstrated that the relation between night-to-day ratio and risk of cardiovascular events is not linear as it is in the case of mean 24-hour systolic and diastolic pressure (16). We observed at low circadian double amplitude which roughly corresponds to the difference between night and day blood pressure (5 mmHg of systolic and 4 mmHg of diastolic pressure) about 30 % higher incidence of cardiovascular events than at circadian double amplitude of 15 to 35 mmHg systolic and of 12 to 20 mmHg diastolic pressure but at double amplitude higher than 35 mmHg in systolic and 28 mmHg in diastolic pressure the incidence was double. This indicates the existence of overswinging or Circadian Hyper-Amplitude-Tension (CHAT) syndrome which is associated with a large increase in cardiovascular disease risk. The incidence of ultra-dipping is more frequent that the incidence of CHAT but existence of CHAT alone can lead to misdiagnosis of risk based on night-today blood pressure ratio.
In conclusion, despite the low night-to-day ratio of blood pressure predicted increased risk for cardiovascular events in large studies, the determination of this value is useless for management of arterial hypertension in individual patients.
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Summary
The evaluation of night-to-day blood pressure variability during 7 days of ambulatory blood pressure measurement was the aim of the present study. Thirty subj ects (18 males, 12 females), twenty one years to seventy three years old, were recruited for seven-day blood pressure monitoring. Colin Medical Instruments (Komaki, Japan) were used for ambulatory blood pressure monitoring (oscillation method, 30-minute interval between measurements). One-hour means of systolic and diastolic blood pressure were evaluated, when night-time was considered from midnight to 0600 h and day-time from 1000 to 2200 h, avoiding the transitional periods. Mean day-time and mean night-time systolic and diastolic pressures were evaluated every day.
Dipper status was evaluated every day. Dippers were defined as those individuals with a 10-20 % fall in nocturnal blood pressure. Non-dipping was defined as a less than 10 % nocturnal fall, and those with no fall in blood pressure were defined as reverse-dippers.
The day-to-day variability of night-to-day ratio is large. The dipping status classification in individual patients is not reliable.
REFERENCES
1. E O'Brien, J Sheridan and K O'Malley, Dippers and non-dippers, Lancet 332 (1988), p.397.
2. T Ohkubo, A Hozawa and J Yamaguchi et al, Prognostic significance of the nocturnal decline in blood pressure in individuals with and without high 24-h blood pressure: the Ohasama study, JHypertens 20 (2002), pp. 2183-2189.
3. TW Hansen, J Jeppesen, F Rasmussen, H Ibsen and C Torp-Pedersen, Ambulatory blood pressure monitoring and mortality: a population-based study, Hypertension 45 (2005), pp. 499-504.
4. E Ingelsson, K Bjôrklund, L Lind, J Ärnlôv and J Sundstrôm, Diurnal blood pressure pattern and risk of congestive heart failure, JAMA 295 (2006), pp. 2859-2866.
5. G Mancia, R Facchetti, M Bombelli, G Grassi and R Sega, Long-term risk of mortality associated with selective and combined elevation in office, home, and ambulatory blood pressure, Hypertension 47 (2006), pp. 846-853.
6. P Verdecchia, C Porcellati and G Schillaci et al, Ambulatory blood pressure. An independent predictor of prognosis in essential hypertension, Hypertension 24 (1994), pp. 793-801.
7. JA Staessen, L Thijs and R Fagard et al, Predicting cardiovascular risk using conventional vs ambulatory blood pressure in older patients with systolic hypertension, JAMA 282 (1999), pp. 539-546.
8. K Kario, TG Pickering, T Matsuo, S Hoshide, JE Schwartz and K Shimada, Stroke prognosis and abnormal nocturnal blood pressure falls in older hypertensives, Hypertension 38 (2001), pp. 852-857.
9. José Boggia, Yan Li, Lutgarde Thijs et all. Prognostic accuracy of day versus night ambulatory blood pressure: a cohort study. Lancet 370 (2007), p.1219-1229.
10. J. Siegelová, J. Dusek, B. Fiser, P. Homolka, P. Vank, M. Kohzuki, G. Cornellisen, F. Halberg. Relationship between circadian blood pressure variation and age analyzed from 7-day ambulatory monitoring. J Hypertension, 2006, vol. 24, Suppl.6, p. 122.
11. Redón J, Vicente A, Alvarez V et. al. Circadian rhythm variability of arterial pressure: methodological aspects for the measurement. Med Clin, 1999 112:258-289.
12. Jerrard-Dune P, Mahmud A, Feely J. Circadian blood pressure variation: relationship between dipper status and measures of arterial stiffness. J Hypertension 2007, 25: 1233-1239.
13. Staessen, CJ Bulpitt and E O'Brien et al, The diurnal blood pressure profile. A population study, Am JHypertens 5 (1992), pp. 386-392.
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14. S Omboni, G Parati and P Palatini etal., Reproducibility and clinical value of nocturnal hypotension: prospective evidence from the SAMPLE study, JHypertens 16 (1998), pp. 733-738.
15. Y Mochizuki, M Okutani and Y Donfeng etal, Limited reproducibility of circadian variation in blood pressure dippers and nondippers, Am JHypertens 11 (1998), pp. 403-409.
16. Cornelissen G, Delcour A, Toussain G et al. Opportunity of detecting pre-hypertension: world wide data on blood pressure overswinging. Biomedicine and Pharmacotherapy 59 (2005) S152-S157.
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DAY AND NIGHT BLOOD PRESSURE VARIABILITY DURING SEVEN-DAY AMBULATORY BLOOD PRESSURE MONITORING
Siegelová J., Havelkova A., Fišer B., Dušek J., Pohanka M., Mašek, M.*, Dunklerová L.,
Cornélissen G.*, Halberg F.*
Department of Physiology, Department of Physiotherapy, Department of Functional Diagnostics and Rehabilitation, Faculty of Medicine, Masaryk University, St. Anna Teaching Hospital, Brno, CZ,
* University of Minnesota, USA *Department of Traumatic Surgery, Faculty of Medicine, University Hospital Brno Bohunice, Brno CZ
Support by grant MSM 0021622402.
The fact that raised nocturnal blood pressure predicted a higher rate of cardiovascular complications was established in several large-scale studies (1 - 6). Recently the investigators of the International Database on Ambulatory blood pressure monitoring in relation to Cardiovascular Outcomes (IDACO) did 24-hour blood pressure monitoring in 7458 people from Denmark, Belgium, Japan, Sweden, Uruguay and China and calculated cohort, sex, age, body-mass index, smoking and drinking, serum cholesterol, history of cardiovascular disease, diabetes mellitus, and antihypertensive drug treatment adjusted hazard ratios for day-time and night-time blood pressure (7). In fully adjusted models, the night-time blood pressure was additionally adjusted for day-time blood pressure. The subjects with mean age of 56.8 years were followed for approximately 10 years (median 9.6 years). Fully adjusted night-time blood pressure predicted total, cardiovascular and non-cardiovascular mortality. Results of all those studies indicated the necessity of 24-hour ambulatory blood pressure recording in clinical practice. Because the diagnosis of hypertension is generally based on casual measurement of blood pressure in general practitioner office and these values of blood pressure are higher than values of ambulatory blood pressure monitoring, the table of blood pressure thresholds for definition of hypertension with different types of measurement is included in the Guidelines for Management of Hypertension (8). According to this table the threshold for systolic blood pressure is 140 mmHg in the office or clinic, 125 - 130 mmHg during 24 hours, 130 -135 mmHg during day and 120 mmHg during night. The corresponding values for diastolic blood pressure are 90 mmHg in the office and clinic, 80 mmHg during 24 hours, 85 mmHg during day and 75 mmHg during night. The values for home measurement are the same as for ambulatory monitoring during day.
The condition for reliability of diagnosis is low day-to-day variation of night-time and day-time pressure values.
The variation of night-time and day-time blood pressure during 7-day continuous ambulatory monitoring was the aim of the present study.
Methods
Thirty subjects (18 males, 12 females), twenty one years to seventy three years old, were recruited for seven-day blood pressure monitoring. Colin Medical Instruments (Komaki, Japan) were used for ambulatory blood pressure monitoring (oscillation method, 30-minute interval between measurements) (9). One-hour means of systolic and diastolic blood pressure were evaluated, when night-time was considered from midnight to 0600 h and day-time from 1000 to 2200 h, avoiding the transitional periods. Mean day-time and mean night-time systolic and diastolic pressures were evaluated every day (10).
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NONINVASIVE METHODS IN CARDIOLOGY 2010
Results
The patients were ordered according mean 7-day SBP (patient No 1: 107 mmHg, patient No 30: 131 mmHg; median value: 123 mmHg).
The variability of one-daytime SBP values during 7-day monitoring is seen in Fig. 1. Taking 135 mmHg of day-time systolic pressure as a threshold for indication to treatment, then 13 patients (43 %) were under this value every day and nobody was over this value every day. 17 patients (57 %) were one day indicated for treatment and the other day not.
The night-time SBP values are seen in Fig. 2. Similarly, if 120 mmHg of night-time systolic pressure is the threshold, then 10 subjects (33 %) were indicated one day for treatment and the other day not. Corresponding value of threshold for diastolic day-time pressure is 85 mmHg, thus 22 patients (73 %) were one day indicated for treatment and the other day not (Fig. 3) and for night diastolic pressure of 70 mmHg 24 patients (80 %) were indicated one day for treatment and the other day not. Only one patient (3%) was indicated for treatment every day on the DBP night basis (Fig. 4). Those data demonstrate large day-to-day SBP and DBP mean day-time and mean night-time variability.
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