INSTITUT LADY DAVIS DE RECHERCHES MÉDICALES / LADY DAVIS INSTITUTE FOR MEDICAL RESEARCH
Cancer and Aging: Two Faces of the Same Coin
(2) Telomere Biology and Aging
Centre Bloomfield de
recherche sur le vieillissement
The Bloomfield Centre
for Research in Aging

TELOMERE BIOLOGY AND AGING
1.Telomeres: composition & function
2.Consequences of telomere shortening
3.Telomere shortening and human aging
4.Telomerase
5.Telomere hypothesis of aging and immortalization
6.Telomere-dependent and independent cellular senescence
7.Cellular senescence, aging, tumor suppression, and tumor promotion
8.Telomerase knockout and transgenic mice

Telomere structure
•Coated with telomeric proteins
•Form a non-linear structure that sequesters/hides the DNA end (T-loop)
Telomere interference :
•telomeric chromosome fusions
•chromosome instability
•replicative senescence
•cell death
Telomere integrity:
•essential for replicative
  immortality
Full Size Image
Griffith, JD et al., Cell 1999
Baumann, P. Cell 2006

End-replication problem
DNA replication
RNA primer removal,
Okazaki fragment ligation
Leading strand
Lagging strand
Leading strand
Lagging strand
Lagging strand
Leading strand
Osterhage and Friedman. 2009. JBC, 284,  16061-16065

Functions of telomeres
•Ensure complete replication of DNA at chromosome ends (via telomerase, a ribonucleoprotein and
reverse transcriptase which synthesizes the telomeric repeats on the G-rich strand)
•‘Cap’ natural chromosome ends to make them stable structures:
–Shield chromosome ends from degradation and end-to-end fusions
–Prevent activation of DNA damage checkpoints




Fig 1 full size Fig 2 full size Fig 3 full size
Cumulative citations for telomerase in Medline
Tetrahymena sequences are added to yeast telomeres in vitro.
Yeast sequences are added to Tetrahymena telomeres in vivo.

Non-shelterin proteins associated with vertebrate telomere maintenance
•
•
Slijepcevic, P. 2006. DNA repair 5,1299-306

Consequences of telomere shortening
End-to-end chromosome fusions
latre03a
DAPI
Telomere
probe
Latre et al., 2003

Cytogenetic abnormalities resulting from telomere shortening/telomere dysfunction
vansteensel98b vansteensel98b
Fusion-bridge-breakage cycles
Telomeric
fusion
‘Bridge’
chromosomes
Chromosome
breakage/
missegregation
Fusion of broken
chromosomes
vanSteensel et al., 1998
vansteensel98b

Cytogenetic consequences of fusion-bridge-breakage cycle
•Chromosome and gene deletions
•Complex non-reciprocal translocations (hallmark of human carcinomas)
DNA DAMAGE

Cellular consequences of telomere shortening-induced DNA damage
•Replicative senescence (permanent growth arrest)
•Apoptosis (programmed cell death)
•Carcinogenesis (in the absence of
      functional DNA damage checkpoints such as p53)

Cellular senescence and apoptosis as major tumor suppressor mechanisms
Carcinogenesis can occur when important DNA damage checkpoint-regulating genes and pathways (eg.
p53, pRb, p16INK4A) are absent or defective.
The products of these tumor suppressor genes ensure that cells with irreparably damaged genomes die
(apoptosis) or stop dividing permanently (replicative senescence).
Cells with damaged genomes can only continue to proliferate if they accumulate genetic mutations
that inhibit the major tumor suppressor pathways.

Major regulators of replicative senescence: p53
‘guardian of the genome’
–Tumor suppressor gene at the hub of many different signaling pathways that provide information
about cellular stress states—DNA damage strongly upregulates p53 activity
–Transcriptional regulator —downregulates many genes; upregulates some others
–p53 signaling elicits cell cycle arrest (in G1, S or G2/M) and/or cell death or senescence
–p53 is inactivated by MDM2, which binds to p53 and inhibits its ability to regulate transcription
–p53 is specifically targeted by many important oncogenic, transforming viruses (e.g. SV40, HPV)
–p53 is mutated or deleted in at least 50% of human cancers, and is dysregulated in many more

Major regulators of replicative senescence:
p16INK4A and p19ARF
•INK4A locus
–Codes for both the p16INK4A and p19ARF tumor suppressor gene products (in alternative reading
frames)
–Frequently deleted or silenced in human cancers (eliminating expression of both p16INK4A and
p19ARF)
•p16INK4A
–Important for replicative senescence in human cells
–Increased expression in primary human fibroblasts with increasing population doubling number
–Mouse primary fibroblasts that bypass senescence lose expression of p16INK4A
–Regulates the pRB (retinoblastoma) pathway via cdk4 and cdk6 (inhibits cellular proliferation)
–Does not require p53 for antiproliferative function (alternative senescence pathway)
–Frequently targeted by oncogenic viruses
–
•p19ARF (also called p14INK4A in human cells)
–Important for replicative senescence in mouse cells
–Binds and sequesters MDM2 (prevents it from inactivating p53)
•

Telomere shortening and human aging
•HUMAN AGING
–CANCER!!! (especially epithelial cancers)
–decline of the immune system
–reduced skin thickness and wound healing capacity
–changes in the morphology and function of epithelial tissues in the digestive and cardiovascular
systems
–reduced fertility
•All tissues in the adult body are renewed by cellular replication
–exception: terminally differentiated (post-mitotic) cells such as neurons and cardiac muscle cells
–
•Apoptosis and replicative senescence  in cells with short telomeres could slow or prevent tissue
self renewal
•Tissues that undergo the highest rates of cell division and self-renewal would be most affected by
replicative senescence and apoptosis (immune system, epithelial tissues)
•…..these are the tissues that are most profoundly affected during aging, and commonly give rise to
cancers in adult humans

Solutions to the end replication problem
•Circular chromosomes (bacteria)
•Terminal hairpin structures (vaccinia virus, some bacteria with linear chromosomes)
•Terminal proteins (adenovirus, Ф29)
•Telomerase (most eukaryotes)
•Retrotransposition (drosophila)
•Alternative mechanisms (ALT) (recombination-based: yeast, 15% human cancer cells)

What is telomerase?
Telomere
DNA repeats
Extension of telomeric
DNA by telomerase
Uniciliates
Yeasts
Plants
Vertebrates
•Essential for replicative immortality
  of most eukaryotic cells
•DNA polymerase
•Caps linear DNA molecules with
  telomere DNA repeats
tetrahymena
Scanning electron
micrograph

micronuclei macronuclei
Vegetative cell undergoing micronuclear
or macronuclear division
TETRAHYMENA
vUnicellular protist
vTwo nuclei: micronucleus is a conventional germline precursor
macronucleus is the somatic or transcriptionally active nucleus
vHighly developed unicell with features characteristic of metazoans
with highly differentiated tissues

Tetrahymena as a model system
for the study of telomerase
Telomerase activity is abundant in Tetrahymena compared to
human (during conjugation and macronuclear development
there is extensive chromosome fragmentation, DNA rearrange-
ment and DNA deletion and amplification creating >10000
chromosome end compared to 92 in humans)
Telomerase activity and the telomerase RNA component were
first identified in Tetrahymena

#5
Greider and Blackburn, 1989


anaphase
Telomere Dysfunction
Consequence of altered telomerase RNA
template in vivo first demonstrated in
Tetrahymena (Yu et al., 1990; Kirk et al.,
1997)
-Altered telomere sequences
-Altered telomere lengths
-Impaired cell division
-Severe delay or block in completing
mitotic anaphase
-Senesence phenotype
Kirk et al., 1997

Human telomerase complex
hTERT
(telomerase
reverse
transcriptase)
hTR
(telomerase
RNA)
aka hTERC
Other telomerase-
interacting proteins:
RNA processing and
ribonucleoprotein assembly
(snoRNA-associated proteins)
Dyskerin, NHP2, NOP10, GAR1
Molecular chaperones (Hsp90, p23)
Localization (TCAB1)
Post-translational
modification
Recruitment of telomerase
to telomeres TPP1, Pot1
DNA replication machinery
hTR-dyskerin
Dokal I. And Vulliamy T. 2003. Blood Rev. 17, 217-225
Minimal telomerase components (RRL reconstitution) = hTR + hTERT

Organization of the reverse transcriptase (RT) motifs in the
telomerase reverse transcriptase (TERT) from
different organisms and HIV-1 RT
Autexier and Lue, 2006 Ann. Rev. Biochem.
Gillis et al. Nature, 455(7213), 633-7, 2008
Structure of the Tribolium castaneum telomerase catalytic subunit TERT

Phylogenetically conserved telomerase RNA structure
Autexier and Lue, 2006 Ann. Rev. Biochem.


Telomerase prevents telomere shortening
3'
5'
DNA Replication
DNA Replication
Telomerase
DNA Polymerase
Telomere shortening:
•telomeric chromosome fusions
•chromosome instability
•replicative senescence
•cell death
Telomere length maintenance:
•essential for replicative immortality

Synthesis of telomeric sequences
1) Recognition
2) Elongation
3) Translocation
DNA substrate binding to hTERT and RNA template
Addition of nucleotides
DNA substrate and enzyme repositioning
CAAUCCCAAUC
3’
5’
hTERT
hTR
5’- GGTTAGGGTTAGGGTTAG
3’- CCAAT
GGTTAG
GGTTAG
GGTTAG
4) Repeated translocation and elongation=repeat addition processivity
G
A
T
T
G
G
TRAP
assay
Direct primer extension
assay

Cell divisions
Cellular Senescence
Germline Cells
Stem cells
Deregulated
Cellular Growth
Checkpoint Escape
-p53, -pRb
Telomerase or ALT
Reactivation
Tumor Cells
Telomere Hypothesis of Cellular Aging
and Immortalization
TELOMERASE
ON
TELOMERASE
ON
TELOMERASE
OFF
Cellular Crisis

Testing the telomere hypothesis of cellular aging and immortalization
•Many studies found a CORRELATION between:
–
–Telomere shortening and cell death or replicative senescence
–Telomere length maintenance, telomerase activity and cellular immortalization
How could you test these correlations?

Testing the telomere hypothesis of cellular aging and immortalization
•Many studies found a CORRELATION between:
–Telomere shortening and cell death or replicative senescence
–Telomere length maintenance, telomerase activity and cellular immortalization
•Test the telomere hypothesis directly by manipulating telomere length via telomerase inhibition or
activation

Question 1
Is telomere shortening a cell division clock that limits cellular lifespan?


Telomerase activation immortalizes
normal human cells
Normal human fibroblast
hTERT
Telomere shortening/senescence
“Tumour suppressor mechanism”
•Telomerase activity induced
•Telomere maintenance or
  elongation occurs
•Cells have an extended lifespan
•Cells do not have characteristics
  of cancer cells
Bodnar et al., 1998

Telomerase activation is not sufficient for immortalization of some human cell types
e.g. express hTERT in keratinocytes and mammary epithelial cells
Result:
•cells senesce
•p16INK4A expression must be downregulated in these cells for
immortalization to occur
Conclusion:
•other factors besides telomere length contribute to replicative
senescence in some cell types

Question 2
Does telomerase activation transform human cells?


Normal skin cells
hTERT
Telomerase activation is essential but not sufficient for transformation of human cells
Alterations in other key cellular genes:
Expression of SV40LTAg (pRB, p53),
SV40 sTAg (protein phosphatase 2A)
and mutant Ras
Tumor cells
Hahn et al., 1999; 2002

vTelomere erosion is unlikely to be a primary tumor suppressor mechanism in rodents
Mouse telomeres ~ 20 KB longer than human telomeres
Telomerase activity is not stringently repressed in the somatic tissues of mice
vReplicative senescence is different in rodent and human cells
Replicative senescence occurs in rodent cells with long telomeres
Rodent cells can spontaneously immortalize in culture at detectable frequencies without the aid of
oncogenes (unlike human cells)
Mouse models: Differences in the biology of telomeres, telomerase and replicative senescence in
mice and humans

Hallmarks of senescent cells
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556
SASP: senescence-associated secretory phenotype

What defines a senescent cell?
(i)Permanent growth arrest that can’t be reversed by known physiological stimuli
(i)Cell size increase
(i)Senescence-associated b-galactosidase, partly reflects the increased lysosomal mass
(i)p16INK4a expression causes formation of senescence-associated heterochromatin foci
-p16INK4a expression increases with age in mice and humans
-p16INK4a activity linked to decreased progenitor cell number in aging tissues
(v)Cells that senesce with persistent DNA damage signaling harbor persistent nuclear foci
termed DNA segments with chromatin alterations reinforcing senescence
DNA-SCARS (include TIFs-telomere dysfunction-induced foci)
(vi) Senescent cells with persistent DNA damage signaling secrete growth factors, proteases,
cytokines, and other factors that have potent autocrine and paracrine activities
(senescence-associated secretory phenotype:SASP)
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556

Causes of cellular senescence
‘Culture stress’: inappropriate
substrata, serum, hyper-
physiological oxygen
Coppé, J.-P. et al. 2010. The senescence-associated secretory phenotype: the dark side of tumor
suppression. Annu. Rev. Pathol. Mech. Dis. 2010. 5, 99-118.
PTEN tumor suppressor loss

Image
p53 and p16/pRb Pathways in the
Senescence Response
By inactivation of p53, but not by
physiological mitogens
Campisi, J. 2005. Senescent cells, tumor suppression, and organismal aging: good citizens, bad
neighbors. Cell 120, 513-522.

Tumor Suppressors
Caretaker tumor suppressors prevent cancer by protecting the genome from
mutation
Gatekeeper tumor suppressors, prevent cancer by acting on intact cells
through the induction of apoptosis or cellular senescence
Deplete nonrenewable/renewable tissues of
proliferating or stem cell pools
Dysfunctional senescent cells may
actively disrupt normal tissues as
they accumulate
Gatekeeper tumor suppressors may be antagonistically pleitropic,
beneficial early in life by suppressing cancer but detrimental later
in life by compromising tissue function
Campisi, J. 2005. Senescent cells, tumor suppression, and organismal aging: good citizens, bad
neighbors. Cell 120, 513-522.

Cellular Senescence as a Tumor Suppressor
•Senescent markers accumulate in premalignant cells but not in
the cancers that can develop from these cells
•Tumor progression can be inhibited by senescence
•Some tumor cells retain the ability to senesce and regress
(e.g. upon p53 reactivation or inactivation of apoptosis)
•Imposes a cell-autonomous block to the proliferation of
oncogenically damaged/stressed cells
•
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556

Cellular Senescence as a Tumor Suppressor
Serrano, M. 2007. Cancer regression by senescence. NEJM 356, 1996-1997.


Cellular Senescence and Aging
Image
Fibroblasts maintain the
stromal support for virtually
all renewable epithelial tissues
Stimulate chronic tissue
remodeling and/or local
inflammation
Extensive evidence that senescent cells (as defined by high levels of p16 and SA-b-gal)
accumulate with age in multiple tissues from both human and rodents; present at sites of
age-related pathologies.
Stimulate the proliferation
of cells that harbor pre-
neoplastic mutations
Campisi, J. 2005. Senescent cells, tumor suppression, and
organismal aging: good citizens, bad neighbors. Cell 120, 513-522.

Cellular Senescence and tumor promotion
•Senescent cells increase with age
•
•SASP factors
stimulate the proliferation of premalignant epithelial cells (growth
related oncogene, IL-6, IL-8)
stimulate endothelial cell migration (VEGF)
facilitate tumor cell invasiveness (matrix metalloproteinases)
•In xenografts, senescent cells can promote malignant progression
of precancerous and established cancer cells
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556

Cellular Senescence and Aging
Constitutive expression of artificially (p53+/m) or naturally truncated p53
 (p44 isoform) in mice leads to p53 activation
•Cancer-free
•Shortened life span and premature aging (can extend lifespan
depending on physiological context-discussed later)
•Tissues accumulated senescent cells
Tyner, S.D. et al. 2002. p53 mutant mice that display early ageing-associated phenotypes. Nature
415, 45-53.
mutant p53 transgenic (pL53) mice containing roughly 20 copies of a mutation at codon 135

Biological activities of cellular senescence
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556
?
p16/p53/pRb

Four Faces of Cellular Senescence
Rodier, F. and Campisi, J. 2011. Four faces of cellular senescence. JCB 192, 547-556


mTR knockout mouse: model for aging?
blasco97
Progressive telomere shortening over successive generations
Blasco et al., 1997

PIIS0092867401800064
rudolph991
•Hair graying, hair loss
•Decreased skin thickness
•Reduced body weight in old age
•Atrophied intestinal villi
rudolph994
Rudolph et al., 1999
mTR knockout mouse phenotypes

PIIS0092867401800064
•Delayed wound healing
•Reduced regenerative capacity
•Decreased peripheral white blood cells and haemoglobin
•Reduced longevity
Rudolph et al., 1999
mTR knockout mouse phenotypes
rudolph995

•Reduction in size of reproductive organs
•Reduced cellularity in seminiferous tubules
•Decreased proliferation of splenocytes following mitogenic stimulation
Lee et al., 1998
mTR knockout mouse phenotypes
lee981 lee982 lee984
Seminiferous tubules

Rudolph et al., 1999
mTR knockout mouse phenotypes
rudolph997
Moderate increased incidence of spontaneous tumors in highly
proliferative epithelial cell types lymphomas
and teratocarcinomas typically much less frequent in mice

Summary of phenotypes of mTR-/- mice
Rudolph et al., 1999


Sahin, E. And DePinho, R.A. 2010. Linking functional decline of telomeres, mitochondria and stem
cells during ageing.
Nature, 464, 520-528..
Dysfunctional telomeres and premature aging

Conclusion
Late generation mTR knockout mice exhibit a phenotype similar to some features of human aging


Can telomerase overexpression extend lifespan?
In mice with enhanced expression of p53, p16 and p19ARF
Improved GI tract epithelial barrier function
Decreased biomarkers of aging
Decreased molecular markers of aging
Increased median life span and longevity
Delayed telomere loss

Aging by Telomere loss can be reversed!
Telomerase reactivation in adult mice after establishment of telomere-induced aging
Use of a knock-in allele encoding a tamoxifen responsive TERT under control of endogenous promoter
Jaskelioff, M. et al. 2011. Telomerase reactivation reverses tissue degeneration in aged
telomerase-deficient mice. Nature
469, 102-106.

Reversal of Degenerative Pathologies
Telomere function
Neural stem cell function
Ameliorate decreased survival of TERT-ER mice but lifespan not extended compared to G0 mice