Cellular changes of the choroid plexus induced by subarachnoid
hemorrhage

SOLÁR, Peter, Ilona KLUSÁKOVÁ, Radim JANČÁLEK, Petr DUBOVÝ and Marek JOUKAL. Cellular changes of the choroid plexus induced by subarachnoid hemorrhage. In Morphology 2017. 2017. ISBN 978-80-263-1315-1.

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TY  - CONF
ID  - 1389527
AU  - Solár, Peter - Klusáková, Ilona - Jančálek, Radim - Dubový, Petr - Joukal, Marek
PY  - 2017
TI  - Cellular changes of the choroid plexus induced by subarachnoid hemorrhage
SN  - 9788026313151
N2  - The subarachnoid hemorrhage (SAH) is a specific form of the hemorrhagic stroke. Choroid plexus (CP) of the brain ventricles forms the blood-cerebrospinal fluid (B-CSF) barrier and is responsible for CSF production. The aim of our study was to describe the cellular changes in the CP after SAH. Wistar rats (n=51; male; 250-300g) were used in our experiment. Stereotaxic injection of autologous arterial blood (SAH group) or artificial CSF (control groups) to the prechiasmatic cisterna was performed and rats were left to survive for 1, 3 and 7 days. After time of survival the SAH and control groups of animals were sacrificed in CO2 together with naïve rats, perfused transcardially by Zamboni´s fixative and the brain was removed. Coronal cryostat sections were cut through the lateral and third ventricles. Immunohistochemical detection of activated (ED1+) and resident (ED2+) macrophages as well as proliferating cells (Ki-67) was performed. Numbers of ED1+, ED2+ and Ki-67+ cells per 1 mm2 of CP were counted and statistically analyzed. Immunostaining revealed ED1+ and ED2+ macrophages as well as proliferating cells (Ki-67+) in epiplexus position. Number of ED1+ macrophages gradually increased following the time of survival. Statistically significant increased number of ED1+ macrophages was found 3 and 7 days after SAH comparing to the of naïve and control rats. SAH induced statistically significant increase number of ED2+ macrophages after 1, 3 and 7 days after SAH comparing to the naive and control groups. Statistically significant increased proliferation was detected in all periods of survival after SAH comparing to naïve and control animals. The CP responds to SAH with increased number of macrophages in epiplexus position and cellular proliferation. Inflammatory reaction expressed by number of ED1+ macrophages increases with time from SAH. These changes may contribute to alteration of B-CSF barrier after SAH.
ER  -

Basic information
Original name	Cellular changes of the choroid plexus induced by subarachnoid hemorrhage
Authors	SOLÁR, Peter, Ilona KLUSÁKOVÁ, Radim JANČÁLEK, Petr DUBOVÝ and Marek JOUKAL.
Edition	Morphology 2017, 2017.

Other information
Original language	English
Type of outcome	Presentations at conferences
Field of Study	30000 3. Medical and Health Sciences
Country of publisher	Czech Republic
Confidentiality degree	is not subject to a state or trade secret
Organization unit	Faculty of Medicine
ISBN	978-80-263-1315-1
Changed by	Changed by: MUDr. Peter Solár, Ph.D., učo 381006. Changed: 16/9/2017 21:17.

Abstract

The subarachnoid hemorrhage (SAH) is a specific form of the hemorrhagic stroke. Choroid plexus (CP) of the brain ventricles forms the blood-cerebrospinal fluid (B-CSF) barrier and is responsible for CSF production. The aim of our study was to describe the cellular changes in the CP after SAH. Wistar rats (n=51; male; 250-300g) were used in our experiment. Stereotaxic injection of autologous arterial blood (SAH group) or artificial CSF (control groups) to the prechiasmatic cisterna was performed and rats were left to survive for 1, 3 and 7 days. After time of survival the SAH and control groups of animals were sacrificed in CO2 together with naïve rats, perfused transcardially by Zamboni´s fixative and the brain was removed. Coronal cryostat sections were cut through the lateral and third ventricles. Immunohistochemical detection of activated (ED1+) and resident (ED2+) macrophages as well as proliferating cells (Ki-67) was performed. Numbers of ED1+, ED2+ and Ki-67+ cells per 1 mm2 of CP were counted and statistically analyzed. Immunostaining revealed ED1+ and ED2+ macrophages as well as proliferating cells (Ki-67+) in epiplexus position. Number of ED1+ macrophages gradually increased following the time of survival. Statistically significant increased number of ED1+ macrophages was found 3 and 7 days after SAH comparing to the of naïve and control rats. SAH induced statistically significant increase number of ED2+ macrophages after 1, 3 and 7 days after SAH comparing to the naive and control groups. Statistically significant increased proliferation was detected in all periods of survival after SAH comparing to naïve and control animals. The CP responds to SAH with increased number of macrophages in epiplexus position and cellular proliferation. Inflammatory reaction expressed by number of ED1+ macrophages increases with time from SAH. These changes may contribute to alteration of B-CSF barrier after SAH.

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Cellular changes of the choroid plexus induced by subarachnoid hemorrhage

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