Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study

Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study

Background: Psychobiological processes linking stress and vascular diseases remain poorly understood. The retina and the brain share a common embryonic-diencephalon origin and blood-barrier physiology e.g. ongoing ischemia facilitates S100B release with astrocytic activity and glial-fibrillary-acidi...

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Main Authors: Leoné Malan, Mark Hamer, Roland von Känel, Roelof D. van Wyk, Annemarie Wentzel, Hendrik S. Steyn, Pieter van Vuuren, Nico T. Malan
Format: Article
Language:English
Published: Elsevier 2020-02-01
Series:Brain, Behavior, & Immunity - Health
Subjects:
Stress
Ischemia
Inflammation
Retina
Glia
Online Access:http://www.sciencedirect.com/science/article/pii/S2666354619300286
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spelling doaj-f1ae9d63589c4c08bc62990cdfe9fde72021-06-10T04:57:21ZengElsevierBrain, Behavior, & Immunity - Health2666-35462020-02-012100027Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA studyLeoné Malan0Mark Hamer1Roland von Känel2Roelof D. van Wyk3Annemarie Wentzel4Hendrik S. Steyn5Pieter van Vuuren6Nico T. Malan7Hypertension in Africa Research Team (HART), North-West University, Potchefstroom, 2520, South Africa; Corresponding author. Hypertension in Africa Research Team (HART), North-West University, Private Bag X6001, Potchefstroom, 2520, South Africa.Division Surgery & Interventional Science, University College London, United KingdomDepartment of Consultation-Liaison Psychiatry and Psychosomatic Medicine, University Hospital Zurich, 8091, SwitzerlandSurgical Ophthalmologist, 85 Peter Mokaba Street, Potchefstroom, 2531, South AfricaHypertension in Africa Research Team (HART), North-West University, Potchefstroom, 2520, South AfricaStatistical Consultation Services, North-West University, Potchefstroom, 2520, South AfricaSchool of Electrical, Electronic and Computer Engineering, North-West University, Potchefstroom, 2520, South AfricaHypertension in Africa Research Team (HART), North-West University, Potchefstroom, 2520, South AfricaBackground: Psychobiological processes linking stress and vascular diseases remain poorly understood. The retina and the brain share a common embryonic-diencephalon origin and blood-barrier physiology e.g. ongoing ischemia facilitates S100B release with astrocytic activity and glial-fibrillary-acidic-protein expression (GFAP). However, GFAP decreases revealed astrocyte pathology in the prefrontal cortex of depression/suicide cases; and might be a key mechanism in stress – disease pathways. Methods: A chronic emotional stress phenotype independent of age, ethnicity or sex was used to stratify the current prospective cohort (N ​= ​359; aged 46 ​± ​9 years) into Stress (N ​= ​236) and no-Stress groups (N ​= ​123). Prospective data for glia ischemia risk markers were obtained, including 24 ​h BP, fasting S100B, GFAP, HbA1C and tumor-necrosis-factor-α (TNF-α). At 3-yr follow-up: diastolic-ocular-perfusion-pressure (indicating hypo-perfusion risk) was measured and retinal vessel calibers were quantified from digital images in the mydriatic eye. Results: Higher hypertension (75% vs. 16%), diabetes (13% vs. 0%) and retinopathy (57% vs. 45%) prevalence was observed in Stress compared to no-Stress individuals. Stressed individuals had consistently raised S100B, TNF-α, HbA1C and higher diastolic-ocular-perfusion-pressure, but decreases in GFAP and GFAP:S100B. Furthermore stroke risk markers, arterial narrowing and venous widening were associated with consistently raised S100B, GFAP:S100B (p ​= ​0.060), TNF-α and higher diastolic-ocular-perfusion-pressure [Adj. R2 0.39–0.41, p ​≤ ​0.05]. No retinal-glia associations were evident in the no-Stress group. Conclusions: Retinal-glia ischemia and inflammation was induced by chronic stress. Persistent higher inflammation and S100B with GFAP decreases further reflected stress-induced astrocyte pathology in the human retina. It is recommended to increase awareness on chronic stress and susceptibility for brain ischemia.http://www.sciencedirect.com/science/article/pii/S2666354619300286StressIschemiaInflammationRetinaGlia
collection DOAJ
language English
format Article
sources DOAJ
author Leoné Malan
Mark Hamer
Roland von Känel
Roelof D. van Wyk
Annemarie Wentzel
Hendrik S. Steyn
Pieter van Vuuren
Nico T. Malan
spellingShingle Leoné Malan
Mark Hamer
Roland von Känel
Roelof D. van Wyk
Annemarie Wentzel
Hendrik S. Steyn
Pieter van Vuuren
Nico T. Malan
Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
Brain, Behavior, & Immunity - Health
Stress
Ischemia
Inflammation
Retina
Glia
author_facet Leoné Malan
Mark Hamer
Roland von Känel
Roelof D. van Wyk
Annemarie Wentzel
Hendrik S. Steyn
Pieter van Vuuren
Nico T. Malan
author_sort Leoné Malan
title Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
title_short Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
title_full Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
title_fullStr Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
title_full_unstemmed Retinal-glia ischemia and inflammation induced by chronic stress: The SABPA study
title_sort retinal-glia ischemia and inflammation induced by chronic stress: the sabpa study
publisher Elsevier
series Brain, Behavior, & Immunity - Health
issn 2666-3546
publishDate 2020-02-01
description Background: Psychobiological processes linking stress and vascular diseases remain poorly understood. The retina and the brain share a common embryonic-diencephalon origin and blood-barrier physiology e.g. ongoing ischemia facilitates S100B release with astrocytic activity and glial-fibrillary-acidic-protein expression (GFAP). However, GFAP decreases revealed astrocyte pathology in the prefrontal cortex of depression/suicide cases; and might be a key mechanism in stress – disease pathways. Methods: A chronic emotional stress phenotype independent of age, ethnicity or sex was used to stratify the current prospective cohort (N ​= ​359; aged 46 ​± ​9 years) into Stress (N ​= ​236) and no-Stress groups (N ​= ​123). Prospective data for glia ischemia risk markers were obtained, including 24 ​h BP, fasting S100B, GFAP, HbA1C and tumor-necrosis-factor-α (TNF-α). At 3-yr follow-up: diastolic-ocular-perfusion-pressure (indicating hypo-perfusion risk) was measured and retinal vessel calibers were quantified from digital images in the mydriatic eye. Results: Higher hypertension (75% vs. 16%), diabetes (13% vs. 0%) and retinopathy (57% vs. 45%) prevalence was observed in Stress compared to no-Stress individuals. Stressed individuals had consistently raised S100B, TNF-α, HbA1C and higher diastolic-ocular-perfusion-pressure, but decreases in GFAP and GFAP:S100B. Furthermore stroke risk markers, arterial narrowing and venous widening were associated with consistently raised S100B, GFAP:S100B (p ​= ​0.060), TNF-α and higher diastolic-ocular-perfusion-pressure [Adj. R2 0.39–0.41, p ​≤ ​0.05]. No retinal-glia associations were evident in the no-Stress group. Conclusions: Retinal-glia ischemia and inflammation was induced by chronic stress. Persistent higher inflammation and S100B with GFAP decreases further reflected stress-induced astrocyte pathology in the human retina. It is recommended to increase awareness on chronic stress and susceptibility for brain ischemia.
topic Stress
Ischemia
Inflammation
Retina
Glia
url http://www.sciencedirect.com/science/article/pii/S2666354619300286
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