4.6 Article

Loss of capillary pericytes and the blood-brain barrier in white matter in poststroke and vascular dementias and Alzheimer's disease

Journal

BRAIN PATHOLOGY
Volume 30, Issue 6, Pages 1087-1101

Publisher

WILEY
DOI: 10.1111/bpa.12888

Keywords

cerebral capillary; collagen type IV; dementia; pericytes; platelet-derived growth factor receptor; vascular dementia; white matter

Funding

  1. UK Medical Research Council (MRC) [G0500247]
  2. Newcastle Centre for Brain Aging and Vitality (BBSRC)
  3. Newcastle Centre for Brain Aging and Vitality (EPSRC)
  4. Newcastle Centre for Brain Aging and Vitality (ESRC)
  5. Newcastle Centre for Brain Aging and Vitality (MRC, LLHW)
  6. Alzheimer's Research (ARUK) [PG2013-22]
  7. UK MRC [G0400074]
  8. Newcastle NIHR Biomedical Research Centre in Aging and Age Related Diseases award
  9. Alzheimer's Society
  10. ARUK as part of the Brains for Dementia Research Project
  11. MRC [G0502157, G0500247, G1100540, G0400074, G0900652] Funding Source: UKRI

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White matter (WM) disease is associated with disruption of the gliovascular unit, which involves breach of the blood-brain barrier (BBB). We quantified pericytes as components of the gliovascular unit and assessed their status in vascular and other common dementias. Immunohistochemical and immunofluorescent methods were developed to assess the distribution and quantification of pericytes connected to the frontal lobe WM capillaries. Pericytes with a nucleus were identified by collagen 4 (COL4) and platelet-derived growth factor receptor-beta (PDGFR-beta) antibodies with further verification using PDGFR-beta-specific ELISA. We evaluated a total of 124 post-mortem brains from subjects with post-stroke dementia (PSD), vascular dementia (VaD), Alzheimer's disease (AD), AD-VaD (Mixed) and post-stroke non-demented (PSND) stroke survivors as well as normal aging controls. COL4 and PDGFR-beta reactive pericytes adopted the characteristic crescent or nodule-like shapes around capillary walls. We estimated densities of pericyte somata to be 225 +/- 38 and 200 +/- 13 (SEM) per COL4 mm(2) area or 2.0 +/- 0.1 and 1.7 +/- 0.1 per mm capillary length in young and older aging controls. Remarkably, WM pericytes were reduced by similar to 35%-45% in the frontal lobe of PSD, VaD, Mixed and AD subjects compared to PSND and controls subjects (P < 0.001). We also found pericyte numbers were correlated with PDGFR-beta reactivity in the WM. Our results first demonstrate a reliable method to quantify COL4-positive pericytes and then, indicate that deep WM pericytes are decreased across different dementias including PSD, VaD, Mixed and AD. Our findings suggest that downregulation of pericytes is associated with the disruption of the BBB in the deep WM in several aging-related dementias.

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