T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline

T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline

Normal aging is characterized by declines in processing speed, learning, memory, and executive function even in the absence of neurodegenerative diseases such as Alzheimer's Disease (AD). In normal aging monkeys and humans, neuronal loss does not account for cognitive impairment. Instead, loss...

Full description

Bibliographic Details
Main Authors: Katelyn V. Batterman, Payton E. Cabrera, Tara L. Moore, Douglas L. Rosene
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-02-01
Series:Frontiers in Immunology
Subjects:
myelin
T cells
aging
cognitive decline
microglia
blood brain barrier
Online Access:https://www.frontiersin.org/articles/10.3389/fimmu.2021.607691/full
id doaj-d5667f875675400c86dd347b8e4aac1b
record_format Article
spelling doaj-d5667f875675400c86dd347b8e4aac1b2021-02-16T04:22:33ZengFrontiers Media S.A.Frontiers in Immunology1664-32242021-02-011210.3389/fimmu.2021.607691607691T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive DeclineKatelyn V. Batterman0Payton E. Cabrera1Tara L. Moore2Tara L. Moore3Tara L. Moore4Douglas L. Rosene5Douglas L. Rosene6Laboratory for Cognitive Neurobiology, Department of Anatomy & Neurobiology, Boston University School of Medicine, Boston, MA, United StatesLaboratory for Cognitive Neurobiology, Department of Anatomy & Neurobiology, Boston University School of Medicine, Boston, MA, United StatesLaboratory for Cognitive Neurobiology, Department of Anatomy & Neurobiology, Boston University School of Medicine, Boston, MA, United StatesLaboratory of Interventions for Cortical Injury and Cognitive Decline, Department of Anatomy & Neurobiology, Boston University School of Medicine, Boston, MA, United StatesCenter for Systems Neuroscience, Boston University, Boston, MA, United StatesLaboratory for Cognitive Neurobiology, Department of Anatomy & Neurobiology, Boston University School of Medicine, Boston, MA, United StatesCenter for Systems Neuroscience, Boston University, Boston, MA, United StatesNormal aging is characterized by declines in processing speed, learning, memory, and executive function even in the absence of neurodegenerative diseases such as Alzheimer's Disease (AD). In normal aging monkeys and humans, neuronal loss does not account for cognitive impairment. Instead, loss of white matter volume and an accumulation of myelin sheath pathology begins in middle age and is associated with cognitive decline. It is unknown what causes this myelin pathology, but it likely involves increased neuroinflammation in white matter and failures in oligodendrocyte function (maturation and repair). In frontal white matter tracts vulnerable to myelin damage, microglia become chronically reactive and secrete harmful pro-inflammatory cytokines. Despite being in a phagocytic state, these microglia are ineffective at phagocytosing accruing myelin debris, which directly inhibits myelin sheath repair. Here, we asked whether reported age-related increases in pro-inflammatory markers were accompanied by an adaptive immune response involving T cells. We quantified T cells with immunohistochemistry in the brains of 34 cognitively characterized monkeys and found an age-related increase in perivascular T cells that surround CNS vasculature. We found a surprising age-related increase in T cells that infiltrate the white matter parenchyma. In the cingulum bundle the percentage of these parenchymal T cells increased with age relative to those in the perivascular space. In contrast, infiltrating T cells were rarely found in surrounding gray matter regions. We assessed whether T cell infiltration correlated with fibrinogen extravasation from the vasculature as a measure of BBB leakiness and found no correlation, suggesting that T cell infiltration is not a result of passive extravasation. Importantly, the density of T cells in the cingulum bundle correlated with microglial reactivity and with cognitive impairment. This is the first demonstration that T cell infiltration of white matter is associated with cognitive decline in the normal aging monkey.https://www.frontiersin.org/articles/10.3389/fimmu.2021.607691/fullmyelinT cellsagingcognitive declinemicrogliablood brain barrier
collection DOAJ
language English
format Article
sources DOAJ
author Katelyn V. Batterman
Payton E. Cabrera
Tara L. Moore
Tara L. Moore
Tara L. Moore
Douglas L. Rosene
Douglas L. Rosene
spellingShingle Katelyn V. Batterman
Payton E. Cabrera
Tara L. Moore
Tara L. Moore
Tara L. Moore
Douglas L. Rosene
Douglas L. Rosene
T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
Frontiers in Immunology
myelin
T cells
aging
cognitive decline
microglia
blood brain barrier
author_facet Katelyn V. Batterman
Payton E. Cabrera
Tara L. Moore
Tara L. Moore
Tara L. Moore
Douglas L. Rosene
Douglas L. Rosene
author_sort Katelyn V. Batterman
title T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
title_short T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
title_full T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
title_fullStr T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
title_full_unstemmed T Cells Actively Infiltrate the White Matter of the Aging Monkey Brain in Relation to Increased Microglial Reactivity and Cognitive Decline
title_sort t cells actively infiltrate the white matter of the aging monkey brain in relation to increased microglial reactivity and cognitive decline
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2021-02-01
description Normal aging is characterized by declines in processing speed, learning, memory, and executive function even in the absence of neurodegenerative diseases such as Alzheimer's Disease (AD). In normal aging monkeys and humans, neuronal loss does not account for cognitive impairment. Instead, loss of white matter volume and an accumulation of myelin sheath pathology begins in middle age and is associated with cognitive decline. It is unknown what causes this myelin pathology, but it likely involves increased neuroinflammation in white matter and failures in oligodendrocyte function (maturation and repair). In frontal white matter tracts vulnerable to myelin damage, microglia become chronically reactive and secrete harmful pro-inflammatory cytokines. Despite being in a phagocytic state, these microglia are ineffective at phagocytosing accruing myelin debris, which directly inhibits myelin sheath repair. Here, we asked whether reported age-related increases in pro-inflammatory markers were accompanied by an adaptive immune response involving T cells. We quantified T cells with immunohistochemistry in the brains of 34 cognitively characterized monkeys and found an age-related increase in perivascular T cells that surround CNS vasculature. We found a surprising age-related increase in T cells that infiltrate the white matter parenchyma. In the cingulum bundle the percentage of these parenchymal T cells increased with age relative to those in the perivascular space. In contrast, infiltrating T cells were rarely found in surrounding gray matter regions. We assessed whether T cell infiltration correlated with fibrinogen extravasation from the vasculature as a measure of BBB leakiness and found no correlation, suggesting that T cell infiltration is not a result of passive extravasation. Importantly, the density of T cells in the cingulum bundle correlated with microglial reactivity and with cognitive impairment. This is the first demonstration that T cell infiltration of white matter is associated with cognitive decline in the normal aging monkey.
topic myelin
T cells
aging
cognitive decline
microglia
blood brain barrier
url https://www.frontiersin.org/articles/10.3389/fimmu.2021.607691/full
work_keys_str_mv AT katelynvbatterman tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT paytonecabrera tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT taralmoore tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT taralmoore tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT taralmoore tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT douglaslrosene tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
AT douglaslrosene tcellsactivelyinfiltratethewhitematteroftheagingmonkeybraininrelationtoincreasedmicroglialreactivityandcognitivedecline
_version_ 1724268436218970112

Similar Items