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White matter damage and glymphatic dysfunction in a model of vascular dementia in rats with no prior vascular pathologies.


ABSTRACT: We investigated cognitive function, axonal/white matter (WM) changes and glymphatic function of vascular dementia using a multiple microinfarction (MMI) model in retired breeder (RB) rats. The MMI model induces significant (p < 0.05) cognitive decline that worsens with age starting at 2 weeks, which persists until at least 6 weeks after MMI. RB rats subjected to MMI exhibit significant axonal/WM damage identified by decreased myelin thickness, oligodendrocyte progenitor cell numbers, axon density, synaptic protein expression in the cortex and striatum, cortical neuronal branching, and dendritic spine density in the cortex and hippocampus compared with age-matched controls. MMI evokes significant dilation of perivascular spaces as well as water channel dysfunction indicated by decreased Aquaporin-4 expression around blood vessels. MMI-induced glymphatic dysfunction with delayed cerebrospinal fluid penetration into the brain parenchyma via paravascular pathways as well as delayed waste clearance from the brain. The MMI model in RB rats decreases Aquaporin-4 and induces glymphatic dysfunction which may play an important role in MMI-induced axonal/WM damage and cognitive deficits.

SUBMITTER: Venkat P 

PROVIDER: S-EPMC5209254 | biostudies-literature | 2017 Feb

REPOSITORIES: biostudies-literature

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White matter damage and glymphatic dysfunction in a model of vascular dementia in rats with no prior vascular pathologies.

Venkat Poornima P   Chopp Michael M   Zacharek Alex A   Cui Chengcheng C   Zhang Li L   Li Qingjiang Q   Lu Mei M   Zhang Talan T   Liu Amy A   Chen Jieli J  

Neurobiology of aging 20161119


We investigated cognitive function, axonal/white matter (WM) changes and glymphatic function of vascular dementia using a multiple microinfarction (MMI) model in retired breeder (RB) rats. The MMI model induces significant (p < 0.05) cognitive decline that worsens with age starting at 2 weeks, which persists until at least 6 weeks after MMI. RB rats subjected to MMI exhibit significant axonal/WM damage identified by decreased myelin thickness, oligodendrocyte progenitor cell numbers, axon densit  ...[more]

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