APOE4 accelerates advanced-stage vascular and neurodegenerative disorder in old Alzheimer's mice via cyclophilin A independently of amyloid-β.
Axel MontagneAngeliki Maria NikolakopoulouMikko T HuuskonenAbhay P SagareErica J LawsonDivna LazicSanket V RegeAlexandra GrondEdward ZunigaSamuel R BarnesJacob PrinceMeghana SagareChing-Ju HsuMary J LaDuRussell E JacobsBerislav V ZlokovicPublished in: Nature aging (2021)
Apolipoprotein E4 ( APOE4 ), the main susceptibility gene for Alzheimer's disease (AD), leads to vascular dysfunction, amyloid-β pathology, neurodegeneration and dementia. How these different pathologies contribute to advanced-stage AD remains unclear. Using aged APOE knock-in mice crossed with 5xFAD mice, we show that, compared to APOE3, APOE4 accelerates blood-brain barrier (BBB) breakdown, loss of cerebral blood flow, neuronal loss and behavioral deficits independently of amyloid-β. BBB breakdown was associated with activation of the cyclophilin A-matrix metalloproteinase-9 BBB-degrading pathway in pericytes. Suppression of this pathway improved BBB integrity and prevented further neuronal loss and behavioral deficits in APOE4;5FAD mice while having no effect on amyloid-β pathology. Thus, APOE4 accelerates advanced-stage BBB breakdown and neurodegeneration in Alzheimer's mice via the cyclophilin A pathway in pericytes independently of amyloid-β, which has implication for the pathogenesis and treatment of vascular and neurodegenerative disorder in AD.
Keyphrases
- blood brain barrier
- cognitive decline
- mild cognitive impairment
- high fat diet
- high fat diet induced
- cerebral ischemia
- traumatic brain injury
- type diabetes
- cerebral blood flow
- oxidative stress
- adipose tissue
- gene expression
- dna methylation
- wild type
- skeletal muscle
- metabolic syndrome
- genome wide
- cognitive impairment
- subarachnoid hemorrhage