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• W4281383144 abstract "Abstract Alzheimer’s disease (AD) has been associated with cardiovascular and cerebrovascular risk factors (CVRFs) during middle age and later and is frequently accompanied by cerebrovascular pathology at death. An interaction between CVRFs and genetic variants might explain the pathogenesis. Genome-wide, gene by CVRF interaction analyses for AD, in 6568 patients and 8101 controls identified FMNL2 ( p = 6.6 × 10 –7 ). A significant increase in FMNL2 expression was observed in the brains of patients with brain infarcts and AD pathology and was associated with amyloid and phosphorylated tau deposition. FMNL2 was also prominent in astroglia in AD among those with cerebrovascular pathology. Amyloid toxicity in zebrafish increased fmnl2a expression in astroglia with detachment of astroglial end feet from blood vessels. Knockdown of fmnl2a prevented gliovascular remodeling, reduced microglial activity and enhanced amyloidosis. APP/PS1dE9 AD mice also displayed increased Fmnl2 expression and reduced the gliovascular contacts independent of the gliotic response. Based on this work, we propose that FMNL2 regulates pathology-dependent plasticity of the blood–brain-barrier by controlling gliovascular interactions and stimulating the clearance of extracellular aggregates. Therefore, in AD cerebrovascular risk factors promote cerebrovascular pathology which in turn, interacts with FMNL2 altering the normal astroglial-vascular mechanisms underlying the clearance of amyloid and tau increasing their deposition in brain." @default.
• W4281383144 created "2022-05-25" @default.
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• W4281383144 date "2022-05-24" @default.
• W4281383144 modified "2023-10-15" @default.
• W4281383144 title "FMNL2 regulates gliovascular interactions and is associated with vascular risk factors and cerebrovascular pathology in Alzheimer’s disease" @default.
• W4281383144 cites W1767010801 @default.
• W4281383144 cites W1835461481 @default.
• W4281383144 cites W1908991493 @default.
• W4281383144 cites W1969619562 @default.
• W4281383144 cites W1969712562 @default.
• W4281383144 cites W1978116054 @default.
• W4281383144 cites W1986091865 @default.
• W4281383144 cites W2005204638 @default.
• W4281383144 cites W2009154081 @default.
• W4281383144 cites W2009869050 @default.
• W4281383144 cites W2018337921 @default.
• W4281383144 cites W2025871751 @default.
• W4281383144 cites W2028546773 @default.
• W4281383144 cites W2043522411 @default.
• W4281383144 cites W2044447672 @default.
• W4281383144 cites W2046081464 @default.
• W4281383144 cites W2047779091 @default.
• W4281383144 cites W2047997229 @default.
• W4281383144 cites W2049733019 @default.
• W4281383144 cites W2053937456 @default.
• W4281383144 cites W2066630911 @default.
• W4281383144 cites W2072890764 @default.
• W4281383144 cites W2080097564 @default.
• W4281383144 cites W2081458774 @default.
• W4281383144 cites W2083736189 @default.
• W4281383144 cites W2086501057 @default.
• W4281383144 cites W2088642279 @default.
• W4281383144 cites W2089936534 @default.
• W4281383144 cites W2095535243 @default.
• W4281383144 cites W2102213696 @default.
• W4281383144 cites W2113179909 @default.
• W4281383144 cites W2115017507 @default.
• W4281383144 cites W2119519240 @default.
• W4281383144 cites W2124681501 @default.
• W4281383144 cites W2125411036 @default.
• W4281383144 cites W2128823466 @default.
• W4281383144 cites W2133520037 @default.
• W4281383144 cites W2135374418 @default.
• W4281383144 cites W2138023910 @default.
• W4281383144 cites W2138482871 @default.
• W4281383144 cites W2142160461 @default.
• W4281383144 cites W2151288448 @default.
• W4281383144 cites W2152907424 @default.
• W4281383144 cites W2162006322 @default.
• W4281383144 cites W2163225965 @default.
• W4281383144 cites W2202769705 @default.
• W4281383144 cites W2327513687 @default.
• W4281383144 cites W2413052180 @default.
• W4281383144 cites W2465803533 @default.
• W4281383144 cites W2470626250 @default.
• W4281383144 cites W2471197622 @default.
• W4281383144 cites W2510973425 @default.
• W4281383144 cites W2512788553 @default.
• W4281383144 cites W2531904292 @default.
• W4281383144 cites W2538431692 @default.
• W4281383144 cites W2543174917 @default.
• W4281383144 cites W2567096679 @default.
• W4281383144 cites W2580671663 @default.
• W4281383144 cites W2610878393 @default.
• W4281383144 cites W2612655633 @default.
• W4281383144 cites W2735124694 @default.
• W4281383144 cites W2746850238 @default.
• W4281383144 cites W2751659948 @default.
• W4281383144 cites W2756319919 @default.
• W4281383144 cites W2758846139 @default.
• W4281383144 cites W2762435278 @default.
• W4281383144 cites W2766294837 @default.
• W4281383144 cites W2784273980 @default.
• W4281383144 cites W2786608785 @default.

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