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• W3206683634 abstract "The roles of APOEε4 and APOEε2—the strongest genetic risk and protective factors for Alzheimer’s disease—in glial responses remain elusive. We tested the hypothesis that APOE alleles differentially impact glial responses by investigating their effects on the glial transcriptome from elderly control brains with no neuritic amyloid plaques. We identified a cluster of microglial genes that are upregulated in APOEε4 and downregulated in APOEε2 carriers relative to APOEε3 homozygotes. This microglia-APOE cluster is enriched in phagocytosis—including TREM2 and TYROBP—and proinflammatory genes, and is also detectable in brains with frequent neuritic plaques. Next, we tested these findings in APOE knock-in mice exposed to acute (lipopolysaccharide challenge) and chronic (cerebral β-amyloidosis) insults and found that these mice partially recapitulate human APOE-linked expression patterns. Thus, the APOEε4 allele might prime microglia towards a phagocytic and proinflammatory state through an APOE–TREM2–TYROBP axis in normal aging as well as in Alzheimer’s disease. The authors found that the Alzheimer’s disease-linked APOEε4 allele may prime microglia towards a phagocytic and pro-inflammatory state in the normal aging brain, even before Alzheimer’s amyloid plaques and neurofibrillary tangles develop." @default.
• W3206683634 created "2021-10-25" @default.
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• W3206683634 date "2021-10-11" @default.
• W3206683634 modified "2023-10-14" @default.
• W3206683634 title "Effect of APOE alleles on the glial transcriptome in normal aging and Alzheimer’s disease" @default.
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• W3206683634 doi "https://doi.org/10.1038/s43587-021-00123-6" @default.
• W3206683634 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36199750" @default.
• W3206683634 hasPublicationYear "2021" @default.

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