Contributions of genetic variation in astrocytes to cell and molecular mechanisms of risk and resilience to late onset Alzheimer's disease.

Lee, Hyo; Pearse, Richard V; Lish, Alexandra M; Pan, Cheryl; Augur, Zachary M; Terzioglu, Gizem; Gaur, Pallavi; Liao, Meichen; Fujita, Masashi; Tio, Earvin S; Duong, Duc M; Felsky, Daniel; Seyfried, Nicholas T; Menon, Vilas; Bennett, David A; De Jager, Philip L; Young-Pearse, Tracy L

Lee, Hyo; Pearse, Richard V; Lish, Alexandra M; Pan, Cheryl; Augur, Zachary M; Terzioglu, Gizem; Gaur, Pallavi; Liao, Meichen; Fujita, Masashi; Tio, Earvin S; Duong, Duc M; Felsky, Daniel; Seyfried, Nicholas T; Menon, Vilas; Bennett, David A; De Jager, Philip L; Young-Pearse, Tracy L.

bioRxiv ; 2024 Jul 31.

Article en En | MEDLINE | ID: mdl-39211227

ABSTRACT

ABSTRACT

Reactive astrocytes are associated with Alzheimer's disease (AD), and several AD genetic risk variants are associated with genes highly expressed in astrocytes. However, the contribution of genetic risk within astrocytes to cellular processes relevant to the pathogenesis of AD remains ill-defined. Here we present a resource for studying AD genetic risk in astrocytes using a large collection of induced pluripotent stem cell (iPSC) lines from deeply phenotyped individuals with a range of neuropathological and cognitive outcomes. IPSC lines from forty-four individuals were differentiated into astrocytes followed by unbiased molecular profiling using RNA sequencing and tandem mass tag-mass spectrometry. We demonstrate the utility of this resource in examining gene- and pathway-level associations with clinical and neuropathological traits, as well as in analyzing genetic risk and resilience factors through parallel analyses of iPSC-astrocytes and brain tissue from the same individuals. Our analyses reveal that genes and pathways altered in iPSC-derived astrocytes from AD individuals are concordantly dysregulated in AD brain tissue. This includes increased prefoldin proteins, extracellular matrix factors, COPI-mediated trafficking components and reduced proteins involved in cellular respiration and fatty acid oxidation. Additionally, iPSC-derived astrocytes from individuals resilient to high AD neuropathology show elevated basal levels of interferon response proteins and increased secretion of interferon gamma. Correspondingly, higher polygenic risk scores for AD are associated with lower levels of interferon response proteins. This study establishes an experimental system that integrates genetic information with a heterogeneous set of iPSCs to identify genetic contributions to molecular pathways affecting AD risk and resilience.

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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Idioma: En Revista: BioRxiv Año: 2024 Tipo del documento: Article Pais de publicación: Estados Unidos

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