Alzheimer's disease transcriptional landscape in ex-vivo human microglia

Author:

Roussos Panos1ORCID,Kosoy Roman1,Fullard John1ORCID,Bendl Jaroslav1ORCID,Kleopoulos Steven1,Shao Zhiping1,Argyriou Stathis1,Mathur Deepika1,Vicari James1ORCID,Ma Yixuan1,Humphrey Jack1ORCID,Brophy Erica1,Raj Towfique2ORCID,Katsel Pavel1ORCID,Voloudakis Georgios1ORCID,Lee Donghoon1ORCID,Bennett David3,Haroutunian Vahram4ORCID,Hoffman Gabriel1ORCID

Affiliation:

1. Icahn School of Medicine at Mount Sinai

2. towfique.raj@mssm.edu

3. Rush University Medical Center

4. Mount Sinai and JJ Peters VA Medical Center

Abstract

Abstract Microglia are resident immune cells of the brain and are implicated in the etiology of Alzheimer’s Disease (AD) and other diseases. Yet the cellular and molecular processes regulating their function throughout the course of the disease are poorly understood. Here, we present the transcriptional landscape of primary microglia from 189 human postmortem brains, including 58 healthy aging individuals and 131 with a range of disease phenotypes, including 63 patients representing the full spectrum of clinical and pathological severity of AD. We identified transcriptional changes associated with multiple AD phenotypes, capturing the severity of dementia and neuropathological lesions. Transcript-level analyses identified additional genes with heterogeneous isoform usage and AD phenotypes. We identified changes in gene-gene coordination in AD, dysregulation of co-expression modules, and disease subtypes with distinct gene expression. Taken together, these data further our understanding of the key role of microglia in AD biology and nominate candidates for therapeutic intervention.

Publisher

Research Square Platform LLC

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