Gene expression and chromatin accessibility comparison in iPSC-derived microglia in African, European, and Amerindian genomes in Alzheimer’s patients and controls

Author:

Moura SofiaORCID,Nasciben Luciana BertholimORCID,Ramirez Aura M.ORCID,Coombs Lauren,Rivero Joe,Van Booven Derek J.,DeRosa Brooke A.,Hamilton-Nelson Kara L.ORCID,Whitehead Patrice L.,Adams Larry D.,Starks Takiyah D.ORCID,Mena Pedro R.,Illanes-Manrique MaryenelaORCID,Tejada Sergio,Byrd Goldie S.ORCID,Cornejo-Olivas Mario R.ORCID,Feliciano-Astacio Briseida E.ORCID,Nuytemans KarenORCID,Wang Liyong,Pericak-Vance Margaret A.,Dykxhoorn Derek M.ORCID,Rajabli FaridORCID,Griswold Anthony J.,Young Juan I.,Vance Jeffery M.ORCID

Abstract

AbstractAlzheimer’s disease (AD) risk differs between population groups, with African Americans and Hispanics being the most affected groups compared to non-Hispanic Whites. Genetic factors contribute significant risk to AD, but the genetic regulatory architectures (GRA) have primarily been studied in Europeans. Many AD genes are expressed in microglia; thus, we explored the impact of genetic ancestry (Amerindian (AI), African (AF), and European (EU)) on the GRA in iPSC-derived microglia from 13 individuals (∼4 each with high global ancestry, AD and controls) through ATAC-seq and RNA-seq analyses. We identified several differentially accessible and expressed genes (2 and 10 AD-related, respectively) between ancestry groups. We also found a high correlation between the transcriptomes of iPSC-derived and brain microglia, supporting their use in human studies. This study provides valuable insights into genetically diverse microglia beyond the analysis of AD.

Publisher

Cold Spring Harbor Laboratory

Reference110 articles.

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