| Literature DB >> 34706222 |
Roshni Roy1, Senthilkumar Ramamoorthy2, Benjamin D Shapiro3, Mary Kaileh1, Dena Hernandez4, Dimitra Sarantopoulou1, Sampath Arepalli4, Sören Boller2, Amit Singh1, Arsun Bektas5, Jaekwan Kim1, Ann Zenobia Moore5, Toshiko Tanaka5, Julia McKelvey6, Linda Zukley6, Cuong Nguyen7, Tonya Wallace7, Christopher Dunn7, Robert Wersto7, William Wood8, Yulan Piao8, Kevin G Becker8, Christopher Coletta8, Supriyo De8, Jyoti Misra Sen9, Alexis Battle3, Nan-Ping Weng1, Rudolf Grosschedl2, Luigi Ferrucci5, Ranjan Sen10.
Abstract
Epigenetic reprogramming underlies specification of immune cell lineages, but patterns that uniquely define immune cell types and the mechanisms by which they are established remain unclear. Here, we identified lineage-specific DNA methylation signatures of six immune cell types from human peripheral blood and determined their relationship to other epigenetic and transcriptomic patterns. Sites of lineage-specific hypomethylation were associated with distinct combinations of transcription factors in each cell type. By contrast, sites of lineage-specific hypermethylation were restricted mostly to adaptive immune cells. PU.1 binding sites were associated with lineage-specific hypo- and hypermethylation in different cell types, suggesting that it regulates DNA methylation in a context-dependent manner. These observations indicate that innate and adaptive immune lineages are specified by distinct epigenetic mechanisms via combinatorial and context-dependent use of key transcription factors. The cell-specific epigenomics and transcriptional patterns identified serve as a foundation for future studies on immune dysregulation in diseases and aging. Published by Elsevier Inc.Entities:
Keywords: DNA methylation; epigenetics; gene expression; human immunity; innate cells; lymphocytes; transcription factors
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Year: 2021 PMID: 34706222 PMCID: PMC9190145 DOI: 10.1016/j.immuni.2021.10.001
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 43.474