| Literature DB >> 32362325 |
Naganari Ohkura1, Yoshiaki Yasumizu2, Yohko Kitagawa3, Atsushi Tanaka1, Yamami Nakamura3, Daisuke Motooka4, Shota Nakamura4, Yukinori Okada5, Shimon Sakaguchi6.
Abstract
The contribution of FOXP3-expressing naturally occurring regulatory T (Treg) cells to common polygenic autoimmune diseases remains ambiguous. Here, we characterized genome-wide epigenetic profiles (CpG methylation and histone modifications) of human Treg and conventional T (Tconv) cells in naive and activated states. We found that single-nucleotide polymorphisms (SNPs) associated with common autoimmune diseases were predominantly enriched in CpG demethylated regions (DRs) specifically present in naive Treg cells but much less enriched in activation-induced DRs common in Tconv and Treg cells. Naive Treg cell-specific DRs were largely included in Treg cell-specific super-enhancers and closely associated with transcription and other epigenetic changes in naive and effector Treg cells. Thus, naive Treg cell-specific CpG hypomethylation had a key role in controlling Treg cell-specific gene transcription and epigenetic modification. The results suggest possible contribution of altered function or development of natural Treg cells to the susceptibility to common autoimmune diseases.Entities:
Keywords: CD25; CTLA-4; DNA methylation; FoxP3; SNPs; autoimmune diseases; epigenome; genetic susceptibility; regulatory T cells; super-enhancer
Year: 2020 PMID: 32362325 DOI: 10.1016/j.immuni.2020.04.006
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745