| Literature DB >> 35939687 |
Chenbo Ding1,2, Hao Xu3, Zhibin Yu1,2, Manolis Roulis3, Rihao Qu3,4,5, Jing Zhou1,2, Joonseok Oh6,7, Jason Crawford6,7,8, Yimeng Gao9,10,11, Ruaidhrí Jackson3, Esen Sefik3, Simiao Li3, Zheng Wei3, Mathias Skadow3, Zhinan Yin12,13, Xinshou Ouyang14, Lei Wang1, Qiang Zou1, Bing Su1,2, Weiguo Hu1, Richard A Flavell3,15, Hua-Bing Li1,2.
Abstract
γδ T cells are an abundant T cell population at the mucosa and are important in providing immune surveillance as well as maintaining tissue homeostasis. However, despite γδ T cells' origin in the thymus, detailed mechanisms regulating γδ T cell development remain poorly understood. N6-methyladenosine (m6A) represents one of the most common posttranscriptional modifications of messenger RNA (mRNA) in mammalian cells, but whether it plays a role in γδ T cell biology is still unclear. Here, we show that depletion of the m6A demethylase ALKBH5 in lymphocytes specifically induces an expansion of γδ T cells, which confers enhanced protection against gastrointestinal Salmonella typhimurium infection. Mechanistically, loss of ALKBH5 favors the development of γδ T cell precursors by increasing the abundance of m6A RNA modification in thymocytes, which further reduces the expression of several target genes including Notch signaling components Jagged1 and Notch2. As a result, impairment of Jagged1/Notch2 signaling contributes to enhanced proliferation and differentiation of γδ T cell precursors, leading to an expanded mature γδ T cell repertoire. Taken together, our results indicate a checkpoint role of ALKBH5 and m6A modification in the regulation of γδ T cell early development.Entities:
Keywords: ALKBH5; Jagged1/Notch2 signaling; RNA m6A modification; developmental checkpoint; γδ T cell development
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Year: 2022 PMID: 35939687 PMCID: PMC9388086 DOI: 10.1073/pnas.2203318119
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 12.779