mRNA destabilization by BTG1 and BTG2 maintains T cell quiescence

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Authors: Soo Seok Hwang ; Jaechul Lim ; Zhibin Yu ; Philip Kong ; Esen Sefik ; Hao Xu ; Christian C D Harman ; Lark Kyun Kim ; Gap Ryol Lee ; Hua-Bing Li ; Richard A Flavell

MeSH: Animals ; Cells, Cultured ; Immediate-Early Proteins / genetics ; Immediate-Early Proteins / physiology* ; Lymphocyte Activation* ; Mice ; Mice, Knockout ; Neoplasm Proteins / genetics ; Neoplasm Proteins / physiology* ; Polyadenylation ; RNA Stability* ; RNA, Messenger / chemistry* ; T-Lymphocytes / immunology* ; Tumor Suppressor Proteins / genetics ; Tumor Suppressor Proteins / physiology*

Abstract: T cells maintain a quiescent state prior to activation. As inappropriate T cell activation can cause disease, T cell quiescence must be preserved. Despite its importance, the mechanisms underlying the "quiescent state" remain elusive. Here, we identify BTG1 and BTG2 (BTG1/2) as factors responsible for T cell quiescence. BTG1/2-deficient T cells show an increased proliferation and spontaneous activation due to a global increase in messenger RNA (mRNA) abundance, which reduces the threshold to activation. BTG1/2 deficiency leads to an increase in polyadenylate tail length, resulting in a greater mRNA half-life. Thus, BTG1/2 promote the deadenylation and degradation of mRNA to secure T cell quiescence. Our study reveals a key mechanism underlying T cell quiescence and suggests that low mRNA abundance is a crucial feature for maintaining quiescence.

Appears in Collections:: 1. College of Medicine (의과대학) > BioMedical Science Institute (의생명과학부) > 1. Journal Papers

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