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SLFN2 protection of tRNAs from stress-induced cleavage is essential for T cell-mediated immunity

Authors :
Bruce Beutler
Lei Sun
Xiaoming Zhan
Duanwu Zhang
Emre E. Turer
Tao Yue
Xiaohong Li
Lijing Su
Jin Huk Choi
Takuma Misawa
Jiexia Quan
Eva Marie Y. Moresco
Darui Xu
Sara Hildebrand
Ruchi Jain
Kuan Wen Wang
Source :
Science (New York, N.Y.). 372(6543)
Publication Year :
2019

Abstract

A T cell sleeper agent against stress Considerable changes in cellular metabolism occur when T cells transition from a resting to an activated state. One side effect of this process is an increase in reactive oxygen species (ROS). These molecules potentiate T cell receptor (TCR) signaling but can also result in detrimental oxidative stress (see the Perspective by Su and Dutta). Yue et al. describe one mechanism by which T cells can resolve this contradiction. Using mice with a T cell-specific deficiency in Schlafen 2 (SLFN2), they found that this protein binds to and protects transfer RNAs from oxidative stress-induced cleavage by the ribonuclease angiogenin. This process is downstream of ROS generation, which allows activated T cells to maintain protein synthesis despite the ROS that would otherwise inhibit translation. Science , this issue p. eaba4220 ; see also p. 683

Details

ISSN :
10959203
Volume :
372
Issue :
6543
Database :
OpenAIRE
Journal :
Science (New York, N.Y.)
Accession number :
edsair.doi.dedup.....ea64c8fb3d2bff448b9e644ad42e44cd