IL-17-receptor-associated adaptor Act1 directly stabilizes mRNAs to mediate IL-17 inflammatory signaling

IL-17 受体相关衔接子 Act1 直接稳定 mRNA 以介导 IL-17 炎症信号传导

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作者：Tomasz Herjan, Lingzi Hong, Jodi Bubenik, Katarzyna Bulek, Wen Qian, Caini Liu, Xiao Li, Xing Chen, Hui Yang, Suidong Ouyang, Hao Zhou, Junjie Zhao, Kommireddy Vasu, Eric Cockman, Mark Aronica, Kewal Asosingh, Donny D Licatalosi, Jun Qin, Paul L Fox, Thomas A Hamilton, Donna Driscoll, Xiaoxia Li

期刊：	Nature Immunology	影响因子：	27.700
时间：	2018	起止号：	2018 Apr;19(4):354-365.
doi：	10.1038/s41590-018-0071-9	方法学：	FCM、IF、IHC-P、WB
靶点：	ELAV1	研究方向：	信号转导
信号通路：	Immunology/Inflammation

Abstract

Mechanisms that degrade inflammatory mRNAs are well known; however, stabilizing mechanisms are poorly understood. Here, we show that Act1, an interleukin-17 (IL-17)-receptor-complex adaptor, binds and stabilizes mRNAs encoding key inflammatory proteins. The Act1 SEFIR domain binds a stem-loop structure, the SEFIR-binding element (SBE), in the 3' untranslated region (UTR) of Cxcl1 mRNA, encoding an inflammatory chemokine. mRNA-bound Act1 directs formation of three compartmentally distinct RNA-protein complexes (RNPs) that regulate three disparate events in inflammatory-mRNA metabolism: preventing mRNA decay in the nucleus, inhibiting mRNA decapping in P bodies and promoting translation. SBE RNA aptamers decreased IL-17-mediated mRNA stabilization in vitro, IL-17-induced skin inflammation and airway inflammation in a mouse asthma model, thus providing a therapeutic strategy for autoimmune diseases. These results reveal a network in which Act1 assembles RNPs on the 3' UTRs of select mRNAs and consequently controls receptor-mediated mRNA stabilization and translation during inflammation.

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