PELI2 is a negative regulator of STING signaling that is dynamically repressed during viral infection

IF 14.5 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Christopher Ritchie, Lingyin Li
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引用次数: 0

Abstract

The innate immune cGAS-STING pathway is activated by cytosolic double-stranded DNA (dsDNA), a ubiquitous danger signal, to produce interferon, a potent anti-viral and anti-cancer cytokine. However, STING activation must be tightly controlled because aberrant interferon production leads to debilitating interferonopathies. Here, we discover PELI2 as a crucial negative regulator of STING. Mechanistically, PELI2 inhibits the transcription factor IRF3 by binding to phosphorylated Thr354 and Thr356 on the C-terminal tail of STING, leading to ubiquitination and inhibition of the kinase TBK1. PELI2 sets a threshold for STING activation that tolerates low levels of cytosolic dsDNA, such as that caused by silenced TREX1, RNASEH2B, BRCA1, or SETX. When this threshold is reached, such as during viral infection, STING-induced interferon production temporarily downregulates PELI2, creating a positive feedback loop allowing a robust immune response. Lupus patients have insufficient PELI2 levels and high basal interferon production, suggesting that PELI2 dysregulation may drive the onset of lupus and other interferonopathies.

Abstract Image

PELI2 是 STING 信号的负调控因子,在病毒感染期间受到动态抑制
先天性免疫 cGAS-STING 通路被细胞膜双链 DNA(dsDNA)--一种无处不在的危险信号--激活,产生干扰素--一种有效的抗病毒和抗癌细胞因子。然而,STING 的激活必须受到严格控制,因为干扰素的异常产生会导致令人衰弱的干扰素病。在这里,我们发现 PELI2 是 STING 的一个重要负调控因子。从机理上讲,PELI2 通过与 STING C 端尾巴上磷酸化的 Thr354 和 Thr356 结合,导致泛素化和抑制激酶 TBK1,从而抑制转录因子 IRF3。PELI2 为 STING 的激活设定了一个阈值,该阈值可容忍低水平的细胞质 dsDNA,例如由沉默的 TREX1、RNASEH2B、BRCA1 或 SETX 引起的低水平 dsDNA。当达到这一阈值时,例如在病毒感染期间,STING 诱导的干扰素产生会暂时下调 PELI2,从而形成一个正反馈回路,产生强有力的免疫反应。红斑狼疮患者的 PELI2 水平不足,而基础干扰素产生量却很高,这表明 PELI2 失调可能是红斑狼疮和其他干扰素病发病的驱动因素。
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来源期刊
Molecular Cell
Molecular Cell 生物-生化与分子生物学
CiteScore
26.00
自引率
3.80%
发文量
389
审稿时长
1 months
期刊介绍: Molecular Cell is a companion to Cell, the leading journal of biology and the highest-impact journal in the world. Launched in December 1997 and published monthly. Molecular Cell is dedicated to publishing cutting-edge research in molecular biology, focusing on fundamental cellular processes. The journal encompasses a wide range of topics, including DNA replication, recombination, and repair; Chromatin biology and genome organization; Transcription; RNA processing and decay; Non-coding RNA function; Translation; Protein folding, modification, and quality control; Signal transduction pathways; Cell cycle and checkpoints; Cell death; Autophagy; Metabolism.
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