Interferon induction by STING requires its translocation to the late endosomes.

IF 3.6 3区生物学 Q3 CELL BIOLOGY

Traffic Pub Date : 2023-12-01 Epub Date: 2023-09-02 DOI:10.1111/tra.12918

Chenyao Wang, Nikhil Sharma, Patricia M Kessler, Ganes C Sen

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Abstract

To combat microbial infections, mammalian cells use a variety of innate immune response pathways to induce synthesis of anti-microbial proteins. The cGAS/STING pathway recognizes cytoplasmic viral or cellular DNA to elicit signals that lead to type I interferon and other cytokine synthesis. cGAMP, synthesized by DNA-activated cGAS, activates the ER-associated protein, STING, which oligomerizes and translocates to other intracellular membrane compartments to trigger different branches of signaling. We have reported that, in the ER, EGFR-mediated phosphorylation of Tyr245 of STING is required for its transit to the late endosomes, where it recruits and activates the transcription factor IRF3 required for IFN induction. In the current study, we inquired whether STING Tyr245 phosphorylation per se or STING's location in the late endosomes was critical for its ability to recruit IRF3 and induce IFN. Using pharmacological inhibitors or genetic ablation of proteins that are essential for specific steps of STING trafficking, we demonstrated that the presence of STING in the late endosomal membranes, even without Tyr245 phosphorylation, was sufficient for IRF3-mediated IFN induction.

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STING诱导干扰素需要将其转移到晚期内体。

为了对抗微生物感染，哺乳动物细胞利用各种先天免疫反应途径诱导抗微生物蛋白的合成。cGAS/STING途径识别细胞质病毒或细胞DNA，以引发导致I型干扰素和其他细胞因子合成的信号。cGAMP由DNA激活的cGAS合成，激活ER相关蛋白STING，STING低聚并转移到其他细胞内膜区室，以触发不同的信号分支。我们已经报道，在ER中，EGFR介导的STING的Tyr245磷酸化是其转运到晚期内体所必需的，在那里它募集并激活IFN诱导所需的转录因子IRF3。在目前的研究中，我们询问STING Tyr245磷酸化本身或STING在晚期内体中的位置是否对其募集IRF3和诱导IFN的能力至关重要。使用药理学抑制剂或对STING运输特定步骤所必需的蛋白质进行基因消融，我们证明了STING在晚期内体膜中的存在，即使没有Tyr245磷酸化，也足以诱导IRF3介导的IFN。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Traffic 生物-细胞生物学

CiteScore

8.10

自引率

2.20%

发文量

审稿时长

2 months

期刊介绍： Traffic encourages and facilitates the publication of papers in any field relating to intracellular transport in health and disease. Traffic papers span disciplines such as developmental biology, neuroscience, innate and adaptive immunity, epithelial cell biology, intracellular pathogens and host-pathogen interactions, among others using any eukaryotic model system. Areas of particular interest include protein, nucleic acid and lipid traffic, molecular motors, intracellular pathogens, intracellular proteolysis, nuclear import and export, cytokinesis and the cell cycle, the interface between signaling and trafficking or localization, protein translocation, the cell biology of adaptive an innate immunity, organelle biogenesis, metabolism, cell polarity and organization, and organelle movement. All aspects of the structural, molecular biology, biochemistry, genetics, morphology, intracellular signaling and relationship to hereditary or infectious diseases will be covered. Manuscripts must provide a clear conceptual or mechanistic advance. The editors will reject papers that require major changes, including addition of significant experimental data or other significant revision. Traffic will consider manuscripts of any length, but encourages authors to limit their papers to 16 typeset pages or less.

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