人类髓样细胞中的DNA炎性小体由NLRP3上游的STING-细胞死亡程序启动。

The DNA Inflammasome in Human Myeloid Cells Is Initiated by a STING-Cell Death Program Upstream of NLRP3.

作者信息

Gaidt Moritz M, Ebert Thomas S, Chauhan Dhruv, Ramshorn Katharina, Pinci Francesca, Zuber Sarah, O'Duill Fionan, Schmid-Burgk Jonathan L, Hoss Florian, Buhmann Raymund, Wittmann Georg, Latz Eicke, Subklewe Marion, Hornung Veit

机构信息

Gene Center and Department of Biochemistry, Ludwig-Maximilians-Universität München, 81377 Munich, Germany.

Institute of Innate Immunity, University Hospital, University of Bonn, 53127 Bonn, Germany.

出版信息

Cell. 2017 Nov 16;171(5):1110-1124.e18. doi: 10.1016/j.cell.2017.09.039. Epub 2017 Oct 12.

DOI:10.1016/j.cell.2017.09.039

PMID:29033128

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5901709/

Abstract

Detection of cytosolic DNA constitutes a central event in the context of numerous infectious and sterile inflammatory conditions. Recent studies have uncovered a bipartite mode of cytosolic DNA recognition, in which the cGAS-STING axis triggers antiviral immunity, whereas AIM2 triggers inflammasome activation. Here, we show that AIM2 is dispensable for DNA-mediated inflammasome activation in human myeloid cells. Instead, detection of cytosolic DNA by the cGAS-STING axis induces a cell death program initiating potassium efflux upstream of NLRP3. Forward genetics identified regulators of lysosomal trafficking to modulate this cell death program, and subsequent studies revealed that activated STING traffics to the lysosome, where it triggers membrane permeabilization and thus lysosomal cell death (LCD). Importantly, the cGAS-STING-NLRP3 pathway constitutes the default inflammasome response during viral and bacterial infections in human myeloid cells. We conclude that targeting the cGAS-STING-LCD-NLRP3 pathway will ameliorate pathology in inflammatory conditions that are associated with cytosolic DNA sensing.

摘要

在众多感染性和无菌性炎症情况下，胞质DNA的检测是一个核心事件。最近的研究发现了一种双链模式的胞质DNA识别方式，其中cGAS-STING轴触发抗病毒免疫，而AIM2触发炎性小体激活。在这里，我们表明在人类髓系细胞中，DNA介导的炎性小体激活不需要AIM2。相反，cGAS-STING轴对胞质DNA的检测会诱导一种细胞死亡程序，该程序在NLRP3上游引发钾离子外流。正向遗传学鉴定出溶酶体运输的调节因子来调控这种细胞死亡程序，随后的研究表明，激活的STING会运输到溶酶体，在那里它会触发膜通透性增加，从而导致溶酶体细胞死亡（LCD）。重要的是，cGAS-STING-NLRP3途径构成了人类髓系细胞在病毒和细菌感染期间默认的炎性小体反应。我们得出结论，靶向cGAS-STING-LCD-NLRP3途径将改善与胞质DNA感知相关的炎症性疾病的病理状况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a257/5901709/43df4d91b60f/emss-77020-f001.jpg

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人类髓样细胞中的DNA炎性小体由NLRP3上游的STING-细胞死亡程序启动。

The DNA Inflammasome in Human Myeloid Cells Is Initiated by a STING-Cell Death Program Upstream of NLRP3.

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