ROS-dependent S-palmitoylation activates cleaved and intact gasdermin D

IF 50.5 1区 综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES Nature Pub Date : 2024-04-10 DOI:10.1038/s41586-024-07373-5
Gang Du, Liam B. Healy, Liron David, Caitlin Walker, Tarick J. El-Baba, Corinne A. Lutomski, Byoungsook Goh, Bowen Gu, Xiong Pi, Pascal Devant, Pietro Fontana, Ying Dong, Xiyu Ma, Rui Miao, Arumugam Balasubramanian, Robbins Puthenveetil, Anirban Banerjee, Hongbo R. Luo, Jonathan C. Kagan, Sungwhan F. Oh, Carol V. Robinson, Judy Lieberman, Hao Wu
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Abstract

Gasdermin D (GSDMD) is the common effector for cytokine secretion and pyroptosis downstream of inflammasome activation and was previously shown to form large transmembrane pores after cleavage by inflammatory caspases to generate the GSDMD N-terminal domain (GSDMD-NT)1–10. Here we report that GSDMD Cys191 is S-palmitoylated and that palmitoylation is required for pore formation. S-palmitoylation, which does not affect GSDMD cleavage, is augmented by mitochondria-generated reactive oxygen species (ROS). Cleavage-deficient GSDMD (D275A) is also palmitoylated after inflammasome stimulation or treatment with ROS activators and causes pyroptosis, although less efficiently than palmitoylated GSDMD-NT. Palmitoylated, but not unpalmitoylated, full-length GSDMD induces liposome leakage and forms a pore similar in structure to GSDMD-NT pores shown by cryogenic electron microscopy. ZDHHC5 and ZDHHC9 are the major palmitoyltransferases that mediate GSDMD palmitoylation, and their expression is upregulated by inflammasome activation and ROS. The other human gasdermins are also palmitoylated at their N termini. These data challenge the concept that cleavage is the only trigger for GSDMD activation. They suggest that reversible palmitoylation is a checkpoint for pore formation by both GSDMD-NT and intact GSDMD that functions as a general switch for the activation of this pore-forming family. Gasdermin D Cys191 is S-palmitoylated, and palmitoylation is required for pore formation.

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依赖于 ROS 的 S-棕榈酰化可激活裂解的和完整的 gasdermin D
Gasdermin D(GSDMD)是炎性细胞活化下游细胞因子分泌和脓毒症的共同效应物,以前的研究表明它在被炎性 Caspase 酶裂解生成 GSDMD N 端结构域(GSDMD-NT)1-10 时会形成大的跨膜孔。在这里,我们报告了 GSDMD Cys191 的 S-棕榈酰化,而棕榈酰化是孔形成所必需的。S-棕榈酰化不会影响 GSDMD 的裂解,但线粒体产生的活性氧(ROS)会增强其作用。令人惊讶的是,裂解缺陷的 D275A GSDMD 在炎症小体刺激或 ROS 激活剂处理后也会发生棕榈酰化,并导致热蛋白沉积,但其效率低于棕榈酰化的 GSDMD-NT。棕榈酰化而非非棕榈酰化的全长 GSDMD 可诱导脂质体渗漏,并形成与低温电子显微镜显示的 GSDMD-NT 孔结构相似的孔。其他人类 gasdermins 的 N 端也存在棕榈酰化。这些数据对 "裂解是 GSDMD 激活的唯一触发因素 "这一观点提出了质疑。它们表明,可逆棕榈酰化是 GSDMD-NT 和完整 GSDMD 形成孔隙的一个检查点,是激活这一孔隙形成家族的一般开关。
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来源期刊
Nature
Nature 综合性期刊-综合性期刊
CiteScore
90.00
自引率
1.20%
发文量
3652
审稿时长
3 months
期刊介绍: Nature is a prestigious international journal that publishes peer-reviewed research in various scientific and technological fields. The selection of articles is based on criteria such as originality, importance, interdisciplinary relevance, timeliness, accessibility, elegance, and surprising conclusions. In addition to showcasing significant scientific advances, Nature delivers rapid, authoritative, insightful news, and interpretation of current and upcoming trends impacting science, scientists, and the broader public. The journal serves a dual purpose: firstly, to promptly share noteworthy scientific advances and foster discussions among scientists, and secondly, to ensure the swift dissemination of scientific results globally, emphasizing their significance for knowledge, culture, and daily life.
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