GSDME 通过调节细胞焦亡、依赖 Drp1 瓜氨酸化的线粒体动态以及肠和肝中的能量平衡来促进 MASLD。
GSDME promotes MASLD by regulating pyroptosis, Drp1 citrullination-dependent mitochondrial dynamic, and energy balance in intestine and liver.
机构信息
Department of Pharmacy, Shanghai Tenth People's Hospital, School of Medicine, Tongji University, Shanghai, China.
Department of Clinical Research, Sichuan Clinical Research Center for Cancer, Sichuan Cancer Hospital & Institute, Sichuan Cancer Center, Affiliated Cancer Hospital of University of Electronic Science and Technology of China, Chengdu, China.
出版信息
Cell Death Differ. 2024 Nov;31(11):1467-1486. doi: 10.1038/s41418-024-01343-0. Epub 2024 Jul 16.
Dysregulated metabolism, cell death, and inflammation contribute to the development of metabolic dysfunction-associated steatohepatitis (MASH). Pyroptosis, a recently identified form of programmed cell death, is closely linked to inflammation. However, the precise role of pyroptosis, particularly gasdermin-E (GSDME), in MASH development remains unknown. In this study, we observed GSDME cleavage and GSDME-associated interleukin-1β (IL-1β)/IL-18 induction in liver tissues of MASH patients and MASH mouse models induced by a choline-deficient high-fat diet (CDHFD) or a high-fat/high-cholesterol diet (HFHC). Compared with wild-type mice, global GSDME knockout mice exhibited reduced liver steatosis, steatohepatitis, fibrosis, endoplasmic reticulum stress, lipotoxicity and mitochondrial dysfunction in CDHFD- or HFHC-induced MASH models. Moreover, GSDME knockout resulted in increased energy expenditure, inhibited intestinal nutrient absorption, and reduced body weight. In the mice with GSDME deficiency, reintroduction of GSDME in myeloid cells-rather than hepatocytes-mimicked the MASH pathologies and metabolic dysfunctions, as well as the changes in the formation of neutrophil extracellular traps and hepatic macrophage/monocyte subclusters. These subclusters included shifts in Tim4 or CD163 resident Kupffer cells, Ly6C pro-inflammatory monocytes, and Ly6CCCR2CX3CR1 patrolling monocytes. Integrated analyses of RNA sequencing and quantitative proteomics revealed a significant GSDME-dependent reduction in citrullination at the arginine-114 (R114) site of dynamin-related protein 1 (Drp1) during MASH. Mutation of Drp1 at R114 reduced its stability, impaired its ability to redistribute to mitochondria and regulate mitophagy, and ultimately promoted its degradation under MASH stress. GSDME deficiency reversed the de-citrullination of Drp1, preserved Drp1 stability, and enhanced mitochondrial function. Our study highlights the role of GSDME in promoting MASH through regulating pyroptosis, Drp1 citrullination-dependent mitochondrial function, and energy balance in the intestine and liver, and suggests that GSDME may be a potential therapeutic target for managing MASH.
代谢失调、细胞死亡和炎症导致代谢相关脂肪性肝炎(MASH)的发生。细胞程序性死亡的一种新形式——细胞焦亡与炎症密切相关。然而,细胞焦亡,特别是 Gasdermin-E(GSDME)在 MASH 发展中的确切作用仍不清楚。本研究观察到 MASH 患者肝组织中 GSDME 裂解和 GSDME 相关的白细胞介素-1β(IL-1β)/IL-18 的诱导,以及胆碱缺乏高脂饮食(CDHFD)或高脂高胆固醇饮食(HFHC)诱导的 MASH 小鼠模型。与野生型小鼠相比,全身性 GSDME 敲除小鼠在 CDHFD 或 HFHC 诱导的 MASH 模型中表现出肝脂肪变性、肝炎、纤维化、内质网应激、脂毒性和线粒体功能障碍减少。此外,GSDME 敲除导致能量消耗增加,抑制肠道营养吸收,体重减轻。在 GSDME 缺陷的小鼠中,髓细胞而非肝细胞中 GSDME 的重新引入模拟了 MASH 病理和代谢功能障碍,以及中性粒细胞胞外诱捕网和肝巨噬细胞/单核细胞亚群的变化。这些亚群包括 Tim4 或 CD163 驻留 Kupffer 细胞、Ly6C 促炎单核细胞和 Ly6CCCR2CX3CR1 巡逻单核细胞的变化。RNA 测序和定量蛋白质组学的综合分析显示,在 MASH 期间,动力相关蛋白 1(Drp1)的精氨酸-114(R114)位点的瓜氨酸化显著依赖于 GSDME。Drp1 在 R114 处的突变降低了其稳定性,损害了其向线粒体重分布和调节线粒体自噬的能力,并最终在 MASH 应激下促进其降解。GSDME 缺失逆转了 Drp1 的去瓜氨酸化,保持了 Drp1 的稳定性,并增强了线粒体功能。本研究强调了 GSDME 通过调节细胞焦亡、依赖 Drp1 瓜氨酸化的线粒体功能以及肠肝能量平衡在促进 MASH 中的作用,并表明 GSDME 可能是管理 MASH 的潜在治疗靶点。
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