ER membrane remodeling by targeting RTN4 induces pyroptosis to facilitate antitumor immune.

IF 13.6 1区 生物学 Q1 CELL BIOLOGY
Mei-Mei Zhao,Ting-Ting Ren,Jing-Kang Wang,Lu Yao,Ting-Ting Liu,Ji-Chao Zhang,Yang Liu,Lan Yuan,Dan Liu,Jiu-Hui Xu,Peng-Fei Tu,Xiao-Dong Tang,Ke-Wu Zeng
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引用次数: 0

Abstract

Pyroptosis is an identified programmed cell death that has been highly linked to endoplasmic reticulum (ER) dynamics. However, the crucial proteins for modulating dynamic ER membrane curvature change that trigger pyroptosis are currently not well understood. In this study, a biotin-labeled chemical probe of potent pyroptosis inducer α-mangostin (α-MG) was synthesized. Through protein microarray analysis, reticulon-4 (RTN4/Nogo), a crucial regulator of ER membrane curvature, was identified as a target of α-MG. We observed that chemically induced proteasome degradation of RTN4 by α-MG through recruiting E3 ligase UBR5 significantly enhances the pyroptosis phenotype in cancer cells. Interestingly, the downregulation of RTN4 expression significantly facilitated a dynamic remodeling of ER membrane curvature through a transition from tubules to sheets, consequently leading to rapid fusion of the ER with the cell plasma membrane. In particular, the ER-to-plasma membrane fusion process is supported by the observed translocation of several crucial ER markers to the "bubble" structures of pyroptotic cells. Furthermore, α-MG-induced RTN4 knockdown leads to PKM2-dependent conventional caspase-3/GSDME cleavages for pyroptosis progression. In vivo, we observed that chemical or genetic RTN4 knockdown significantly inhibited cancer cells growth, which further exhibited an antitumor immune response with anti-PD-1. In translational research, RTN4 high expression was closely correlated with the tumor metastasis and death of patients. Taken together, RTN4 plays a fundamental role in inducing pyroptosis through the modulation of ER membrane curvature remodeling, thus representing a prospective druggable target for anticancer immunotherapy.
通过靶向 RTN4 重塑 ER 膜,诱导热蛋白沉积,促进抗肿瘤免疫。
裂解病是一种已确定的程序性细胞死亡,与内质网(ER)的动力学有很大关系。然而,目前还不太清楚调节ER膜动态曲率变化从而引发裂解的关键蛋白。本研究合成了一种生物素标记的强效裂解诱导剂α-芒果苷(α-MG)化学探针。通过蛋白质微阵列分析,我们发现ER膜曲率的一个关键调节因子--reticulon-4(RTN4/Nogo)是α-MG的靶标。我们观察到,α-MG 通过招募 E3 连接酶 UBR5 化学诱导蛋白酶体降解 RTN4,显著增强了癌细胞的热休克表型。有趣的是,RTN4表达的下调极大地促进了ER膜曲率的动态重塑,从管状过渡到片状,从而导致ER与细胞质膜的快速融合。特别是,观察到一些重要的ER标记物转位到热休克细胞的 "气泡 "结构,支持了ER与质膜的融合过程。此外,α-MG 诱导的 RTN4 基因敲除导致 PKM2 依赖于传统的 Caspase-3/GSDME 裂解,从而促进了热凋亡的进展。在体内,我们观察到化学或基因敲除 RTN4 能显著抑制癌细胞的生长,并进一步表现出抗 PD-1 的抗肿瘤免疫反应。在转化研究中,RTN4的高表达与肿瘤转移和患者死亡密切相关。综上所述,RTN4通过调节ER膜曲率重塑在诱导热休克中发挥着基础性作用,因此是抗癌免疫疗法的潜在药物靶点。
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
Protein & Cell
Protein & Cell CELL BIOLOGY-
CiteScore
24.00
自引率
0.90%
发文量
1029
审稿时长
6-12 weeks
期刊介绍: Protein & Cell is a monthly, peer-reviewed, open-access journal focusing on multidisciplinary aspects of biology and biomedicine, with a primary emphasis on protein and cell research. It publishes original research articles, reviews, and commentaries across various fields including biochemistry, biophysics, cell biology, genetics, immunology, microbiology, molecular biology, neuroscience, oncology, protein science, structural biology, and translational medicine. The journal also features content on research policies, funding trends in China, and serves as a platform for academic exchange among life science researchers.
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