Gasdermin D半胱氨酸残基协同控制其棕榈酰化介导的膜靶向和组装。

IF 9.4 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
EMBO Journal Pub Date : 2024-10-01 Epub Date: 2024-08-14 DOI:10.1038/s44318-024-00190-6
Eleonora Margheritis, Shirin Kappelhoff, John Danial, Nadine Gehle, Wladislaw Kohl, Rainer Kurre, Ayelén González Montoro, Katia Cosentino
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引用次数: 0

摘要

Gasdermin D(GSDMD)通过组装成能使质膜通透的低聚物来执行细胞死亡程序--热昏迷。在这里,我们通过单分子成像,阐明了尚不清楚的 Gasdermin D 孔组装机制以及半胱氨酸残基在 GSDMD 寡聚化中的作用。我们的研究表明,GSDMD 在膜上预组装成二聚体和三聚体构件,这些构件既可以插入膜中,也可以在插入膜前进一步组装成高阶寡聚体。GSDMD残基Cys39、Cys57和Cys192是参与GSDMD寡聚化的唯一相关半胱氨酸。Cys192 的 S-棕榈酰化与带负电荷的脂质的存在相结合,控制着 GSDMD 的膜靶向性。Cys39/57/192 同时突变为丙氨酸(Ala),而不是 Cys192 或 Cys39/57 一对单独的 Ala 突变,可完全阻止 GSDMD 插入人工膜以及质膜。最后,无论是 Cys192 还是 Cys39/Cys57 对都足以形成 GSDMD 二聚体/三聚体,但它们都是功能性高阶寡聚体形成所必需的。总之,我们的研究揭示了 Cys192 棕榈酰化介导的膜结合和 Cys39/57/192 介导的低聚物在 GSDMD 孔组装中的合作作用。这项研究支持这样一个模型,即 Gasdermin D 的寡聚化依赖于由特定半胱氨酸残基介导的两步机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Gasdermin D cysteine residues synergistically control its palmitoylation-mediated membrane targeting and assembly.

Gasdermin D (GSDMD) executes the cell death program of pyroptosis by assembling into oligomers that permeabilize the plasma membrane. Here, by single-molecule imaging, we elucidate the yet unclear mechanism of Gasdermin D pore assembly and the role of cysteine residues in GSDMD oligomerization. We show that GSDMD preassembles at the membrane into dimeric and trimeric building blocks that can either be inserted into the membrane, or further assemble into higher-order oligomers prior to insertion into the membrane. The GSDMD residues Cys39, Cys57, and Cys192 are the only relevant cysteines involved in GSDMD oligomerization. S-palmitoylation of Cys192, combined with the presence of negatively-charged lipids, controls GSDMD membrane targeting. Simultaneous Cys39/57/192-to-alanine (Ala) mutations, but not Ala mutations of Cys192 or the Cys39/57 pair individually, completely abolish GSDMD insertion into artificial membranes as well as into the plasma membrane. Finally, either Cys192 or the Cys39/Cys57 pair are sufficient to enable formation of GSDMD dimers/trimers, but they are all required for functional higher-order oligomer formation. Overall, our study unveils a cooperative role of Cys192 palmitoylation-mediated membrane binding and Cys39/57/192-mediated oligomerization in GSDMD pore assembly. This study supports a model in which Gasdermin D oligomerization relies on a two-step mechanism mediated by specific cysteine residues.

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来源期刊
EMBO Journal
EMBO Journal 生物-生化与分子生物学
CiteScore
18.90
自引率
0.90%
发文量
246
审稿时长
1.5 months
期刊介绍: The EMBO Journal has stood as EMBO's flagship publication since its inception in 1982. Renowned for its international reputation in quality and originality, the journal spans all facets of molecular biology. It serves as a platform for papers elucidating original research of broad general interest in molecular and cell biology, with a distinct focus on molecular mechanisms and physiological relevance. With a commitment to promoting articles reporting novel findings of broad biological significance, The EMBO Journal stands as a key contributor to advancing the field of molecular biology.
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