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贴补修复可保护细胞免受小孔形成毒素 aerolysin 的侵害。

Patch repair protects cells from the small pore-forming toxin aerolysin.

机构信息

Department of Biological Sciences, Texas Tech University, Lubbock, TX 79409, USA.

出版信息

J Cell Sci. 2023 Apr 15;136(8). doi: 10.1242/jcs.261018. Epub 2023 Apr 20.

Abstract

Aerolysin family pore-forming toxins damage the membrane, but membrane repair responses used to resist them, if any, remain controversial. Four proposed membrane repair mechanisms include toxin removal by caveolar endocytosis, clogging by annexins, microvesicle shedding catalyzed by MEK, and patch repair. Which repair mechanism aerolysin triggers is unknown. Membrane repair requires Ca2+, but it is controversial if Ca2+ flux is triggered by aerolysin. Here, we determined Ca2+ influx and repair mechanisms activated by aerolysin. In contrast to what is seen with cholesterol-dependent cytolysins (CDCs), removal of extracellular Ca2+ protected cells from aerolysin. Aerolysin triggered sustained Ca2+ influx. Intracellular Ca2+ chelation increased cell death, indicating that Ca2+-dependent repair pathways were triggered. Caveolar endocytosis failed to protect cells from aerolysin or CDCs. MEK-dependent repair did not protect against aerolysin. Aerolysin triggered slower annexin A6 membrane recruitment compared to CDCs. In contrast to what is seen with CDCs, expression of the patch repair protein dysferlin protected cells from aerolysin. We propose aerolysin triggers a Ca2+-dependent death mechanism that obscures repair, and the primary repair mechanism used to resist aerolysin is patch repair. We conclude that different classes of bacterial toxins trigger distinct repair mechanisms.

摘要

aerolysin 家族的成孔毒素破坏膜,但用于抵抗它们的膜修复反应(如果有的话)仍然存在争议。提出了四种拟议的膜修复机制,包括 caveolar 胞吞作用去除毒素、膜联蛋白堵塞、MEK 催化的微泡脱落和补丁修复。aerolysin 触发哪种修复机制尚不清楚。膜修复需要 Ca2+,但 aerolysin 是否触发 Ca2+ 流仍存在争议。在这里,我们确定了 aerolysin 激活的 Ca2+ 内流和修复机制。与胆固醇依赖性细胞溶素 (CDCs) 不同,去除细胞外 Ca2+ 可保护细胞免受 aerolysin 的侵害。aerolysin 触发持续的 Ca2+内流。细胞内 Ca2+螯合增加细胞死亡,表明触发了 Ca2+依赖性修复途径。 caveolar 胞吞作用不能保护细胞免受 aerolysin 或 CDCs 的侵害。MEK 依赖性修复不能防止 aerolysin。与 CDCs 不同,补丁修复蛋白 dysferlin 的表达可保护细胞免受 aerolysin 的侵害。我们提出,aerolysin 触发一种掩盖修复的 Ca2+依赖性死亡机制,而抵抗 aerolysin 的主要修复机制是补丁修复。我们得出结论,不同类别的细菌毒素触发不同的修复机制。

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