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Bax assembles into large ring‐like structures remodeling the mitochondrial outer membrane in apoptosis

机译:Bax组装成大的环状结构重塑细胞凋亡中的线粒体外膜

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摘要

The Bcl‐2 family proteins Bax and Bak are essential for the execution of many apoptotic programs. During apoptosis, Bax translocates to the mitochondria and mediates the permeabilization of the outer membrane, thereby facilitating the release of pro‐apoptotic proteins. Yet the mechanistic details of the Bax‐induced membrane permeabilization have so far remained elusive. Here, we demonstrate that activated Bax molecules, besides forming large and compact clusters, also assemble, potentially with other proteins including Bak, into ring‐like structures in the mitochondrial outer membrane. STED nanoscopy indicates that the area enclosed by a Bax ring is devoid of mitochondrial outer membrane proteins such as Tom20, Tom22, and Sam50. This strongly supports the view that the Bax rings surround an opening required for mitochondrial outer membrane permeabilization (MOMP). Even though these Bax assemblies may be necessary for MOMP, we demonstrate that at least in Drp1 knockdown cells, these assemblies are not sufficient for full cytochrome c release. Together, our super‐resolution data provide direct evidence in support of large Bax‐delineated pores in the mitochondrial outer membrane as being crucial for Bax‐mediated MOMP in cells.
机译:Bcl-2家族蛋白Bax和Bak对于执行许多凋亡程序至关重要。在凋亡过程中,Bax易位至线粒体并介导外膜的通透性,从而促进促凋亡蛋白的释放。到目前为止,Bax引起的膜通透性的机制细节仍然难以捉摸。在这里,我们证明了活化的Bax分子除了形成大而紧凑的簇外,还可能与其他蛋白质(包括Bak)组装到线粒体外膜的环状结构中。 STED纳米显微镜检查表明,被Bax环包围的区域没有线粒体外膜蛋白,例如Tom20,Tom22和Sam50。这强烈支持了Bax环围绕线粒体外膜通透性(MOMP)所需的开口的观点。即使这些Bax程序集对于MOMP可能是必需的,我们也证明至少在Drp1敲低细胞中,这些程序集不足以完全释放细胞色素c。总之,我们的超分辨率数据提供了直接的证据,证明线粒体外膜中大的Bax描绘的孔对于细胞中Bax介导的MOMP至关重要。

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