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可互换接头调节线粒体动力蛋白的组装以进行膜分裂。

Interchangeable adaptors regulate mitochondrial dynamin assembly for membrane scission.

机构信息

Department of Biochemistry, University of Utah School of Medicine, Salt Lake City, UT 84112, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Apr 9;110(15):E1342-51. doi: 10.1073/pnas.1300855110. Epub 2013 Mar 25.

Abstract

Mitochondrial fission is mediated by the dynamin-related GTPases Dnm1/Drp1 (yeast/mammals), which form spirals around constricted sites on mitochondria. Additional membrane-associated adaptor proteins (Fis1, Mdv1, Mff, and MiDs) are required to recruit these GTPases from the cytoplasm to the mitochondrial surface. Whether these adaptors participate in both GTPase recruitment and membrane scission is not known. Here we use a yeast strain lacking all fission proteins to identify the minimal combinations of GTPases and adaptors sufficient for mitochondrial fission. Although Fis1 is dispensable for fission, membrane-anchored Mdv1, Mff, or MiDs paired individually with their respective GTPases are sufficient to divide mitochondria. In addition to their role in Drp1 membrane recruitment, MiDs coassemble with Drp1 in vitro. The resulting heteropolymer adopts a dramatically different structure with a narrower diameter than Drp1 homopolymers assembled in isolation. This result demonstrates that an adaptor protein alters the architecture of a mitochondrial dynamin GTPase polymer in a manner that could facilitate membrane constriction and severing activity.

摘要

线粒体的分裂是由与动力蛋白相关的 GTP 酶 Dnm1/Drp1(酵母/哺乳动物)介导的,它们在被收缩的线粒体部位周围形成螺旋。需要额外的膜相关衔接蛋白(Fis1、Mdv1、Mff 和 MiDs)将这些 GTP 酶从细胞质招募到线粒体表面。这些衔接蛋白是否参与 GTP 酶的招募和膜分裂尚不清楚。在这里,我们使用一种缺乏所有分裂蛋白的酵母菌株来鉴定对于线粒体分裂来说,GTP 酶和衔接蛋白的最小组合。虽然 Fis1 对于分裂不是必需的,但单独与各自的 GTP 酶结合的膜锚定的 Mdv1、Mff 或 MiDs 足以分裂线粒体。除了在 Drp1 膜募集中的作用外,MiDs 还在体外与 Drp1 共组装。由此产生的异聚体的结构明显不同,其直径比单独组装的 Drp1 同聚体更窄。这一结果表明,衔接蛋白以一种可能促进膜收缩和分裂活性的方式改变了线粒体动力蛋白 GTP 酶聚合物的结构。

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