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将贩卖与强大的线粒体中的融合和裂变联系起来。

Tying trafficking to fusion and fission at the mighty mitochondria.

机构信息

The Department of Biochemistry and Molecular Biology, The University of Nebraska Medical Center, Omaha, Nebraska.

The Fred and Pamela Buffett Cancer Center, The University of Nebraska Medical Center, Omaha, Nebraska.

出版信息

Traffic. 2018 Aug;19(8):569-577. doi: 10.1111/tra.12573. Epub 2018 May 11.

Abstract

The mitochondrion is a unique organelle that serves as the main site of ATP generation needed for energy in the cell. However, mitochondria also play essential roles in cell death through apoptosis and necrosis, as well as a variety of crucial functions related to stress regulation, autophagy, lipid synthesis and calcium storage. There is a growing appreciation that mitochondrial function is regulated by the dynamics of its membrane fusion and fission; longer, fused mitochondria are optimal for ATP generation, whereas fission of mitochondria facilitates mitophagy and cell division. Despite the significance of mitochondrial homeostasis for such crucial cellular events, the intricate regulation of mitochondrial fusion and fission is only partially understood. Until very recently, only a single mitochondrial fission protein had been identified. Moreover, only now have researchers turned to address the upstream machinery that regulates mitochondrial fusion and fission proteins. Herein, we review the known GTPases involved in mitochondrial fusion and fission, but also highlight recent studies that address the mechanisms by which these GTPases are regulated. In particular, we draw attention to a substantial new body of literature linking endocytic regulatory proteins, such as the retromer VPS35 cargo selection complex subunit, to mitochondrial homeostasis. These recent studies suggest that relationships and cross-regulation between endocytic and mitochondrial pathways may be more widespread than previously assumed.

摘要

线粒体是一种独特的细胞器,是细胞内产生能量所需的 ATP 的主要生成场所。然而,线粒体通过细胞凋亡和坏死,以及与应激调节、自噬、脂质合成和钙储存等各种关键功能相关,也起着至关重要的作用。人们越来越认识到,线粒体的功能受到其膜融合和裂变动力学的调节;较长的融合线粒体最有利于 ATP 的生成,而线粒体的裂变则有利于 mitophagy 和细胞分裂。尽管线粒体的动态平衡对于这些关键的细胞事件非常重要,但线粒体融合和裂变的复杂调节机制还只是部分了解。直到最近,才发现了一种单一的线粒体裂变蛋白。此外,研究人员才刚刚开始研究调节线粒体融合和裂变蛋白的上游机制。在这里,我们综述了已知参与线粒体融合和裂变的 GTPase,但也强调了最近的研究,这些研究探讨了这些 GTPase 是如何被调节的。特别是,我们提请注意大量新的文献,这些文献将内吞调节蛋白(如 retromer VPS35 货物选择复合物亚基)与线粒体的动态平衡联系起来。这些最近的研究表明,内吞和线粒体途径之间的关系和交叉调节可能比以前认为的更为广泛。

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