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线粒体如何融合。

How mitochondria fuse.

作者信息

Meeusen Shelly L, Nunnari Jodi

机构信息

Department of Molecular and Cellular Biology, University of California-Davis, 1 Shields Avenue, Davis, CA 95616, USA.

出版信息

Curr Opin Cell Biol. 2005 Aug;17(4):389-94. doi: 10.1016/j.ceb.2005.06.014.

Abstract

Mitochondrial fusion is unique; no paradigm exists to explain how two sets of compositionally distinct membranes become coordinately fused. Genetic approaches coupled with in vivo observations of mitochondrial dynamics and morphology have identified the machinery involved in mitochondrial fusion but these approaches alone yield limited mechanistic insight. The recent recapitulation of mitochondrial fusion in vitro has allowed the fusion process to be dissected into two mechanistically distinct, resolvable steps: outer membrane fusion and inner membrane fusion. Outer membrane fusion requires homotypic trans interactions of the ancient dynamin-related GTPase Fzo1, the proton-gradient component of the inner membrane electrical potential, and low levels of GTP hydrolysis. Fusion of inner membranes requires the electrical component (Deltapsi) of the inner membrane electrical potential and elevated levels of GTP hydrolysis. Regulation of mitochondrial fusion is likely to involve transcript processing in mammalian cells as well as variation in the level of fusion proteins in a given cell; slight changes in the electrical potential of the inner membrane may also serve to fine-tune fusion rates. Mitochondrial fusion components also serve to protect cells against apoptosis through mechanisms that are largely unknown. Resolving the mechanism of mitochondrial fusion will provide insight into the role of fusion components in apoptosis.

摘要

线粒体融合是独特的;目前尚无范例来解释两组组成不同的膜如何协调融合。遗传学方法与线粒体动力学和形态学的体内观察相结合,已确定了参与线粒体融合的机制,但仅靠这些方法获得的机制性见解有限。最近体外线粒体融合的重现使得融合过程能够被分解为两个机制上不同、可解析的步骤:外膜融合和内膜融合。外膜融合需要古老的动力蛋白相关GTP酶Fzo1的同型反式相互作用、内膜电势的质子梯度成分以及低水平的GTP水解。内膜融合需要内膜电势的电成分(ΔΨ)和高水平的GTP水解。线粒体融合的调节可能涉及哺乳动物细胞中的转录加工以及给定细胞中融合蛋白水平的变化;内膜电势的轻微变化也可能用于微调融合速率。线粒体融合成分还通过很大程度上未知的机制保护细胞免受凋亡。解析线粒体融合机制将有助于深入了解融合成分在凋亡中的作用。

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