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剖析哺乳动物和果蝇电压依赖性阴离子通道功能的遗传策略。

Genetic strategies for dissecting mammalian and Drosophila voltage-dependent anion channel functions.

作者信息

Craigen William J, Graham Brett H

机构信息

Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX 77030, USA.

出版信息

J Bioenerg Biomembr. 2008 Jun;40(3):207-12. doi: 10.1007/s10863-008-9146-x.

Abstract

Voltage-dependent anion channels (VDACs), also known as mitochondrial porins, are a family of small pore-forming proteins of the mitochondrial outer membrane that are found in all eukaryotes. VDACs are thought to play important roles in the regulated flux of metabolites between the cytosolic and mitochondrial compartments, in overall energy metabolism via interactions with cytosolic kinases, and a debated role in programmed cell death (apoptosis). The mammalian genome contains three VDAC loci termed Vdac1, Vdac2, and Vdac3, raising the question as to what function each isoform may be performing. Based upon expression studies of the mouse VDACs in yeast, biophysical differences can be identified but the physiologic significance of these differences remains unclear. Creation of "knockout" cell lines and mice that lack one or more VDAC isoforms has led to the characterization of distinct phenotypes that provide a different set of insights into function which must be interpreted in the context of complex physiologic systems. Functions in male reproduction, the central nervous system and glucose homeostasis have been identified and require a deeper and more mechanistic examination. Annotation of the genome sequence of Drosophila melanogaster has recently revealed three additional genes (CG17137, CG17139, CG17140) with homology to porin, the previously described gene that encodes the VDAC of D. melanogaster. Molecular analysis of these novel VDACs has revealed a complex pattern of gene organization and expression. Sequence comparisons with other insect VDAC homologs suggest that this gene family evolved through a mechanism of duplication and divergence from an ancestral VDAC gene during the radiation of the genus Drosophila. Striking similarities to mouse VDAC mutants can be found that emphasize the conservation of function over a long evolutionary time frame.

摘要

电压依赖性阴离子通道(VDACs),也被称为线粒体孔蛋白,是线粒体外膜上一类形成小孔的小蛋白家族,存在于所有真核生物中。VDACs被认为在细胞质和线粒体区室之间代谢物的调节通量、通过与细胞质激酶相互作用参与整体能量代谢以及在程序性细胞死亡(凋亡)中发挥有争议的作用方面发挥重要作用。哺乳动物基因组包含三个VDAC基因座,分别称为Vdac1、Vdac2和Vdac3,这就引发了关于每个异构体可能执行何种功能的问题。基于对酵母中小鼠VDACs的表达研究,可以识别出生物物理差异,但这些差异的生理意义仍不清楚。创建缺乏一种或多种VDAC异构体的“敲除”细胞系和小鼠,已导致对不同表型的表征,这些表型为功能提供了不同的见解,必须在复杂的生理系统背景下进行解释。已确定其在雄性生殖、中枢神经系统和葡萄糖稳态中的功能,需要更深入和更具机制性的研究。黑腹果蝇基因组序列的注释最近揭示了另外三个与孔蛋白同源的基因(CG17137、CG17139、CG17140),孔蛋白是先前描述的编码黑腹果蝇VDAC的基因。对这些新型VDACs的分子分析揭示了复杂的基因组织和表达模式。与其他昆虫VDAC同源物的序列比较表明,这个基因家族是在果蝇属辐射期间通过从一个祖先VDAC基因复制和分化的机制进化而来的。可以发现与小鼠VDAC突变体有惊人的相似之处,这强调了在漫长的进化时间框架内功能的保守性。

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