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Role of the AAA protease Yme1 in folding of proteins in the intermembrane space of mitochondria

机译:AAA蛋白酶Yme1在线粒体膜间空间蛋白质折叠中的作用

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The vast majority of mitochondrial proteins are synthesized in the cytosol and transported into the organelle in a largely, if not completely, unfolded state. The proper function of mitochondria thus depends on folding of several hundreds of proteins in the various subcompartments of the organelle. Whereas folding of proteins in the mitochondrial matrix is supported by members of several chaperone families, very little is known about folding of proteins in the intermembrane space (IMS). We targeted dihydrofolate reductase (DHFR) as a model substrate to the IMS of yeast mitochondria and analyzed its folding. DHFR can fold in this compartment, and its aggregation upon heat shock can be prevented in an ATP-dependent manner. Yme1, an AAA (ATPases associated with diverse cellular activities) protease of the IMS, prevented aggregation of DHFR. Analysis of protein aggregates in mitochondria lacking Yme1 revealed the presence of a number of proteins involved in the establishment of mitochondrial ultrastructure, lipid metabolism, protein import, and respiratory growth. These findings explain the pleiotropic effects of deletion of YME1 and suggest an important role for Yme1 as a folding assistant, in addition to its proteolytic function, in the protein homeostasis of mitochondria
机译:绝大多数线粒体蛋白是在细胞质中合成的,并以很大的(即使不是完全的)未折叠的状态转运到细胞器中。因此,线粒体的正常功能取决于细胞器各个子室中数百种蛋白质的折叠。线粒体基质中蛋白质的折叠受几个伴侣家族成员的支持,而关于膜间空间(IMS)中蛋白质的折叠知之甚少。我们将二氢叶酸还原酶(DHFR)作为酵母线粒体IMS的模型底物,并对其折叠进行了分析。 DHFR可以在该隔室中折叠,并且可以以ATP依赖的方式防止热激时其聚集。 Yme1是IMS的AAA(与多种细胞活性相关的ATPase)蛋白酶,可防止DHFR聚集。缺乏Yme1的线粒体中蛋白质聚集体的分析显示,存在许多参与线粒体超微结构建立,脂质代谢,蛋白质导入和呼吸生长的蛋白质。这些发现解释了YME1缺失的多效性作用,并表明Yme1除其蛋白水解功能外,在线粒体蛋白质稳态中还起着重要的折叠辅助作用。

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