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首页> 外文期刊>Journal of Molecular Biology >Two modular forms of the mitochondrial sorting and assembly machinery are involved in biogenesis of alpha-helical outer membrane proteins.
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Two modular forms of the mitochondrial sorting and assembly machinery are involved in biogenesis of alpha-helical outer membrane proteins.

机译:线粒体分选和组装机制的两种模块化形式参与了α-螺旋外膜蛋白的生物合成。

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The mitochondrial outer membrane contains two translocase machineries for precursor proteins--the translocase of the outer membrane (TOM complex) and the sorting and assembly machinery (SAM complex). The TOM complex functions as the main mitochondrial entry gate for nuclear-encoded proteins, whereas the SAM complex was identified according to its function in the biogenesis of beta-barrel proteins of the outer membrane. The SAM complex is required for the assembly of precursors of the TOM complex, including not only the beta-barrel protein Tom40 but also a subset of alpha-helical subunits. While the interaction of beta-barrel proteins with the SAM complex has been studied in detail, little is known about the interaction between the SAM complex and alpha-helical precursor proteins. We report that the SAM is not static but that the SAM core complex can associate with different partner proteins to form two large SAM complexes with different functions in the biogenesis of alpha-helical Tom proteins. We found that a subcomplex of TOM, Tom5-Tom40, associates with the SAM core complex to form a new large SAM complex. This SAM-Tom5/Tom40 complex binds the alpha-helical precursor of Tom6 after the precursor has been inserted into the outer membrane in an Mim1 (mitochondrial import protein 1)-dependent manner. The second large SAM complex, SAM-Mdm10 (mitochondrial distribution and morphology protein), binds the alpha-helical precursor of Tom22 and promotes its membrane integration. We suggest that the modular composition of the SAM complex provides a flexible platform to integrate the sorting pathways of different precursor proteins and to promote their assembly into oligomeric complexes.
机译:线粒体外膜包含两个前体蛋白的转位酶机制-外膜的转位酶(TOM复合体)和分选和组装机械(SAM复合体)。 TOM复合物充当核编码蛋白的主要线粒体进入门,而SAM复合物是根据其在外膜β-桶状蛋白的生物发生中的功能鉴定的。 SAM复合物是TOM复合物前体的组装所必需的,TOM复合物的前体不仅包括β-桶形蛋白质Tom40,还包括α-螺旋亚基的子集。虽然已经详细研究了β桶蛋白与SAM复合物的相互作用,但对SAM复合物与α螺旋前体蛋白之间的相互作用了解甚少。我们报告说,SAM不是静态的,但是SAM核心复合物可以与不同的伴侣蛋白缔合,从而形成两个大的SAM复合物,它们在α螺旋Tom蛋白的生物发生中具有不同的功能。我们发现,TOM的一个子复合体Tom5-Tom40与SAM核心复合体关联在一起,形成了一个新的大型SAM复合体。此SAM-Tom5 / Tom40复合物以Mim1(线粒体导入蛋白1)依赖性方式将Tom6的α-螺旋前体插入外膜后。第二种大型SAM复合物SAM-Mdm10(线粒体分布和形态蛋白)结合Tom22的α螺旋前体并促进其膜整合。我们建议,SAM复合物的模块化组成提供了一个灵活的平台,可以整合不同前体蛋白的分选途径并促进其组装成寡聚复合物。

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