首页> 外文期刊>Journal of cell biology >Sam37 is crucial for formation of the mitochondrial TOM–SAM supercomplex, thereby promoting β-barrel biogenesis
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Sam37 is crucial for formation of the mitochondrial TOM–SAM supercomplex, thereby promoting β-barrel biogenesis

机译:Sam37对于线粒体TOM-SAM超复合物的形成至关重要,从而促进了β-桶生物合成

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摘要

Biogenesis of mitochondrial β-barrel proteins requires two preprotein translocases, the general translocase of the outer membrane (TOM) and the sorting and assembly machinery (SAM). TOM and SAM form a supercomplex that promotes transfer of β-barrel precursors. The SAM core complex contains the channel protein Sam50, which cooperates with Sam35 in precursor recognition, and the peripheral membrane protein Sam37. The molecular function of Sam37 has been unknown. We report that Sam37 is crucial for formation of the TOM–SAM supercomplex. Sam37 interacts with the receptor domain of Tom22 on the cytosolic side of the mitochondrial outer membrane and links TOM and SAM complexes. Sam37 thus promotes efficient transfer of β-barrel precursors to the SAM complex. We conclude that Sam37 functions as a coupling factor of the translocase supercomplex of the mitochondrial outer membrane.
机译:线粒体β-桶状蛋白的生物发生需要两个前蛋白转位酶,即一般的外膜转位酶(TOM)和分选和组装机器(SAM)。 TOM和SAM形成促进β-桶前体转移的超复合物。 SAM核心复合物包含通道蛋白Sam50(与Sam35协同进行前体识别)和外围膜蛋白Sam37。 Sam37的分子功能尚不清楚。我们报告说,Sam37对于形成TOM-SAM超复合物至关重要。 Sam37与线粒体外膜胞质侧Tom22的受体域相互作用,并连接TOM和SAM复合物。因此,Sam37促进了β桶前体向SAM复合物的有效转移。我们得出的结论是,Sam37充当线粒体外膜的跨酶超复合物的偶联因子。

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