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Phosphatidylcholine Affects the Role of the Sorting and Assembly Machinery in the Biogenesis of Mitochondrial β-Barrel Proteins

机译:磷脂酰胆碱影响分选和组装机制在线粒体β-桶蛋白的生物发生中的作用。

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摘要

Two protein translocases drive the import of β-barrel precursor proteins into the mitochondrial outer membrane: The translocase of the outer membrane (TOM complex) promotes transport of the precursor to the intermembrane space, whereas the sorting and assembly machinery (SAM complex) mediates subsequent folding of the β-barrel and its integration into the target membrane. The non-bilayer-forming phospholipids phosphatidylethanolamine (PE) and cardiolipin (CL) are required for the biogenesis of β-barrel proteins. Whether bilayer-forming phospholipids such as phosphatidylcholine (PC), the most abundant phospholipid of the mitochondrial outer membrane, play a role in the import of β-barrel precursors is unclear. In this study, we show that PC is required for stability and function of the SAM complex during the biogenesis of β-barrel proteins. PC further promotes the SAM-dependent assembly of the TOM complex, indicating a general role of PC for the function of the SAM complex. In contrast to PE-deficient mitochondria precursor accumulation at the TOM complex is not affected by depletion of PC. We conclude that PC and PE affect the function of distinct protein translocases in mitochondrial β-barrel biogenesis.
机译:有两个蛋白质转运蛋白驱动β-桶前体蛋白进入线粒体外膜:外膜的转运蛋白(TOM复合物)促进前体向膜间空间的运输,而分选和组装机械(SAM复合物)随后介导β-桶的折叠及其整合到目标膜中。非双层形成的磷脂磷脂酰乙醇胺(PE)和心磷脂(CL)是生物合成的β-桶蛋白。尚不清楚形成双层的磷脂(例如,磷脂酰胆碱(PC))是线粒体外膜中最丰富的磷脂,在β-桶形前体的进口中是否起作用。在这项研究中,我们表明PC是β-桶状蛋白质生物合成过程中SAM复合物的稳定性和功能所必需的。 PC进一步促进了TOM复合体的SAM依赖装配,这表明PC在SAM复合体功能方面的一般作用。与PE缺乏的线粒体前体相比,TOM复合物中的堆积不受PC耗尽的影响。我们得出的结论是,PC和PE影响线粒体β-桶生物发生中独特的蛋白转运酶的功能。

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