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Mitochondria Use Different Mechanisms for Transport of Multispanning Membrane Proteins through the Intermembrane Space

机译:线粒体利用不同的机制跨膜空间运输跨膜蛋白。

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The mitochondrial inner membrane contains numerous multispanning integral proteins. The precursors of these hydrophobic proteins are synthesized in the cytosol and therefore have to cross the mitochondrial outer membrane and intermembrane space to reach the inner membrane. While the import pathways of noncleavable multispanning proteins, such as the metabolite carriers, have been characterized in detail by the generation of translocation intermediates, little is known about the mechanism by which cleavable preproteins of multispanning proteins, such as Oxa1, are transferred from the outer membrane to the inner membrane. We have identified a translocation intermediate of the Oxa1 preprotein in the translocase of the outer membrane (TOM) and found that there are differences from the import mechanisms of carrier proteins. The intermembrane space domain of the receptor Tom22 supports the stabilization of the Oxa1 intermediate. Transfer of the Oxa1 preprotein to the inner membrane is not affected by inactivation of the soluble TIM complexes. Both the inner membrane potential and matrix heat shock protein 70 are essential to release the preprotein from the TOM complex, suggesting a close functional cooperation of the TOM complex and the presequence translocase of the inner membrane. We conclude that mitochondria employ different mechanisms for translocation of multispanning proteins across the aqueous intermembrane space.
机译:线粒体内膜包含许多跨度完整的蛋白质。这些疏水蛋白的前体在细胞质中合成,因此必须穿过线粒体的外膜和膜间空间才能到达内膜。尽管不可裂解的多跨蛋白(例如代谢产物载体)的导入途径已通过转运中间体的产生进行了详细描述,但对多跨蛋白的可裂解前蛋白(如Oxa1)从外部转移的机理了解甚少。膜到内膜。我们已经确定了外膜(TOM)的转位酶中的Oxa1前蛋白的易位中间体,并发现与载体蛋白的导入机制存在差异。受体Tom22的膜间空间结构域支持Oxa1中间体的稳定。 Oxa1前蛋白向内膜的转移不受可溶性TIM复合物失活的影响。内膜电位和基质热休克蛋白70都是从TOM复合物中释放前蛋白所必需的,这表明TOM复合物与内膜的前序列转位酶之间功能密切相关。我们得出的结论是,线粒体采用不同的跨跨蛋白跨膜空间跨蛋白转运的机制。

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