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线粒体内膜中蛋白质复合物的超分子组织

Supramolecular organization of protein complexes in the mitochondrial inner membrane.

作者信息

Vonck Janet, Schäfer Eva

机构信息

Department of Structural Biology, Max-Planck-Institute of Biophysics, Max-von-Laue-Strasse 3, D-60438 Frankfurt am Main, Germany.

出版信息

Biochim Biophys Acta. 2009 Jan;1793(1):117-24. doi: 10.1016/j.bbamcr.2008.05.019. Epub 2008 Jun 3.

DOI:10.1016/j.bbamcr.2008.05.019
PMID:18573282
Abstract

The liquid state model that envisions respiratory chain complexes diffusing freely in the membrane is increasingly challenged by reports of supramolecular organization of the complexes in the mitochondrial inner membrane. Supercomplexes of complex III with complex I and/or IV can be isolated after solubilisation with mild detergents like digitonin. Electron microscopic studies have shown that these have a distinct architecture and are not random aggregates. A 3D reconstruction of a I1III2IV1 supercomplex shows that the ubiquinone and cytochrome c binding sites of the individual complexes are facing each other, suggesting a role in substrate channelling. Formation of supercomplexes plays a role in the assembly and stability of the complexes, suggesting that the supercomplexes are the functional state of the respiratory chain. Furthermore, a supramolecular organisation of ATP synthases has been observed in mitochondria, where ATP synthase is organised in dimer rows. Dimers can be isolated by mild detergent extraction and recent electron microscopic studies have shown that the membrane domains of the two partners in the dimer are at an angle to each other, indicating that in vivo the dimers would cause the membrane to bend. The suggested role in crista formation is supported by the observation of rows of ATP synthase dimers in the most curved parts of the cristae. Together these observations show that the mitochondrial inner membrane is highly organised and that the molecular events leading to ATP synthesis are carefully coordinated.

摘要

认为呼吸链复合物在膜中自由扩散的液态模型,越来越受到线粒体内膜中复合物超分子组织报告的挑战。用温和的去污剂(如洋地黄皂苷)增溶后,可以分离出复合物III与复合物I和/或IV的超复合物。电子显微镜研究表明,这些超复合物具有独特的结构,并非随机聚集体。对I1III2IV1超复合物的三维重建显示,各个复合物的泛醌和细胞色素c结合位点彼此相对,表明其在底物通道化中发挥作用。超复合物的形成在复合物的组装和稳定性中起作用,这表明超复合物是呼吸链的功能状态。此外,在线粒体中观察到了ATP合酶的超分子组织,其中ATP合酶以二聚体行排列。通过温和的去污剂提取可以分离出二聚体,最近的电子显微镜研究表明,二聚体中两个亚基的膜结构域彼此成一定角度,这表明在体内二聚体会导致膜弯曲。在嵴最弯曲部分观察到的ATP合酶二聚体行支持了其在嵴形成中的作用。这些观察结果共同表明,线粒体内膜高度有序,导致ATP合成的分子事件得到了精心协调。

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