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线粒体中禁阻蛋白形成膜结合环复合物。

Formation of membrane-bound ring complexes by prohibitins in mitochondria.

作者信息

Tatsuta Takashi, Model Kirstin, Langer Thomas

机构信息

Institut für Genetik and Zentrum für Molekulare Medizin, Universität zu Köln, 50674 Köln, Germany.

出版信息

Mol Biol Cell. 2005 Jan;16(1):248-59. doi: 10.1091/mbc.e04-09-0807. Epub 2004 Nov 3.

Abstract

Prohibitins comprise a remarkably conserved protein family in eukaryotic cells with proposed functions in cell cycle progression, senescence, apoptosis, and the regulation of mitochondrial activities. Two prohibitin homologues, Phb1 and Phb2, assemble into a high molecular weight complex of approximately 1.2 MDa in the mitochondrial inner membrane, but a nuclear localization of Phb1 and Phb2 also has been reported. Here, we have analyzed the biogenesis and structure of the prohibitin complex in Saccharomyces cerevisiae. Both Phb1 and Phb2 subunits are targeted to mitochondria by unconventional noncleavable targeting sequences at their amino terminal end. Membrane insertion involves binding of newly imported Phb1 to Tim8/13 complexes in the intermembrane space and is mediated by the TIM23-translocase. Assembly occurs via intermediate-sized complexes of approximately 120 kDa containing both Phb1 and Phb2. Conserved carboxy-terminal coiled-coil regions in both subunits mediate the formation of large assemblies in the inner membrane. Single particle electron microscopy of purified prohibitin complexes identifies diverse ring-shaped structures with outer dimensions of approximately 270 x 200 angstroms. Implications of these findings for proposed cellular activities of prohibitins are discussed.

摘要

抑制素是真核细胞中一个高度保守的蛋白质家族,在细胞周期进程、衰老、凋亡以及线粒体活动调节中具有推测的功能。两个抑制素同源物,Phb1和Phb2,在线粒体内膜组装成一个分子量约为1.2 MDa的高分子量复合物,但也有报道称Phb1和Phb2存在核定位。在这里,我们分析了酿酒酵母中抑制素复合物的生物发生和结构。Phb1和Phb2亚基均通过其氨基末端非常规的不可切割靶向序列靶向线粒体。膜插入涉及新导入的Phb1与膜间隙中的Tim8/13复合物结合,并由TIM23转位酶介导。组装通过包含Phb1和Phb2的约120 kDa的中等大小复合物进行。两个亚基中保守的羧基末端卷曲螺旋区域介导内膜中大型组装体的形成。纯化的抑制素复合物的单颗粒电子显微镜鉴定出各种外部尺寸约为270×200埃的环形结构。讨论了这些发现对抑制素推测的细胞活性的影响。

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