首页> 美国卫生研究院文献>The EMBO Journal >Coa1 links the Mss51 post-translational function to Cox1 cofactor insertion in cytochrome c oxidase assembly
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Coa1 links the Mss51 post-translational function to Cox1 cofactor insertion in cytochrome c oxidase assembly

机译:Coa1将Mss51翻译后功能链接到细胞色素C氧化酶装配中的Cox1辅助因子插入

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摘要

The assembly of cytochrome c oxidase (CcO) in yeast mitochondria is shown to be dependent on a new assembly factor designated Coa1 that associates with the mitochondrial inner membrane. Translation of the mitochondrial-encoded subunits of CcO occurs normally in coa1Δ cells, but these subunits fail to accumulate. The respiratory defect in coa1Δ cells is suppressed by high-copy MSS51, MDJ1 and COX10. Mss51 functions in Cox1 translation and elongation, whereas Cox10 participates in the biosynthesis of heme a, a key cofactor of CcO. Respiration in coa1Δ and shy1Δ cells is enhanced when Mss51 and Cox10 are coexpressed. Shy1 has been implicated in formation of the heme a3-CuB site in Cox1. The interaction between Coa1 and Cox1, and the physical and genetic interactions between Coa1 and Mss51, Shy1 and Cox14 suggest that Coa1 coordinates the transition of newly synthesized Cox1 from the Mss51:Cox14 complex to the heme a cofactor insertion involving Shy1. coa1Δ cells also display a mitochondrial copper defect suggesting that Coa1 may have a direct link to copper metallation of CcO.
机译:酵母线粒体中细胞色素C氧化酶(CcO)的组装显示依赖于新的组装因子Coa1,该因子与线粒体内膜相关。线粒体编码的CcO亚基的翻译通常发生在coa1Δ细胞中,但这些亚基无法积累。高拷贝MSS51,MDJ1和COX10抑制了coa1Δ细胞的呼吸缺陷。 Mss51在Cox1翻译和延伸中起作用,而Cox10参与血红素a(CcO的关键辅因子)的生物合成。 Mss51和Cox10共表达时,coa1Δ和shy1Δ细胞的呼吸作用增强。 Shy1与Cox1中血红素a3-CuB位点的形成有关。 Coa1和Cox1之间的相互作用,以及Coa1与Mss51,Shy1和Cox14之间的物理和遗传相互作用表明Coa1协调了新合成的Cox1从Mss51:Cox14复合体到涉及Shy1的血红素辅因子插入的过渡。 coa1Δ细胞还显示线粒体铜缺陷,表明Coa1可能与CcO的铜金属化直接相关。

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