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对复合体I膜亚基装配途径的分析表明,亚基L(ND5)可能最后装配进去。

Analysis of the assembly pathway for membrane subunits of Complex I reveals that subunit L (ND5) can assemble last in .

作者信息

Zhang Fang, Vik Steven B

机构信息

Department of Biological Sciences, Southern Methodist University, Dallas, Texas 75275-0376 USA.

出版信息

BBA Adv. 2021;1. doi: 10.1016/j.bbadva.2021.100027. Epub 2021 Oct 17.

Abstract

Respiratory Complex I, a multi-subunit, membrane-bound enzyme, oxidizes NADH in the electron transport chains of mammalian mitochondria, and many bacterial species. We have examined assembly of the membrane subunits of Complex I from . Complexes of J-K, L-M, M-N, and J-K-L-M-N were observed by both native gel electrophoresis and co-immunoprecipitation, when subsets of the genes were expressed. Subunit L (ND5 in humans), the most distal membrane subunit, with an unusual extended C-terminal segment, did not join with M-N, and but could join with J-K-M-N. When the genes were split between two plasmids, with L, M, and N subunits expressed in various combinations from one plasmid, the resulting enzyme activity in membrane vesicles dropped to 19-60% relative to expression from the whole operon encoded on one plasmid. When L was expressed after a time-delay, rather than simultaneously, the activity increased from 28% to 100%, indicating that it can efficiently join a preformed complex lacking L. In contrast, when larger groups of membrane subunits were expressed last, LMN or JKLMN, assembly was much less efficient. The two-plasmid expression system was used to re-analyze C-terminal mutations in subunit K (ND4L), which occur near the overlapping and genes. These mutations were found to disrupt assembly, indicating the importance of the junction of L, N and K subunits. The results highlight the temporal and spatial aspects of gene expression that allow efficient assembly of the membrane subunits of Complex I.

摘要

呼吸链复合体I是一种多亚基的膜结合酶,可在哺乳动物线粒体和许多细菌物种的电子传递链中氧化NADH。我们研究了来自[具体来源未明确]的复合体I膜亚基的组装情况。当表达部分基因时,通过非变性凝胶电泳和共免疫沉淀观察到了J-K、L-M、M-N以及J-K-L-M-N复合体。最远端的膜亚基L(人类中的ND5)具有不寻常的延长C末端片段,它不与M-N结合,但可与J-K-M-N结合。当基因在两个质粒之间分开,L、M和N亚基以各种组合从一个质粒表达时,相对于在一个质粒上编码的整个操纵子的表达,膜囊泡中的酶活性降至19%-60%。当L延迟表达而不是同时表达时,活性从28%增加到100%,这表明它可以有效地加入缺乏L的预先形成的复合体。相比之下,当最后表达较大的膜亚基组,即LMN或JKLMN时,组装效率要低得多。双质粒表达系统用于重新分析亚基K(ND4L)中靠近重叠基因[具体基因未明确]的C末端突变。发现这些突变会破坏组装,表明L、N和K亚基连接的重要性。结果突出了基因表达的时间和空间方面,这些方面有助于呼吸链复合体I膜亚基的有效组装。

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