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对复合物II中醌结合位点进化的结构洞察。

Structural Insight into Evolution of the Quinone Binding Site in Complex II.

作者信息

Maklashina Elena

机构信息

Department of Biochemistry and Biophysics, University of California, San Francisco, CA 94143, USA.

出版信息

Biochemistry (Mosc). 2022 Aug;87(8):752-761. doi: 10.1134/S0006297922080077.

Abstract

The Complex II family encompasses membrane bound succinate:quinones reductases and quinol:fumarate reductases that catalyze interconversion of succinate and fumarate coupled with reduction and oxidation of quinone. These enzymes are found in all biological genres and share a modular structure where a highly conserved soluble domain is bound to a membrane-spanning domain that is represented by distinct variations. The current classification of the complex II family members is based on the number of subunits and co-factors in the membrane anchor (types A-F). This classification also provides insights into possible evolutionary paths and suggests that some of the complex II enzymes (types A-C) co-evolved as the whole assembly. Origin of complex II types D and F may have arisen from independent events of de novo association of the conserved soluble domain with a new anchor. Here we analyze a recent structure of Mycobacterium smegmatis Sdh2, a complex II enzyme with two transmembrane subunits and two heme b molecules. This analysis supports an earlier hypothesis suggesting that mitochondrial complex II (type C) with a single heme b may have evolved as an assembled unit from an ancestor similar to M. smegmatis Sdh2.

摘要

复合体II家族包括膜结合的琥珀酸:醌还原酶和醌醇:富马酸还原酶,它们催化琥珀酸和富马酸的相互转化,并伴随着醌的还原和氧化。这些酶存在于所有生物类别中,并具有模块化结构,其中一个高度保守的可溶性结构域与一个由不同变体代表的跨膜结构域相连。目前对复合体II家族成员的分类基于膜锚定结构域中的亚基数量和辅因子(A-F型)。这种分类也为可能的进化路径提供了见解,并表明一些复合体II酶(A-C型)作为一个整体共同进化。D型和F型复合体II的起源可能源于保守可溶性结构域与新锚定结构域的独立从头关联事件。在这里,我们分析了耻垢分枝杆菌Sdh2的最新结构,它是一种具有两个跨膜亚基和两个血红素b分子的复合体II酶。该分析支持了一个早期假设,即具有单个血红素b的线粒体复合体II(C型)可能是从类似于耻垢分枝杆菌Sdh2的祖先作为一个组装单元进化而来的。

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