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一种新型细菌细胞色素c的成熟需要一种专门的血红素裂解酶,该细胞色素c具有非常规的共价血红素结合方式。

A dedicated haem lyase is required for the maturation of a novel bacterial cytochrome c with unconventional covalent haem binding.

作者信息

Hartshorne Robert S, Kern Melanie, Meyer Björn, Clarke Thomas A, Karas Michael, Richardson David J, Simon Jörg

机构信息

School of Biological Sciences, University of East Anglia, Norwich NR4 7TJ, UK.

出版信息

Mol Microbiol. 2007 May;64(4):1049-60. doi: 10.1111/j.1365-2958.2007.05712.x.

Abstract

In bacterial c-type cytochromes, the haem cofactor is covalently attached via two cysteine residues organized in a haem c-binding motif. Here, a novel octa-haem c protein, MccA, is described that contains only seven conventional haem c-binding motifs (CXXCH), in addition to several single cysteine residues and a conserved CH signature. Mass spectrometric analysis of purified MccA from Wolinella succinogenes suggests that two of the single cysteine residues are actually part of an unprecedented CX15CH sequence involved in haem c binding. Spectroscopic characterization of MccA identified an unusual high-potential haem c with a red-shifted absorption maximum, not unlike that of certain eukaryotic cytochromes c that exceptionally bind haem via only one thioether bridge. A haem lyase gene was found to be specifically required for the maturation of MccA in W. succinogenes. Equivalent haem lyase-encoding genes belonging to either the bacterial cytochrome c biogenesis system I or II are present in the vicinity of every known mccA gene suggesting a dedicated cytochrome c maturation pathway. The results necessitate reconsideration of computer-based prediction of putative haem c-binding motifs in bacterial proteomes.

摘要

在细菌c型细胞色素中,血红素辅因子通过以血红素c结合基序排列的两个半胱氨酸残基共价连接。本文描述了一种新型的八血红素c蛋白MccA,除了几个单一半胱氨酸残基和一个保守的CH特征外,它仅含有七个传统的血红素c结合基序(CXXCH)。对来自产琥珀酸沃林氏菌的纯化MccA进行质谱分析表明,其中两个单一半胱氨酸残基实际上是参与血红素c结合的前所未有的CX15CH序列的一部分。MccA的光谱表征鉴定出一种异常的高电位血红素c,其吸收最大值发生红移,这与某些仅通过一个硫醚桥异常结合血红素的真核细胞色素c的情况并无不同。发现一个血红素裂合酶基因是产琥珀酸沃林氏菌中MccA成熟所特需的。属于细菌细胞色素c生物合成系统I或II的等效血红素裂合酶编码基因存在于每个已知mccA基因附近,这表明存在一条专门的细胞色素c成熟途径。这些结果有必要重新考虑基于计算机对细菌蛋白质组中假定的血红素c结合基序的预测。

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