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探究为什么锥虫会组装具有非典型 AxxCH 血红素结合基序而不是 CxxCH 的细胞色素 c。

Probing why trypanosomes assemble atypical cytochrome c with an AxxCH haem-binding motif instead of CxxCH.

机构信息

Faculty of Health and Medicine, Division of Biomedical and Life Sciences, Lancaster University, Lancaster LA1 4YQ, UK.

出版信息

Biochem J. 2012 Dec 1;448(2):253-60. doi: 10.1042/BJ20120757.

DOI:10.1042/BJ20120757
PMID:22928879
Abstract

Mitochondrial cytochromes c and c1 are core components of the respiratory chain of all oxygen-respiring eukaryotes. These proteins contain haem, covalently bound to the polypeptide in a catalysed post-translational modification. In all eukaryotes, except members of the protist phylum Euglenozoa, haem attachment is to the cysteine residues of a CxxCH haem-binding motif. In the Euglenozoa, which include medically relevant trypanosomatid parasites, haem attachment is to a single cysteine residue in an AxxCH haem-binding motif. Moreover, genes encoding known c-type cytochrome biogenesis machineries are all absent from trypanosomatid genomes, indicating the presence of a novel biosynthetic apparatus. In the present study, we investigate expression and maturation of cytochrome c with a typical CxxCH haem-binding motif in the trypanosomatids Crithidia fasciculata and Trypanosoma brucei. Haem became attached to both cysteine residues of the haem-binding motif, indicating that, in contrast with previous hypotheses, nothing prevents formation of a CxxCH cytochrome c in euglenozoan mitochondria. The cytochrome variant was also able to replace the function of wild-type cytochrome c in T. brucei. However, the haem attachment to protein was not via the stereospecifically conserved linkage universally observed in natural c-type cytochromes, suggesting that the trypanosome cytochrome c biogenesis machinery recognized and processed only the wild-type single-cysteine haem-binding motif. Moreover, the presence of the CxxCH cytochrome c resulted in a fitness cost in respiration. The level of cytochrome c biogenesis in trypanosomatids was also found to be limited, with the cells operating at close to maximum capacity.

摘要

线粒体细胞色素 c 和 c1 是所有需氧真核生物呼吸链的核心组成部分。这些蛋白质含有血红素,通过催化的翻译后修饰共价结合到多肽上。在所有真核生物中,除了原生动物门 Euglenozoa 的成员外,血红素的附着都是在 CxxCH 血红素结合基序的半胱氨酸残基上。在 Euglenozoa 中,包括具有医学相关性的锥虫寄生虫,血红素附着在 AxxCH 血红素结合基序中的单个半胱氨酸残基上。此外,编码已知 c 型细胞色素生物发生机制的基因在锥虫基因组中均缺失,表明存在新型生物合成装置。在本研究中,我们研究了具有典型 CxxCH 血红素结合基序的锥虫 Crithidia fasciculata 和 Trypanosoma brucei 中细胞色素 c 的表达和成熟。血红素附着在血红素结合基序的两个半胱氨酸残基上,这表明与之前的假设相反,在 Euglenozoa 线粒体中没有任何东西可以阻止 CxxCH 细胞色素 c 的形成。这种细胞色素变体也能够在 T. brucei 中替代野生型细胞色素 c 的功能。然而,血红素与蛋白质的结合不是通过普遍存在于天然 c 型细胞色素中的立体特异性保守连接,这表明锥虫细胞色素 c 生物发生机制仅识别和处理野生型单半胱氨酸血红素结合基序。此外,CxxCH 细胞色素 c 的存在导致呼吸的适应度降低。还发现锥虫生物体内细胞色素 c 的生物发生水平有限,细胞接近最大容量运行。

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