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c型细胞色素在脑膜炎奈瑟菌呼吸作用中的作用

Roles of c-type cytochromes in respiration in Neisseria meningitidis.

作者信息

Deeudom Manu, Koomey Michael, Moir James W B

机构信息

Department of Microbiology, Faculty of Medicine, Chiangmai University, Chiangmai 50200, Thailand.

Department of Biology (Area 10), University of York, Heslington, York YO10 5YW, UK.

出版信息

Microbiology (Reading). 2008 Sep;154(Pt 9):2857-2864. doi: 10.1099/mic.0.2008/020339-0.

Abstract

Three c-type cytochromes were identified in Neisseria meningitidis, based on predictions from genome sequences, that were hypothesized to be involved in electron transport to terminal electron acceptor reductases for oxygen (the cytochrome cbb(3) oxidase) and nitrite (the nitrite reductase, AniA). Mutants were generated by allelic exchange with disrupted copies of the genes encoding these cytochromes and the phenotypes of the resultant mutants analysed. It was found that cytochrome c(5) is required for in vivo nitrite reductase activity, whereas cytochromes c(x) and c(4) are both required for efficient growth using oxygen as an electron acceptor. Mutants in c(x), c(4), and c(x)+c(4) have a decreased capacity to reduce oxygen, but there is a background oxygen-reduction activity, indicating that there may be other routes for electron transfer from the cytochrome bc(1) complex to the cytochrome cbb(3) oxidase, whereas cytochrome c(5) appears to be the sole route of electrons to the nitrite reductase in N. meningitidis. Interestingly, cytochrome c(x) is highly similar to a domain of copper nitrite reductases from various proteobacteria, whereas cytochrome c(5) has high identity with a domain of the cytochrome cbb(3) oxidase of Neisseria gonorrhoeae, yet these two proteins function in oxygen respiration and nitrite respiration, respectively. This highlights a limitation of predicting protein function from similarity to known proteins, i.e. very closely related protein domains in different organisms can have different redox partners.

摘要

基于基因组序列预测,在脑膜炎奈瑟菌中鉴定出三种c型细胞色素,据推测它们参与电子传递至氧的末端电子受体还原酶(细胞色素cbb(3)氧化酶)和亚硝酸盐(亚硝酸还原酶,AniA)。通过与编码这些细胞色素的基因的破坏拷贝进行等位基因交换产生突变体,并分析所得突变体的表型。结果发现,细胞色素c(5)是体内亚硝酸还原酶活性所必需的,而细胞色素c(x)和c(4)都是以氧作为电子受体进行高效生长所必需的。c(x)、c(4)和c(x)+c(4)的突变体还原氧的能力降低,但存在背景氧还原活性,这表明可能存在从细胞色素bc(1)复合物到细胞色素cbb(3)氧化酶的其他电子传递途径,而细胞色素c(5)似乎是脑膜炎奈瑟菌中电子传递至亚硝酸还原酶的唯一途径。有趣的是,细胞色素c(x)与来自各种变形菌门的铜亚硝酸还原酶的一个结构域高度相似,而细胞色素c(5)与淋病奈瑟菌的细胞色素cbb(3)氧化酶的一个结构域具有高度同源性,但这两种蛋白质分别在氧呼吸和亚硝酸呼吸中发挥作用。这突出了从与已知蛋白质的相似性预测蛋白质功能的局限性,即不同生物体中非常密切相关的蛋白质结构域可以有不同的氧化还原伙伴。

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