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病毒巯基氧化酶中的二聚体界面迁移

Dimer interface migration in a viral sulfhydryl oxidase.

作者信息

Hakim Motti, Fass Deborah

机构信息

Department of Structural Biology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

J Mol Biol. 2009 Aug 28;391(4):758-68. doi: 10.1016/j.jmb.2009.06.070. Epub 2009 Jul 2.

Abstract

Large double-stranded DNA viruses, including poxviruses and mimiviruses, encode enzymes to catalyze the formation of disulfide bonds in viral proteins produced in the cell cytosol, an atypical location for oxidative protein folding. These viral disulfide catalysts belong to a family of sulfhydryl oxidases that are dimers of a small five-helix fold containing a Cys-X-X-Cys motif juxtaposed to a flavin adenine dinucleotide cofactor. We report that the sulfhydryl oxidase pB119L from African swine fever virus (ASFV) uses for self-assembly surface different from that observed in homologs from mammals, plants, and fungi. Within a protein family, different packing interfaces for the same oligomerization state are extremely rare. We find that the alternate dimerization mode seen in ASFV pB119L is not characteristic of all viral sulfhydryl oxidases, as the flavin-binding domain from a mimivirus sulfhydryl oxidase assumes the same dimer structure as the known eukaryotic enzymes. ASFV pB119L demonstrates the potential of large double-stranded DNA viruses, which have faster mutation rates than their hosts and the tendency to incorporate host genes, to pioneer new protein folds and self-assembly modes.

摘要

大型双链DNA病毒,包括痘病毒和巨型病毒,编码酶以催化在细胞溶质中产生的病毒蛋白中二硫键的形成,这是氧化蛋白折叠的一个非典型位置。这些病毒二硫键催化剂属于巯基氧化酶家族,它们是一个小的五螺旋折叠的二聚体,含有与黄素腺嘌呤二核苷酸辅因子并列的Cys-X-X-Cys基序。我们报告说,非洲猪瘟病毒(ASFV)的巯基氧化酶pB119L用于自我组装的表面与在哺乳动物、植物和真菌的同源物中观察到的不同。在一个蛋白质家族中,相同寡聚化状态的不同堆积界面极为罕见。我们发现,ASFV pB119L中看到的交替二聚化模式并非所有病毒巯基氧化酶的特征,因为巨型病毒巯基氧化酶的黄素结合结构域与已知的真核酶具有相同的二聚体结构。ASFV pB119L展示了大型双链DNA病毒的潜力,这些病毒的突变率比其宿主更快,并且有整合宿主基因的倾向,能够开创新的蛋白质折叠和自我组装模式。

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