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从祖先的β-β发夹到外膜β-桶的进化。

Evolution of outer membrane beta-barrels from an ancestral beta beta hairpin.

机构信息

Department of Biochemistry, Gene Center Munich and Center for Integrated Protein Science (CIPSM), Ludwig-Maximilians-Universtät München, Munich, Germany.

出版信息

Mol Biol Evol. 2010 Jun;27(6):1348-58. doi: 10.1093/molbev/msq017. Epub 2010 Jan 27.

DOI:10.1093/molbev/msq017
PMID:20106904
Abstract

Outer membrane beta-barrels (OMBBs) are the major class of outer membrane proteins from Gram-negative bacteria, mitochondria, and plastids. Their transmembrane domains consist of 8-24 beta-strands forming a closed, barrel-shaped beta-sheet around a central pore. Despite their obvious structural regularity, evidence for an origin by duplication or for a common ancestry has not been found. We use three complementary approaches to show that all OMBBs from Gram-negative bacteria evolved from a single, ancestral beta beta hairpin. First, we link almost all families of known single-chain bacterial OMBBs with each other through transitive profile searches. Second, we identify a clear repeat signature in the sequences of many OMBBs in which the repeating sequence unit coincides with the structural beta beta hairpin repeat. Third, we show that the observed sequence similarity between OMBB hairpins cannot be explained by structural or membrane constraints on their sequences. The third approach addresses a longstanding problem in protein evolution: how to distinguish between a very remotely homologous relationship and the opposing scenario of "sequence convergence." The origin of a diverse group of proteins from a single hairpin module supports the hypothesis that, around the time of transition from the RNA to the protein world, proteins arose by amplification and recombination of short peptide modules that had previously evolved as cofactors of RNAs.

摘要

外膜β-桶(OMBBs)是革兰氏阴性菌、线粒体和质体的主要外膜蛋白类。它们的跨膜结构域由 8-24 条β-折叠组成,围绕中央孔形成一个封闭的桶状β-折叠。尽管它们的结构明显具有规则性,但尚未发现其起源于复制或共同祖先的证据。我们使用三种互补的方法表明,所有来自革兰氏阴性菌的 OMBB 都由一个单一的祖先ββ发夹演变而来。首先,我们通过传递式轮廓搜索将几乎所有已知的单链细菌 OMBB 家族彼此联系起来。其次,我们在许多 OMBB 的序列中识别出一个清晰的重复特征,其中重复序列单元与结构ββ发夹重复一致。第三,我们表明,在 OMBB 发夹之间观察到的序列相似性不能用其序列对结构或膜的限制来解释。第三种方法解决了蛋白质进化中的一个长期存在的问题:如何区分非常遥远的同源关系和相反的“序列趋同”情景。一组多样化的蛋白质由一个发夹模块产生,这支持了这样一种假设,即在从 RNA 到蛋白质世界的过渡时期,蛋白质是通过扩增和重组以前作为 RNA 辅助因子进化而来的短肽模块产生的。

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