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Phylogenomic analysis of the cystatin superfamily in eukaryotes and prokaryotes

机译:真核生物和原核生物中胱抑素超家族的系统学分析

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Background The cystatin superfamily comprises cysteine protease inhibitors that play key regulatory roles in protein degradation processes. Although they have been the subject of many studies, little is known about their genesis, evolution and functional diversification. Our aim has been to obtain a comprehensive insight into their origin, distribution, diversity, evolution and classification in Eukaryota, Bacteria and Archaea. Results We have identified in silico the full complement of the cystatin superfamily in more than 2100 prokaryotic and eukaryotic genomes. The analysis of numerous eukaryotic genomes has provided strong evidence for the emergence of this superfamily in the ancestor of eukaryotes. The progenitor of this superfamily was most probably intracellular and lacked a signal peptide and disulfide bridges, much like the extant Giardia cystatin. A primordial gene duplication produced two ancestral eukaryotic lineages, cystatins and stefins. While stefins remain encoded by a single or a small number of genes throughout the eukaryotes, the cystatins have undergone a more complex and dynamic evolution through numerous gene and domain duplications. In the cystatin superfamily we discovered twenty vertebrate-specific and three angiosperm-specific orthologous families, indicating that functional diversification has occurred only in multicellular eukaryotes. In vertebrate orthologous families, the prevailing trends were loss of the ancestral inhibitory activity and acquisition of novel functions in innate immunity. Bacterial cystatins and stefins may be emergency inhibitors that enable survival of bacteria in the host, defending them from the host's proteolytic activity. Conclusion This study challenges the current view on the classification, origin and evolution of the cystatin superfamily and provides valuable insights into their functional diversification. The findings of this comprehensive study provide guides for future structural and evolutionary studies of the cystatin superfamily as well as of other protease inhibitors and proteases.
机译:背景技术胱抑素超家族包含在蛋白质降解过程中起关键调节作用的半胱氨酸蛋白酶抑制剂。尽管它们已成为许多研究的主题,但对其起源,进化和功能多样化知之甚少。我们的目的是获得对它们在真核生物,细菌和古细菌中的起源,分布,多样性,进化和分类的全面了解。结果我们已经在计算机上鉴定了超过2100个原核和真核基因组中胱抑素超家族的完整互补物。对许多真核生物基因组的分析为该超家族在真核生物祖先中的出现提供了有力的证据。这个超家族的祖细胞很可能是细胞内的,并且缺乏信号肽和二硫键,就像现存的贾第虫半胱氨酸蛋白酶一样。原始基因重复产生了两个祖先的真核细胞谱系,胱抑素和硬脂蛋白。虽然在整个真核生物中,stefin仍由单个或少数几个基因编码,但半胱氨酸蛋白酶抑制剂通过大量的基因和结构域重复已经经历了更为复杂和动态的进化。在半胱氨酸蛋白酶抑制剂超家族中,我们发现了20个脊椎动物特有的和3个被子植物特有的直系同源家族,这表明功能多样化仅在多细胞真核生物中发生。在脊椎动物直系同源家族中,普遍的趋势是祖先抑制活性的丧失和获得先天免疫的新功能。细菌半胱氨酸蛋白酶抑制剂和Stefin可能是紧急抑制剂,可以使细菌在宿主中存活,从而保护它们免受宿主的蛋白水解作用。结论本研究挑战了关于胱抑素超家族的分类,起源和进化的当前观点,并为它们的功能多样化提供了宝贵的见解。这项全面研究的结果为胱抑素超家族以及其他蛋白酶抑制剂和蛋白酶的未来结构和进化研究提供了指导。

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