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祖先旁系同源基因和假旁系同源基因及其在真核细胞出现中的作用。

Ancestral paralogs and pseudoparalogs and their role in the emergence of the eukaryotic cell.

作者信息

Makarova Kira S, Wolf Yuri I, Mekhedov Sergey L, Mirkin Boris G, Koonin Eugene V

机构信息

National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Bethesda, MD 20894, USA.

出版信息

Nucleic Acids Res. 2005 Aug 16;33(14):4626-38. doi: 10.1093/nar/gki775. Print 2005.

Abstract

Gene duplication is a crucial mechanism of evolutionary innovation. A substantial fraction of eukaryotic genomes consists of paralogous gene families. We assess the extent of ancestral paralogy, which dates back to the last common ancestor of all eukaryotes, and examine the origins of the ancestral paralogs and their potential roles in the emergence of the eukaryotic cell complexity. A parsimonious reconstruction of ancestral gene repertoires shows that 4137 orthologous gene sets in the last eukaryotic common ancestor (LECA) map back to 2150 orthologous sets in the hypothetical first eukaryotic common ancestor (FECA) [paralogy quotient (PQ) of 1.92]. Analogous reconstructions show significantly lower levels of paralogy in prokaryotes, 1.19 for archaea and 1.25 for bacteria. The only functional class of eukaryotic proteins with a significant excess of paralogous clusters over the mean includes molecular chaperones and proteins with related functions. Almost all genes in this category underwent multiple duplications during early eukaryotic evolution. In structural terms, the most prominent sets of paralogs are superstructure-forming proteins with repetitive domains, such as WD-40 and TPR. In addition to the true ancestral paralogs which evolved via duplication at the onset of eukaryotic evolution, numerous pseudoparalogs were detected, i.e. homologous genes that apparently were acquired by early eukaryotes via different routes, including horizontal gene transfer (HGT) from diverse bacteria. The results of this study demonstrate a major increase in the level of gene paralogy as a hallmark of the early evolution of eukaryotes.

摘要

基因复制是进化创新的关键机制。真核生物基因组的很大一部分由旁系同源基因家族组成。我们评估了可追溯到所有真核生物的最后一个共同祖先的祖先旁系同源性的程度,并研究了祖先旁系同源基因的起源及其在真核细胞复杂性出现中的潜在作用。对祖先基因库的简约重建表明,最后一个真核生物共同祖先(LECA)中的4137个直系同源基因集可追溯到假设的第一个真核生物共同祖先(FECA)中的2150个直系同源集[旁系同源商(PQ)为1.92]。类似的重建表明原核生物中的旁系同源性水平明显较低,古菌为1.19,细菌为1.25。真核生物蛋白质中唯一一类旁系同源簇显著超过平均值的功能类别包括分子伴侣和具有相关功能的蛋白质。该类别中的几乎所有基因在早期真核生物进化过程中都经历了多次复制。在结构方面,最突出的旁系同源基因集是具有重复结构域的超结构形成蛋白,如WD-40和TPR。除了在真核生物进化开始时通过复制进化而来的真正祖先旁系同源基因外,还检测到了许多假旁系同源基因,即早期真核生物显然通过不同途径获得的同源基因,包括来自各种细菌的水平基因转移(HGT)。这项研究的结果表明,基因旁系同源性水平大幅增加是真核生物早期进化的一个标志。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6f48/1187821/3f55494d585e/gki775f1.jpg

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