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FGGY 碳水化合物激酶家族:对功能特异性进化的深入了解。

The FGGY carbohydrate kinase family: insights into the evolution of functional specificities.

机构信息

Graduate School of Biomedical Sciences, Sanford-Burnham Medical Research Institute, La Jolla, California, United States of America.

出版信息

PLoS Comput Biol. 2011 Dec;7(12):e1002318. doi: 10.1371/journal.pcbi.1002318. Epub 2011 Dec 22.

Abstract

Function diversification in large protein families is a major mechanism driving expansion of cellular networks, providing organisms with new metabolic capabilities and thus adding to their evolutionary success. However, our understanding of the evolutionary mechanisms of functional diversity in such families is very limited, which, among many other reasons, is due to the lack of functionally well-characterized sets of proteins. Here, using the FGGY carbohydrate kinase family as an example, we built a confidently annotated reference set (CARS) of proteins by propagating experimentally verified functional assignments to a limited number of homologous proteins that are supported by their genomic and functional contexts. Then, we analyzed, on both the phylogenetic and the molecular levels, the evolution of different functional specificities in this family. The results show that the different functions (substrate specificities) encoded by FGGY kinases have emerged only once in the evolutionary history following an apparently simple divergent evolutionary model. At the same time, on the molecular level, one isofunctional group (L-ribulokinase, AraB) evolved at least two independent solutions that employed distinct specificity-determining residues for the recognition of a same substrate (L-ribulose). Our analysis provides a detailed model of the evolution of the FGGY kinase family. It also shows that only combined molecular and phylogenetic approaches can help reconstruct a full picture of functional diversifications in such diverse families.

摘要

功能多样化是驱动细胞网络扩张的主要机制之一,为生物体提供了新的代谢能力,从而增加了它们的进化成功。然而,我们对这类家族中功能多样性的进化机制的理解非常有限,这在许多其他原因之外,还由于缺乏功能上得到很好表征的蛋白质集。在这里,我们以 FGGY 碳水化合物激酶家族为例,通过将经过实验验证的功能分配传播到数量有限的、得到基因组和功能背景支持的同源蛋白质,构建了一个置信度高的蛋白质注释参考集 (CARS)。然后,我们在系统发育和分子水平上分析了该家族中不同功能特异性的进化。结果表明,FGGY 激酶编码的不同功能(底物特异性)仅在一个简单的分歧进化模型之后的进化历史中出现过一次。同时,在分子水平上,一个同工酶组(L-核酮糖激酶,AraB)至少进化出了两种独立的解决方案,它们使用不同的特异性决定残基来识别相同的底物(L-核酮糖)。我们的分析提供了 FGGY 激酶家族进化的详细模型。它还表明,只有结合分子和系统发育方法,才能帮助重建此类多样化家族中功能多样化的全貌。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/348e/3245297/08fd4fa2fe66/pcbi.1002318.g001.jpg

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