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类似酶的共现决定了柔性环中发生非保守突变后一个新的(βα)8异构酶亚家族的进化。

Co-occurrence of analogous enzymes determines evolution of a novel (βα)8-isomerase sub-family after non-conserved mutations in flexible loop.

作者信息

Verduzco-Castro Ernesto A, Michalska Karolina, Endres Michael, Juárez-Vazquez Ana L, Noda-García Lianet, Chang Changsoo, Henry Christopher S, Babnigg Gyorgy, Joachimiak Andrzej, Barona-Gómez Francisco

机构信息

Evolution of Metabolic Diversity Laboratory, Unidad de Genómica Avanzada (Langebio), Cinvestav-IPN, Irapuato, CP36821, México.

Midwest Center for Structural Genomics, Argonne National Laboratory, Argonne, Illinois 60439, U.S.A. Structural Biology Center, Biosciences Division, Argonne National Laboratory, Argonne, Illinois 60439, U.S.A.

出版信息

Biochem J. 2016 May 1;473(9):1141-52. doi: 10.1042/BJ20151271. Epub 2016 Feb 29.

Abstract

We investigate the evolution of co-occurring analogous enzymes involved in L-tryptophan and L-histidine biosynthesis in Actinobacteria Phylogenetic analysis of trpF homologues, a missing gene in certain clades of this lineage whose absence is complemented by a dual-substrate HisA homologue, termed PriA, found that they fall into three categories: (i) trpF-1, an L-tryptophan biosynthetic gene horizontally acquired by certain Corynebacterium species; (ii) trpF-2, a paralogue known to be involved in synthesizing a pyrrolopyrrole moiety and (iii) trpF-3, a variable non-conserved orthologue of trpF-1 We previously investigated the effect of trpF-1 upon the evolution of PriA substrate specificity, but nothing is known about the relationship between trpF-3 and priA After in vitro steady-state enzyme kinetics we found that trpF-3 encodes a phosphoribosyl anthranilate isomerase. However, mutation of this gene in Streptomyces sviceus did not lead to auxothrophy, as expected from the biosynthetic role of trpF-1 Biochemical characterization of a dozen co-occurring TrpF-2 or TrpF-3, with PriA homologues, explained the prototrophic phenotype, and unveiled an enzyme activity trade-off between TrpF and PriA. X-ray structural analysis suggests that the function of these PriA homologues is mediated by non-conserved mutations in the flexible L5 loop, which may be responsible for different substrate affinities. Thus, the PriA homologues that co-occur with TrpF-3 represent a novel enzyme family, termed PriB, which evolved in response to PRA isomerase activity. The characterization of co-occurring enzymes provides insights into the influence of functional redundancy on the evolution of enzyme function, which could be useful for enzyme functional annotation.

摘要

我们研究了放线菌中参与L-色氨酸和L-组氨酸生物合成的共现类似酶的进化情况。对trpF同源物进行系统发育分析,trpF是该谱系某些分支中缺失的基因,其缺失由一种双底物HisA同源物(称为PriA)互补。结果发现它们分为三类:(i)trpF-1,一种由某些棒状杆菌属物种水平获得的L-色氨酸生物合成基因;(ii)trpF-2,一个已知参与合成吡咯并吡咯部分的旁系同源物;(iii)trpF-3,trpF-1的可变非保守直系同源物。我们之前研究了trpF-1对PriA底物特异性进化的影响,但对于trpF-3与priA之间的关系却一无所知。经过体外稳态酶动力学研究,我们发现trpF-3编码一种磷酸核糖基邻氨基苯甲酸异构酶。然而,在浅绿链霉菌中该基因的突变并未导致营养缺陷型,这与trpF-1的生物合成作用预期不同。对十几种与PriA同源物共现的TrpF-2或TrpF-3进行生化特性分析,解释了原养型表型,并揭示了TrpF和PriA之间的酶活性权衡。X射线结构分析表明,这些PriA同源物的功能由柔性L5环中的非保守突变介导,这可能导致不同的底物亲和力。因此,与TrpF-3共现的PriA同源物代表了一个新的酶家族,称为PriB,它是为响应PRA异构酶活性而进化的。对共现酶的特性分析为功能冗余对酶功能进化的影响提供了见解,这可能有助于酶的功能注释。

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