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Functionally diverging molecular quasi-species evolve by crossing two enzymes

机译:通过交叉两种酶进化功能上不同的分子准种

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摘要

Molecular evolution is frequently portrayed by structural relationships, but delineation of separate functional species is more elusive. We have generated enzyme variants by stochastic recombinations of DNA encoding two homologous detoxication enzymes, human glutathione transferases M1-1 and M2-2, and explored their catalytic versatilities. Sampled mutants were screened for activities with eight alternative substrates, and the activity fingerprints were subjected to principal component analysis. This phenotype characterization clearly identified at least three distributions of substrate selectivity, where one was orthogonal to those of the parent-like distributions. This approach to evolutionary data mining serves to identify emerging molecular quasi-species and indicates potential trajectories available for further protein evolution.
机译:分子进化通常通过结构关系来刻画,但是对单独的功能性物种的描述则更加难以捉摸。我们已经通过编码两种同源脱毒酶,人谷胱甘肽转移酶M1-1和M2-2的DNA的随机重组产生了酶变体,并探索了它们的催化通用性。筛选出的突变体具有八种替代底物的活性,并对活性指纹进行主成分分析。该表型表征清楚地确定了底物选择性的至少三种分布,其中一种与母体样分布的正交。这种用于进化数据挖掘的方法可用于识别新兴的分子准物种,并指出可用于进一步蛋白质进化的潜在轨迹。

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