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Mutation network-based understanding of pleiotropic and epistatic mutational behavior of Enterococcus faecalis FMN-dependent azoreductase

机译:基于突变网络的粪肠球菌FMN依赖性偶氮还原酶的多效性和上位性突变行为的理解

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摘要

We previously identified a highly active homodimeric FMN-dependent NADH-preferred azoreductase (AzoA) from Enterococcus faecalis, which cleaves the azo bonds (R-N˭N-R) of diverse azo dyes, and determined its crystal structure. The preliminary network-based mutational analysis suggested that the two residues, Arg-21 and Asn-121, have an apparent mutational potential for fine-tuning of AzoA, based on their beneficial pleiotropic feedbacks. However, epistasis between the two promising mutational spots in AzoA has not been obtained in terms of substrate binding and azoreductase activity. In this study, we further quantified, visualized, and described the pleiotropic and/or epistatic behavior of six single or double mutations at the positions, Arg-21 and Asn-121, as a further research endeavor for beneficial fine-tuning of AzoA. Based on this network-based mutational analysis, we showed that pleiotropy and epistasis are common, sensitive, and complex mutational behaviors, depending mainly on the structural and functional responsibility and the physicochemical properties of the residue(s) in AzoA.
机译:我们先前从粪肠球菌中鉴定了高活性的同二聚体FMN依赖性NADH首选偶氮还原酶(AzoA),该酶可裂解各种偶氮染料的偶氮键(R-N˭N-R),并确定其晶体结构。基于网络的初步突变分析表明,基于它们的有益多效反馈,两个残基Arg-21和Asn-121具有对AzoA进行微调的明显突变潜力。但是,就底物结合和偶氮还原酶活性而言,尚未获得AzoA中两个有希望的突变点之间的上位性。在这项研究中,我们进一步量化,可视化和描述了在Arg-21和Asn-121位置上的六个单突变或双突变的多效性和/或上位性行为,作为对AzoA进行有益的微调的进一步研究方法。基于此基于网络的突变分析,我们表明多效性和上位性是常见,敏感和复杂的突变行为,主要取决于AzoA中残基的结构和功能责任以及理化特性。

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