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一种杂乱的异分支酸丙酮酸裂解酶向高效分支酸变位酶的(反向)进化

(Reverse) Evolution of a Promiscuous Isochorismate Pyruvate Lyase into an Efficient Chorismate Mutase.

作者信息

Künzler Dominik E, Bressan Luca, Jäger Linda, Gamper Marianne, Kast Peter

机构信息

Laboratory of Organic Chemistry, ETH Zurich, CH-8093 Zurich, Switzerland.

出版信息

Biochemistry. 2025 Aug 5;64(15):3459-3473. doi: 10.1021/acs.biochem.5c00157. Epub 2025 Jul 22.

DOI:10.1021/acs.biochem.5c00157
PMID:40694666
Abstract

PchB is an isochorismate pyruvate lyase (IPL) involved in siderophore biosynthesis in . Besides catalyzing the [1,5]-sigmatropic rearrangement of isochorismate, PchB also has weak chorismate mutase (CM) activity, promoting the [3,3]-sigmatropic transformation of chorismate. It has been suggested that the secondary metabolism enzyme PchB evolved from a primary metabolism CM precursor. Here, we employed directed evolution to convert PchB (back) into an efficient CM. A total of seven residues around the active site differing between PchB and a prototypical CM from were randomized, and the resulting gene library was subjected to selection for CM activity. After growth selection in an auxotrophic strain, a catalyst with 10-fold increased CM activity emerged. The improved enzyme was again randomized at three active site positions and subjected to selection, leading to a PchB variant with a / of 96,000 M s, which is 40 times higher than that of the parent enzyme and well within the range of dedicated natural CMs. The facile conversion of an IPL into a CM by directed evolution coincides with the fact that both reactions proceed through mechanistically interesting pericyclic processes, reaction types otherwise rarely used by enzymes. When probing typical established CMs for catalytic promiscuity, we discovered spurious IPL activity for the secreted CM from . Our results hint at active site features, particularly a Val at the bottom of the substrate-binding pocket that may have served as a steppingstone for the evolution of IPL activity in a primordial CM.

摘要

PchB是一种异分支酸丙酮酸裂解酶(IPL),参与[具体物种]中铁载体的生物合成。除了催化异分支酸的[1,5] - 迁移重排反应外,PchB还具有较弱的分支酸变位酶(CM)活性,可促进分支酸的[3,3] - 迁移转化。有人提出,次生代谢酶PchB是从初级代谢CM前体进化而来的。在此,我们采用定向进化将PchB(反向)转化为一种高效的CM。对PchB与来自[具体物种]的典型CM之间活性位点周围总共七个不同的残基进行随机化处理,然后对所得基因文库进行CM活性筛选。在营养缺陷型菌株中进行生长筛选后,出现了一种CM活性提高了10倍的催化剂。对这种改进后的酶在三个活性位点位置再次进行随机化处理并进行筛选,得到了一个PchB变体,其催化常数(kcat/Km)为96,000 M-1 s-1,比亲本酶高40倍,且完全处于专用天然CM的范围内。通过定向进化将IPL轻松转化为CM这一事实与以下情况相符:这两个反应均通过机理上有趣的周环过程进行,而这种反应类型在酶中很少被使用。当探究典型的已确立的CM的催化多效性时,我们发现来自[具体物种]的分泌型CM具有虚假的IPL活性。我们的结果暗示了活性位点特征,特别是底物结合口袋底部的一个缬氨酸,它可能是原始CM中IPL活性进化的一个垫脚石。

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