【2h】

Exploring modular allostery via interchangeable regulatory domains

机译:通过可互换的监管领域探索模块化变构

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摘要

Most proteins comprise two or more domains from a limited suite of protein families. These domains are often rearranged in various combinations through gene fusion events to evolve new protein functions, including the acquisition of protein allostery through the incorporation of regulatory domains. The enzyme 3-deoxy-d-arabino-heptulosonate 7-phosphate synthase (DAH7PS) is the first enzyme of aromatic amino acid biosynthesis and displays a diverse range of allosteric mechanisms. DAH7PSs adopt a common architecture with a shared (β/α)8 catalytic domain which can be attached to an ACT-like or a chorismate mutase regulatory domain that operates via distinct mechanisms. These respective domains confer allosteric regulation by controlling DAH7PS function in response to ligand Tyr or prephenate. Starting with contemporary DAH7PS proteins, two protein chimeras were created, with interchanged regulatory domains. Both engineered proteins were catalytically active and delivered new functional allostery with switched ligand specificity and allosteric mechanisms delivered by their nonhomologous regulatory domains. This interchangeability of protein domains represents an efficient method not only to engineer allostery in multidomain proteins but to create a new bifunctional enzyme.
机译:大多数蛋白质包含一组有限的蛋白质家族中的两个或多个域。这些结构域通常通过基因融合事件以各种组合重排以进化新的蛋白质功能,包括通过引入调节域来获得蛋白质变构物。 3-脱氧-d-阿拉伯糖-庚二酸7-磷酸合酶(DAH7PS)是芳香族氨基酸生物合成的第一种酶,并显示出多种变构机制。 DAH7PS采用具有共享(β/α)8催化结构域的通用架构,该结构域可以连接至通过不同机制起作用的ACT样或分支酸突变酶调节域。这些各自的域通过响应配体Tyr或苯甲酸酯来控制DAH7PS功能,从而赋予了变构调节作用。从当代的DAH7PS蛋白开始,创建了两个蛋白嵌合体,它们具有互换的调节域。两种工程蛋白均具有催化活性,并通过交换的配体特异性和由其非同源调节域传递的变构机制传递新的功能变构。蛋白质结构域的这种可互换性不仅代表了一种有效的方法,不仅可以工程化多域蛋白中的变构结构,而且可以创建新的双功能酶。

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