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Engineering an artificial zymogen by alternate frame protein folding

机译:通过交替的框架蛋白折叠工程化人工酶原

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摘要

Alternate frame folding (AFF) is a novel mechanism by which allostery can be introduced into a protein where none may have existed previously. We employ this technology to convert the cytotoxic ribonuclease barnase into an artificial zymogen that is activated by HIV-1 protease. The AFF modification entails partial duplication of the polypeptide chain and mutation of a key catalytic residue in one of the duplicated segments. The resulting molecule can fold in one of two “frames” to yield the wild-type structure or a circularly permuted form in which the positions of the N- and C-termini are exchanged with a surface loop. It cannot take on both structures simultaneously because each competes for a shared amino acid sequence. An HIV-1 protease recognition sequence is inserted into one of the surface loops in the nonpermuted frame, and cleavage induces a shift from the nonpermuted fold to the permuted fold. Using the AFF mechanism, we were able to suppress kcat/KM by 250-fold in the proenzyme relative to wild-type barnase. HIV-1 protease cleavage subsequently increases kcat/KM by 130-fold. AFF is significant because it is general and can in principle be used to control activity of many enzymes, including those whose functions are not regulated by any existing mechanism.
机译:交替折叠框架(AFF)是一种新颖的机制,可通过该机制将变构引入到以前可能不存在的蛋白质中。我们采用这项技术将细胞毒性核糖核酸酶barnase转换为由HIV-1蛋白酶激活的人工酶原。 AFF修饰需要在重复的片段之一中部分重复多肽链和关键催化残基的突变。所得分子可以在两个“框架”之一中折叠以产生野生型结构或圆形排列形式,其中N和C末端的位置与表面环交换。它不能同时具有两个结构,因为每个结构都竞争一个共享的氨基酸序列。将HIV-1蛋白酶识别序列插入非置换框架的一个表面环中,切割会导致从非置换折叠向置换折叠的转变。使用AFF机制,我们能够将kcat / KM抑制的酶量相对于野生型芽孢杆菌酶而言高250倍。 HIV-1蛋白酶裂解随后使kcat / KM增加130倍。 AFF是很重要的,因为它是通用的,原则上可以用来控制许多酶的活性,包括那些功能不受任何现有机制调控的酶。

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