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比较软骨素酶 ABC I 结构上连接螺旋的相似版本。

Comparing similar versions of a connecting helix on the structure of Chondroitinase ABC I.

机构信息

Department of Biology, Faculty of Sciences, University of Zanjan, Zanjan, Iran.

Department of Biochemistry, Faculty of Biological Sciences, Tarbiat Modares University, Tehran, Iran.

出版信息

Enzyme Microb Technol. 2022 Oct;160:110073. doi: 10.1016/j.enzmictec.2022.110073. Epub 2022 Jun 6.

Abstract

Regarding the existence of similar helices on the structure of different proteins, recently, novel variants of Chondroitinase ABC I (cABC I) have been constructed, where a representative helix between two structural motifs in Chondroitinase ABC I from Proteus vulgaris has been replaced by similar versions of helices found in other proteins. The previous study has revealed that the structural features and the activity of double mutants M886A/G887E (inspired by the 30 S ribosomal protein S1 from Geminocystis herdmanii) and M889I/Q891K (inspired by the chondroitin lyase from Proteus mirabilis) is comparable with that of wild-type (WT) cABC I. Here, the kinetic parameters of the enzyme activity for the WT and double mutants were determined. Of the recombinant double mutants, M889I/Q891K gave the highest catalytic efficiency with the k/K value of approximately 2.3-fold increase, as compared with the WT and M886A/G887E. Modeling of experimental data showed that the mechanism of the heat-induced structural alteration, and the enzyme-substrate complex formation, changed upon mutation. These natural versions of the connecting helix can be used as an efficient linker in protein engineering studies as well as those investigations involving the use of biological linkers.

摘要

关于不同蛋白质结构中存在类似螺旋的问题,最近,已经构建了新型 Chondroitinase ABC I(cABC I)变体,其中变形菌 Proteus vulgaris 中的 Chondroitinase ABC I 两个结构基序之间的代表性螺旋已被其他蛋白质中发现的类似版本的螺旋所取代。先前的研究表明,双突变体 M886A/G887E(受粪产碱菌 30S 核糖体蛋白 S1 启发)和 M889I/Q891K(受变形奇异菌软骨素裂解酶启发)的结构特征和活性与野生型(WT)cABC I 相当。在这里,测定了酶活性的 WT 和双突变体的动力学参数。在重组双突变体中,与 WT 和 M886A/G887E 相比,M889I/Q891K 的催化效率最高,k/K 值约增加了 2.3 倍。实验数据的建模表明,热诱导结构改变的机制以及酶-底物复合物的形成在突变后发生了变化。这些连接螺旋的天然变体可用于蛋白质工程研究以及涉及使用生物接头的研究。

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