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首页> 外文期刊>Angewandte Chemie >Directed Evolution of an Artificial Imine Reductase
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Directed Evolution of an Artificial Imine Reductase

机译:人工亚洲还原酶的定向演变

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Artificial metalloenzymes, resulting from incorporation of a metal cofactor within a host protein, have received increasing attention in the last decade. The directed evolution is presented of an artificial transfer hydrogenase (ATHase) based on the biotin-streptavidin technology using a straightforward procedure allowing screening in cell-free extracts. Two streptavidin isoforms were yielded with improved catalytic activity and selectivity for the reduction of cyclic imines. The evolved ATHases were stable under biphasic catalytic conditions. The X-ray structure analysis reveals that introducing bulky residues within the active site results in flexibility changes of the cofactor, thus increasing exposure of the metal to the protein surface and leading to a reversal of enantioselectivity. This hypothesis was confirmed by a multiscale approach based mostly on molecular dynamics and protein-ligand dockings.
机译:由于在宿主蛋白内掺入金属辅因子而导致的人造金属酶在过去十年中得到了越来越多的关注。 通过使用直接的程序呈现基于生物素 - 链霉抗生物素蛋白技术的人工转移氢酶(Athase)的定向演变,允许在无细胞提取物中筛选。 产生两种链霉抗生物素蛋白同种型,得到改善的催化活性和选择性,用于减少环状亚胺。 在双相催化条件下,进化的疗法稳定。 X射线结构分析显示,在活性部位内引入庞大残留会导致辅助因子的柔韧性变化,从而增加金属暴露于蛋白质表面并导致对映射性的逆转。 通过多尺度方法基于分子动力学和蛋白质配体斩波来证实该假设。

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