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Molecular engineering of myosin

机译:肌球蛋白的分子工程

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摘要

Protein engineering and design provide excellent tools to investigate the principles by which particular structural features relate to the mechanisms that underlie the biological function of a protein. In addition to studies aimed at dissecting the communication pathways within enzymes, recent advances in protein engineering approaches make it possible to generate enzymes with increased catalytic efficiency and specifically altered or newly introduced functions. Here, two approaches using state-of-the-art protein design and engineering are described in detail to demonstrate how key features of the myosin motor can be changed in a specific and predictable manner. First, it is shown how replacement of an actin-binding surface loop with synthetic sequences, whose flexibility and charge density is varied, can be employed to manipulate the acrin affinity, the catalytic activity and the efficiency of coupling between actin- and nucleotide-binding sites of myosin motor constructs. Then the use of pre-existing molecular building blocks, which are derived from unrelated proteins, is described for manipulating the velocity and even the direction of movement of recombinant myosins.
机译:蛋白质工程和设计提供了出色的工具,可用来研究特定结构特征与构成蛋白质生物学功能基础的机制有关的原理。除了旨在剖析酶内通信途径的研究之外,蛋白质工程方法的最新进展还使得可能产生具有提高的催化效率并特别改变或新引入的功能的酶。在此,详细介绍了使用最新蛋白质设计和工程方法的两种方法,以展示如何以特定且可预测的方式改变肌球蛋白马达的关键特征。首先,显示了如何用合成序列代替肌动蛋白结合表面环,其柔性和电荷密度是变化的,可用于操纵蛋白的亲和力,催化活性以及肌动蛋白与核苷酸结合之间的偶联效率肌球蛋白运动结构的位点。然后,描述了使用源自不相关蛋白质的预先存在的分子构件来操纵重组肌球蛋白的速度甚至运动方向。

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