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Bridging conformational dynamics and function using single-molecule spectroscopy

机译:使用单分子光谱技术桥接构象动力学和功能

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摘要

In a typical structure-function relation study, the primary structure of proteins or nucleic acids is changed by mutagenesis and its functional effect is measured via biochemical means. Single-molecule spectroscopy has begun to give a whole new meaning to the "structure-function relation" by measuring the realtime conformational changes of individual biological macromolecules while they are functioning. This review discusses a few recent examples: untangling internal chemistry and conformational dynamics of a ribozyme, branch migration landscape of a Holliday junction at a single-step resolution, tRNA selection and dynamics in a ribosome, repetitive shuttling and snapback of a helicase, and discrete rotation of an ATP synthase.
机译:在典型的结构-功能关系研究中,蛋白质或核酸的一级结构通过诱变而改变,并且其功能作用是通过生化手段测量的。通过测量单个生物大分子运行时的实时构象变化,单分子光谱学已开始为“结构-功能关系”赋予全新的含义。这篇综述讨论了一些最近的例子:核酶的内部化学和构象动力学的混乱,单步分离的霍利迪结的分支迁移态势,核糖体中的tRNA选择和动力学,解旋酶的重复穿梭和回弹以及离散ATP合酶的旋转。

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