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Engineered control of enzyme structural dynamics and function

机译:工程控制酶的结构动力学和功能

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摘要

Enzymes undergo a range of internal motions from local, active site fluctuations to large‐scale, global conformational changes. These motions are often important for enzyme function, including in ligand binding and dissociation and even preparing the active site for chemical catalysis. Protein engineering efforts have been directed towards manipulating enzyme structural dynamics and conformational changes, including targeting specific amino acid interactions and creation of chimeric enzymes with new regulatory functions. Post‐translational covalent modification can provide an additional level of enzyme control. These studies have not only provided insights into the functional role of protein motions, but they offer opportunities to create stimulus‐responsive enzymes. These enzymes can be engineered to respond to a number of external stimuli, including light, pH, and the presence of novel allosteric modulators. Altogether, the ability to engineer and control enzyme structural dynamics can provide new tools for biotechnology and medicine.
机译:酶经历一系列内部运动,从局部活动位点波动到大规模,整体构象变化。这些运动通常对酶的功能很重要,包括配体结合和解离,甚至为化学催化准备活性位点。蛋白质工程研究的方向已转向操纵酶的结构动力学和构象变化,包括靶向特定的氨基酸相互作用和创建具有新调控功能的嵌合酶。翻译后共价修饰可以提供更高水平的酶控制。这些研究不仅提供了对蛋白质运动功能作用的见解,而且为创造刺激响应酶提供了机会。可以对这些酶进行改造,使其对多种外部刺激作出反应,包括光照,pH值和新型变构调节剂的存在。总之,工程学和控制酶结构动力学的能力可以为生物技术和医学提供新的工具。

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