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The use of biophysical methods increases success in obtaining liganded crystal structures

机译:生物物理方法的使用增加了获得配体晶体结构的成功

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摘要

In attempts to determine the crystal structure of small molecule–protein complexes, a common frustration is the absence of ligand binding once the protein structure has been solved. While the first structure, even with no ligand bound (apo), can be a cause for celebration, the solution of dozens of apo structures can give an unwanted sense of déjà vu. Much time and material is wasted on unsuccessful experiments, which can have a serious impact on productivity and morale. There are many reasons for the lack of observed binding in crystals and this paper highlights some of these. Biophysical methods may be used to confirm and optimize solution conditions to increase the success rate of crystallizing protein–ligand complexes. As there are an overwhelming number of biophysical methods available, some of the factors that need to be considered when choosing the most appropriate technique for a given system are discussed. Finally, a few illustrative examples where biophysical methods have proven helpful in real systems are given.
机译:在尝试确定小分子-蛋白质复合物的晶体结构时,常见的障碍是一旦蛋白质结构被解决,就没有配体结合。尽管第一个结构即使没有配体键合(apo)也可能值得庆祝,但数十种apo结构的解决方案却会给人一种不必要的déjàvu感觉。不成功的实验浪费了很多时间和材料,这会严重影响生产力和士气。缺乏观察到的晶体结合的原因很多,本文重点介绍了其中一些。生物物理方法可用于确认和优化溶液条件,以提高结晶蛋白-配体复合物的成功率。由于存在大量可用的生物物理方法,因此讨论了为给定系统选择最合适的技术时需要考虑的一些因素。最后,给出了一些说明性示例,其中生物物理方法已被证明对实际系统有用。

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