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首页> 外文期刊>CrystEngComm >A microfluidic-based protein crystallization method in 10 micrometer-sized crystallization space
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A microfluidic-based protein crystallization method in 10 micrometer-sized crystallization space

机译:10微米大小的结晶空间中基于微流体的蛋白质结晶方法

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摘要

Protein crystallization and subsequent X-ray diffraction analysis of the three-dimensional structure are necessary for elucidation of the biological functions of proteins and effective rational drug design. Therefore, controlling protein crystallization is important to obtain high resolution X-ray diffraction data. Here, a simple microfluidic method using chips with 10 and 50 mu m high crystallization chambers to selectively form suitable single protein crystals for X-ray analysis is demonstrated. As proof of concept, three different types of proteins: lysozyme, glucokinase from Pseudoalteromonas sp. AS-131 (PsGK), and NADPH-cytochrome P450 oxidoreductase-heme oxygenase complex were crystallized. We demonstrate that the crystal growth orientation depends on the height of the crystallization chamber regardless of the protein type. Our results suggest that the confined micro space induces the protein molecules to adhere to a specific crystal face and affects the growth kinetics of each crystal face. The present microfluidic-based protein crystallization method can reform a suitable single protein crystal for X-ray analysis from aggregates of needle-shaped protein crystals.
机译:蛋白质结晶和随后的三维结构X射线衍射分析对于阐明蛋白质的生物学功能和有效的合理药物设计是必不可少的。因此,控制蛋白质的结晶对于获得高分辨率X射线衍射数据很重要。在此,展示了一种简单的微流体方法,该方法使用具有10和50μm高结晶室的芯片选择性地形成合适的单个蛋白质晶体进行X射线分析。作为概念的证明,三种不同类型的蛋白质:溶菌酶,假单胞菌属物种的葡糖激酶。将AS-131(PsGK)和NADPH-细胞色素P450氧化还原酶-血红素加氧酶复合物结晶。我们证明了晶体的生长方向取决于结晶室的高度,而与蛋白质类型无关。我们的结果表明,狭窄的微空间会诱导蛋白质分子粘附到特定的晶面上,并影响每个晶面的生长动力学。本基于微流体的蛋白质结晶方法可以从针状蛋白质晶体的聚集体中改造出合适的单一蛋白质晶体用于X射线分析。

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