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Membrane crystallization of macromolecular solutions

机译:大分子溶液的膜结晶

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摘要

Crystal growth is the critical step in determining the protein X-ray crystal structure. Hundreds, or even thousands, of crystallization trials must often be performed on a target macromolecule and, unfortunately, less than 1% of them typically yield promising results. Many macromolecules are reluctant to crystallize and, usually, their crystalline arrangement is not good enough to provide diffraction data at a resolution sufficient to establish struture-function correlation. The history of macromolecular crystallization emphasizes the importance of new observations and ideas that are useful in initiating more systematic studies using novel technieques and creative approaches. On this basis an innovative methodology, the membrane crystallization, has been introduced in order to promote the formation of macromolecular crystals. Lysozyme crystals, produced by removing the solvent (in vapour phase) from the protein solution by using microporous hydrophobic membranes, showed a good structural quality suitable for successive X-ray diffraction analysis.
机译:晶体生长是确定蛋白质X射线晶体结构的关键步骤。通常必须在目标大分子上进行数百甚至数千次结晶试验,但不幸的是,少于1%的结晶通常会产生可喜的结果。许多大分子不愿结晶,通常,它们的结晶排列不足以提供足以建立结构-功能相关性的分辨率的衍射数据。大分子结晶的历史强调了新的观察和观点的重要性,这些观点和观点对于使用新颖的技术和创造性的方法开展更系统的研究非常有用。在此基础上,引入了一种创新的方法,即膜结晶法,以促进大分子晶体的形成。通过使用微孔疏水膜从蛋白质溶液中去除溶剂(气相)而产生的溶菌酶晶体,具有良好的结构质量,适用于连续的X射线衍射分析。

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