首页> 外文期刊>Acta crystallographica. Section D, Structural biology. >Well-based crystallization of lipidic cubic phase microcrystals for serial X-ray crystallography experiments
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Well-based crystallization of lipidic cubic phase microcrystals for serial X-ray crystallography experiments

机译:建立油脂的立方相的结晶微晶核系列x射线晶体学实验

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摘要

Serial crystallography is having an increasing impact on structural biology. This emerging technique opens up new possibilities for studying protein structures at room temperature and investigating structural dynamics using time-resolved X-ray diffraction. A limitation of the method is the intrinsic need for large quantities of well ordered micrometre-sized crystals. Here, a method is presented to screen for conditions that produce microcrystals of membrane proteins in the lipidic cubic phase using a well-based crystallization approach. A key advantage over earlier approaches is that the progress of crystal formation can be easily monitored without interrupting the crystallization process. In addition, the protocol can be scaled up to efficiently produce large quantities of crystals for serial crystallography experiments. Using the well-based crystallization methodology, novel conditions for the growth of showers of microcrystals of three different membrane proteins have been developed. Diffraction data are also presented from the first user serial crystallography experiment performed at MAX IV Laboratory.
机译:连续结晶学是有增加对结构生物学的影响。技术为研究开辟了新的可能性在室温和蛋白质结构研究结构动力学使用时间分辨的x射线衍射。该方法的内在需要大量的命令micrometre-sized晶体。产生微晶核的条件膜蛋白在油脂的立方相通过建立结晶的方法。方法是早些时候关键优势晶体的形成可以很容易地进步监控不打断结晶的过程。协议可以扩大有效地生产大量的水晶系列晶体学实验。结晶方法,新的条件淋浴的微晶核的生长三个人们提出了不同的膜蛋白。提出从衍射数据第一个用户串行晶体学实验在马克斯第四实验室。

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