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Merging of synchrotron serial crystallographic data by a genetic algorithm

机译:合并的同步串行晶体数据由遗传算法

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摘要

Recent advances in macromolecular crystallography have made it practical to rapidly collect hundreds of sub‐data sets consisting of small oscillations of incomplete data. This approach, generally referred to as serial crystallography, has many uses, including an increased effective dose per data set, the collection of data from crystals without harvesting ( in situ data collection) and studies of dynamic events such as catalytic reactions. However, selecting which data sets from this type of experiment should be merged can be challenging and new methods are required. Here, it is shown that a genetic algorithm can be used for this purpose, and five case studies are presented in which the merging statistics are significantly improved compared with conventional merging of all data.
机译:大分子晶体学的最新进展取得了快速收集实用吗数以百计的辅助数据集组成的小不完整的数据的振荡。一般称为串行结晶学,有许多用途,包括增加有效每个数据集,数据的收集没有收获的晶体(原位数据集合)和研究动态等事件催化反应。从这种类型的实验数据集合并可以挑战和新的方法必需的。算法可用于这一目的,5案例研究提出了合并统计数据相比显著提高与传统的合并所有数据。

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