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MR‐REX MR‐REX : molecular replacement by cooperative conformational search and occupancy optimization on low‐accuracy protein models

机译:像雷克斯先生要像雷克斯先生:分子置换合作构象搜索和入住率优化低蛋白质模型准确性

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摘要

Molecular replacement (MR) has commonly been employed to derive the phase information in protein crystal X‐ray diffraction, but its success rate decreases rapidly when the search model is dissimilar to the target. MR‐REX has been developed to perform an MR search by replica‐exchange Monte Carlo simulations, which enables cooperative rotation and translation searches and simultaneous clash and occupancy optimization. MR‐REX was tested on a set of 1303 protein structures of different accuracies and successfully placed 699 structures at positions that have an r.m.s.d. of below 2?? to the target position, which is 10% higher than was obtained by Phaser . However, cases studies show that many of the models for which Phaser failed and MR‐REX succeeded can be solved by Phaser by pruning them and using nondefault parameters. The factors effecting success and the parts of the methodology which lead to success are studied. The results demonstrate a new avenue for molecular replacement which outperforms (and has results that are complementary to) the state‐of‐the‐art MR methods, in particular for distantly homologous proteins.
机译:一般分子置换(先生)推导了相位信息但其蛋白质晶体X射线衍射应承担的当搜索成功率下降迅速模型是不同的目标。开发执行搜索副本交换应承担的蒙特卡罗模拟,使合作旋转和翻译搜索和同时发生的冲突和入住率优化。不同的精度和蛋白质结构成功地将699结构的位置下面的r.m.s.d. 2 ? ?位置,高出10%移相器。移相器的模型失败,奥雷克斯成功可以通过移相器通过修剪来解决和使用默认的参数。影响成功的部分研究方法导致成功。结果显示一个新的途径分子替代优于(,补充)的结果应承担的艺术状态优先车道先生的方法,特别是冷淡地同源蛋白质。

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