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Coping with strong translational noncrystallographic symmetry and extreme anisotropy in molecular replacement with Phaser: human Rab27a

机译:在使用Phaser替代分子时应对强翻译非晶体对称性和极端各向异性:人类Rab27a

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摘要

Data pathologies caused by effects such as diffraction anisotropy and translational noncrystallographic symmetry (tNCS) can dramatically complicate the solution of the crystal structures of macromolecules. Such problems were encountered in determining the structure of a mutant form of Rab27a, a member of the Rab GTPases. Mutant Rab27a constructs that crystallize in the free form were designed for use in the discovery of drugs to reduce primary tumour invasiveness and metastasis. One construct, hRab27aMut, crystallized within 24 h and diffracted to 2.82 Å resolution, with a unit cell possessing room for a large number of protein copies. Initial efforts to solve the structure using molecular replacement by Phaser were not successful. Analysis of the data set revealed that the crystals suffered from both extreme anisotropy and strong tNCS. As a result, large numbers of reflections had estimated standard deviations that were much larger than their measured intensities and their expected intensities, revealing problems with the use of such data at the time in Phaser. By eliminating extremely weak reflections with the largest combined effects of anisotropy and tNCS, these problems could be avoided, allowing a molecular-replacement solution to be found. The lessons that were learned in solving this structure have guided improvements in the numerical analysis used in Phaser, particularly in identifying diffraction measurements that convey very little information content. The calculation of information content could also be applied as an alternative to ellipsoidal truncation. The post-mortem analysis also revealed an oversight in accounting for measurement errors in the fast rotation function. While the crystal of mutant Rab27a is not amenable to drug screening, the structure can guide new modifications to obtain more suitable crystal forms.
机译:由诸如衍射各向异性和平移非晶体对称性(tNCS)之类的效应引起的数据病理会极大地使大分子晶体结构的解决方案复杂化。在确定Rab GTPases成员Rab27a突变形式的结构时遇到了此类问题。将以游离形式结晶的突变Rab27a构建体设计用于发现减少原发性肿瘤侵袭和转移的药物。一种构建体hRab27a Mut ,在24h内结晶并衍射至2.82A分辨率,其单位细胞具有大量蛋白质拷贝的空间。通过使用Phaser进行分子替代来解决结构的最初努力并未成功。对数据集的分析表明,晶体既具有极端的各向异性又具有强大的tNCS。结果,大量反射的估计标准偏差远大于其测量强度和预期强度,这揭示了当时在Phaser中使用此类数据的问题。通过消除具有各向异性和tNCS的最大组合效应的极弱反射,可以避免这些问题,从而找到分子替代解决方案。解决此结构的经验教训指导了Phaser中数值分析的改进,特别是在识别传达很少信息内容的衍射测量方面。信息内容的计算也可以用作椭圆截断的替代方法。事后分析还显示了对快速旋转功能中的测量误差的考虑的监督。尽管突变Rab27a的晶体不适合药物筛选,但其结构可以指导新的修饰以获得更合适的晶体形式。

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