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On the routine use of soft X-rays in macromolecular crystallography. Part IV. Efficient determination of anomalous substructures in biomacromolecules using longer X-ray wavelengths.

机译:在大分子晶体学中常规使用软X射线。第四部分使用更长的X射线波长可以有效确定生物大分子中异常的子结构。

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摘要

23 different crystal forms of 19 different biological macromolecules were examined with respect to their anomalously scattering substructures using diffraction data collected at a wavelength of 2.0 A (6.2 keV). In more than 90% of the cases the substructure was found to contain more than just the protein S atoms. The data presented suggest that chloride, sulfate, phosphate or metal ions from the buffer or even from the purification protocol are frequently bound to the protein molecule and that these ions are often overlooked, especially if they are not bound at full occupancy. Thus, in order to fully describe the macromolecule under study, it seems desirable that any structure determination be complemented with a long-wavelength data set.
机译:使用在2.0 A(6.2 keV)波长下收集的衍射数据,检查了19种不同生物大分子的23种不同晶体形式的异常散射亚结构。在超过90%的情况下,发现亚结构不仅包含蛋白质S原子,还包含更多的蛋白质。呈现的数据表明,来自缓冲液甚至来自纯化方案的氯离子,硫酸根,磷酸根或金属离子经常与蛋白质分子结合,并且这些离子经常被忽略,尤其是如果它们未完全结合时。因此,为了充分描述所研究的大分子,似乎需要将任何结构确定与长波长数据集相补充。

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