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软X射线的见解:CK2α/DRB复合物的氯和硫亚结构

Insights from soft X-rays: the chlorine and sulfur sub-structures of a CK2alpha/DRB complex.

作者信息

Raaf Jennifer, Issinger Olaf-Georg, Niefind Karsten

机构信息

Universität zu Köln, Institut für Biochemie, Zülpicher Strasse 47, 50674, Köln, Germany.

出版信息

Mol Cell Biochem. 2008 Sep;316(1-2):15-23. doi: 10.1007/s11010-008-9826-1. Epub 2008 Jul 8.

DOI:10.1007/s11010-008-9826-1
PMID:18607692
Abstract

The diffraction pattern of a protein crystal is normally a product of the interference of electromagnetic waves scattered by electrons of the crystalline sample. The diffraction pattern undergoes systematic changes in case additionally X-ray absorption occurs, meaning if the wavelength of the primary X-ray beam is relatively close to the absorption edge of selected elements of the sample. The resulting effects are summarized as "anomalous dispersion" and can be always observed with "soft" X-rays (wavelength around 2 A) since they match the absorption edges of sulfur and chlorine. A particularly useful application of this phenomenon is the experimental detection of the sub-structures of the anomalous scatterers in protein crystals. We demonstrate this here with a crystal of a C-terminally truncated variant of human CK2alpha to which two molecules of the inhibitor 5,6-dichloro-1-beta-D-ribo-furanosyl-benzimidazole (DRB) are bound. The structure of this co-crystal has been solved recently. For this study we measured an additional diffraction data set at a wavelength of 2 A which showed strong anomalous dispersion effects. On the basis of these effects we detected all sulfur atoms of the protein, the two liganded DRB molecules and a total of 16 additional chloride ions some of them emerging at positions filled with water molecules in previous structure determinations. A number of chloride ions are bound to structural and functional important locations fitting to the constitutive activity and the acidophilic substrate specificity of the enzyme.

摘要

蛋白质晶体的衍射图案通常是由晶体样品中的电子散射的电磁波干涉产生的。如果额外发生X射线吸收,即如果初级X射线束的波长相对接近样品中选定元素的吸收边缘,衍射图案会发生系统性变化。由此产生的效应被总结为“反常色散”,并且用“软”X射线(波长约为2埃)总能观察到这种现象,因为它们与硫和氯的吸收边缘相匹配。这种现象的一个特别有用的应用是对蛋白质晶体中反常散射体的亚结构进行实验检测。我们在此用人类CK2α C末端截短变体的晶体来证明这一点,该晶体结合了两个抑制剂5,6-二氯-1-β-D-呋喃核糖基苯并咪唑(DRB)分子。这种共晶体的结构最近已得到解析。在本研究中,我们在2埃波长下测量了一组额外的衍射数据集,该数据集显示出强烈的反常色散效应。基于这些效应,我们检测到了蛋白质的所有硫原子、两个配位的DRB分子以及总共16个额外的氯离子,其中一些氯离子在先前的结构测定中出现在水分子占据的位置。许多氯离子结合在对酶的组成活性和嗜酸底物特异性至关重要的结构和功能位置上。

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