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尿素与溶菌酶相互作用的结构基础。

A structural basis for the interaction of urea with lysozyme.

作者信息

Pike A C, Acharya K R

机构信息

School of Biology and Biochemistry, University of Bath, United Kingdom.

出版信息

Protein Sci. 1994 Apr;3(4):706-10. doi: 10.1002/pro.5560030419.

Abstract

The effect of urea on the crystal structure of hen egg-white lysozyme has been investigated using X-ray crystallography. High resolution structures have been determined from crystals grown in the presence of 0, 0.7, 2, 3, 4, and 5 M urea and from crystals soaked in 9 M urea. All the forms are essentially isomorphous with the native type II crystals, and the derived structures exhibit excellent geometry and RMS differences from ideality in bond distances and angles. Comparison of the urea complex structures with the native enzyme (type II form, at 1.5 A resolution) indicates that the effect of urea is minimal over the concentration range studied. The mean difference in backbone conformation between the native enzyme and its urea complexes varies from 0.18 to 0.49 A. Conformational changes are limited to flexible surface loops (Thr 69-Asn 74, Ser 100-Asn 103), the active site loop (Asn 59-Cys 80), and the C-terminus (Cys 127-Leu 129). Urea molecules are bound to distinct sites on the surface of the protein. One molecule is bound to the active site cleft's C subsite, at all concentrations, in a fashion analogous to that of the N-acetyl substituent of substrate and inhibitor sugars normally bound to this site. Occupation of this subsite by urea alone does not appear to induce the conformational changes associated with inhibitor binding.

摘要

已使用X射线晶体学研究了尿素对鸡蛋清溶菌酶晶体结构的影响。已从在0、0.7、2、3、4和5 M尿素存在下生长的晶体以及浸泡在9 M尿素中的晶体中确定了高分辨率结构。所有形式与天然II型晶体基本同晶型,并且推导的结构在键距和角度方面显示出优异的几何形状和与理想值的均方根偏差。将尿素复合物结构与天然酶(II型形式,分辨率为1.5 Å)进行比较表明,在所研究的浓度范围内尿素的影响最小。天然酶与其尿素复合物之间主链构象的平均差异在0.18至0.49 Å之间变化。构象变化仅限于柔性表面环(Thr 69 - Asn 74,Ser 100 - Asn 103)、活性位点环(Asn 59 - Cys 80)和C末端(Cys 127 - Leu 129)。尿素分子结合到蛋白质表面的不同位点。在所有浓度下,一个分子以类似于通常结合到该位点的底物和抑制剂糖的N - 乙酰取代基的方式结合到活性位点裂隙的C亚位点。仅尿素占据该亚位点似乎不会诱导与抑制剂结合相关的构象变化。

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