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在共结晶条件下,内在蛋白质无序可能被忽视:一个同步辐射圆二色光谱的案例研究。

Intrinsic protein disorder could be overlooked in cocrystallization conditions: An SRCD case study.

作者信息

Németh Eszter, Balogh Ria K, Borsos Katalin, Czene Anikó, Thulstrup Peter W, Gyurcsik Béla

机构信息

Department of Inorganic and Analytical Chemistry, University of Szeged, Szeged, 6720, Hungary.

MTA-SZTE, Bioinorganic Chemistry Research Group, Hungarian Academy of Sciences, Szeged, 6720, Hungary.

出版信息

Protein Sci. 2016 Nov;25(11):1977-1988. doi: 10.1002/pro.3010. Epub 2016 Aug 23.

Abstract

X-ray diffractometry dominates protein studies, as it can provide 3D structures of these diverse macromolecules or their molecular complexes with interacting partners: substrates, inhibitors, and/or cofactors. Here, we show that under cocrystallization conditions the results could reflect induced protein folds instead of the (partially) disordered original structures. The analysis of synchrotron radiation circular dichroism spectra revealed that the Im7 immunity protein stabilizes the native-like solution structure of unfolded NColE7 nuclease mutants via complex formation. This is consistent with the fact that among the several available crystal structures with its inhibitor or substrate, all NColE7 structures are virtually the same. Our results draw attention to the possible structural consequence of protein modifications, which is often hidden by compensational effects of intermolecular interactions. The growing evidence on the importance of protein intrinsic disorder thus, demands more extensive complementary experiments in solution phase with the unligated form of the protein of interest.

摘要

X射线衍射法在蛋白质研究中占据主导地位,因为它能够提供这些多样的大分子及其与相互作用伙伴(底物、抑制剂和/或辅因子)形成的分子复合物的三维结构。在此,我们表明在共结晶条件下,结果可能反映的是诱导的蛋白质折叠,而非(部分)无序的原始结构。同步辐射圆二色光谱分析表明,Im7免疫蛋白通过形成复合物来稳定未折叠的NColE7核酸酶突变体的天然样溶液结构。这与以下事实相符:在其与抑制剂或底物的几种可用晶体结构中,所有NColE7结构实际上都是相同的。我们的结果提醒人们注意蛋白质修饰可能产生的结构后果,而这种后果常常被分子间相互作用的补偿效应所掩盖。因此,越来越多关于蛋白质内在无序重要性的证据表明,需要对感兴趣的蛋白质的未结合形式在溶液相中进行更广泛的补充实验。

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