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首页> 外文期刊>The Journal of Biochemistry >Probing dynamics and conformational change of the GroEL-GroES complex by 13C NMR spectroscopy.
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Probing dynamics and conformational change of the GroEL-GroES complex by 13C NMR spectroscopy.

机译:通过13C NMR光谱探测GroEL-GroES配合物的动力学和构象变化。

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摘要

Bacterial chaperonin GroEL with a molecular mass of 800 kDa was studied by (13)C NMR spectroscopy. Carbonyl carbons of GroEL were labeled with (13)C in an amino acid specific manner in order to reduce the number of signals to be observed in the spectrum. Combination of selective labeling and site-directed mutagenesis enabled us to establish the sequence specific assignment of the (13)C resonances from GroEL. ADP-binding induced a chemical shift change of Tyr478 in the equatorial domain and His401 in the intermediate domain, but little of Tyr203 in the apical domain. Upon complex formation with co-chaperonin GroES in the presence of ADP, Tyr478 exhibits two peaks that would originate from the cis and trans rings of the asymmetric GroEL-GroES complex. Comparison between the line width of the GroEL resonances and those from GroES in complex with GroEL revealed broadening disproportionate to the size of GroEL, implying the existence of conformational fluctuations which may be pertinent to the chaperone activity. Based on these results, we concluded that (13)C NMR observation in combination with selective labeling and site-directed mutagenesis can be utilized for probing the conformational change and dynamics of the extremely large molecules that are inaccessible with current NMR methods.
机译:通过(13)C NMR光谱研究了分子量为800kDa的细菌伴侣蛋白GroEL。 GroEL的羰基碳以氨基酸特异性方式用(13)C标记,以减少在光谱中观察到的信号数量。选择性标记和定点诱变的结合使我们能够建立来自GroEL的(13)C共振的序列特异性分配。 ADP绑定诱导赤道域中的Tyr478和中间域中的His401的化学位移变化,而在顶端域中的Tyr203很少。在ADP存在下与伴侣蛋白GroES形成复合物后,Tyr478出现两个峰,它们起源于不对称GroEL-GroES复合物的顺式和反式环。 GroEL共振的线宽和GroES与GroEL配合使用的GroES共振的线宽之间的比较显示,与GroEL的尺寸不成比例地变宽,这意味着可能存在与伴侣活性有关的构象波动。根据这些结果,我们得出的结论是,(13)C NMR观察与选择性标记和定点诱变相结合可用于探测当前NMR方法无法接近的超大分子的构象变化和动力学。

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