首页> 外文期刊>Protein Science: A Publication of the Protein Society >The orientations of cytochrome c in the highly dynamic complex with cytochrome b5 visualized by NMR and docking using HADDOCK.
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The orientations of cytochrome c in the highly dynamic complex with cytochrome b5 visualized by NMR and docking using HADDOCK.

机译:通过NMR可视化并与HADDOCK对接,可在高度动态的复合物中与细胞色素b5的细胞色素c定向。

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The interaction of bovine microsomal ferricytochrome b5 with yeast iso-1-ferri and ferrocytochrome c has been investigated using heteronuclear NMR techniques. Chemical-shift perturbations for 1H and 15N nuclei of both cytochromes, arising from the interactions with the unlabeled partner proteins, were used for mapping the interacting surfaces on both proteins. The similarity of the binding shifts observed for oxidized and reduced cytochrome c indicates that the complex formation is not influenced by the oxidation state of the cytochrome c. Protein-protein docking simulations have been performed for the binary cytochrome b5-cytochrome c and ternary (cytochrome b5)-(cytochrome c)2 complexes using a novel HADDOCK approach. The docking procedure, which makes use of the experimental data to drive the docking, identified a range of orientations assumed by the proteins in the complex. It is demonstrated that cytochrome c uses a confined surface patch for interaction with a much more extensive surface area of cytochrome b5. Taken together, the experimental data suggest the presence of a dynamic ensemble of conformations assumed by the proteins in the complex.
机译:使用异核NMR技术研究了牛微粒体铁细胞色素b5与酵母异1-铁和铁细胞色素c的相互作用。与未标记的伴侣蛋白相互作用产生的两种细胞色素1H和15N核的化学位移扰动用于绘制两种蛋白上相互作用的表面的图谱。对于氧化和还原的细胞色素c观察到的结合位移的相似性表明,复合物的形成不受细胞色素c氧化态的影响。已使用新型HADDOCK方法对二元细胞色素b5-细胞色素c和三元(细胞色素b5)-(细胞色素c)2复合物进行了蛋白质-蛋白质对接模拟。利用实验数据驱动对接的对接程序确定了复合物中蛋白质所假定的一系列方向。已经证明,细胞色素c使用受限的表面补丁与细胞色素b5的更大表面积相互作用。两者合计,实验数据表明存在由复合物中的蛋白质假定的构象的动态整体。

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