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Carbon and amide detect backbone assignment methods of a novel repeat protein from the staphylocoagulase in S. aureus

机译:碳和酰胺检测金黄色葡萄球菌葡萄球菌凝固酶新重复蛋白的骨架分配方法

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摘要

The C-terminal repeat domain of staphylocoagulase that is secreted by the S. aureus is believed to play an important role interacting with fibrinogen and promotes blood clotting. To study this interaction by NMR, full assignment of each amide residue in the HSQC spectrum was required. Despite of the short sequence of the repeat construct, the HSQC spectrum contained a substantial amount of overlapped and exchange broadened resonances, indicating little secondary or tertiary structure. This caused severe problems while using the conventional, amide based NMR method for the backbone assignment. With the growing interest in small apparently disordered proteins, these issues are being faced more frequently. An alternative strategy to improve the backbone assignment capability involved carbon direct detection methods. Circumventing the amide proton detection offers a larger signal dispersion and more uniform signal intensity. For peptides with higher concentrations and in combination with the cold carbon channels of new cryoprobes, higher fields, and sufficiently long relaxation times, the disadvantage of the lower sensitivity of the 13C nucleus can be overcome. Another advantage of this method is the assignment of the proline backbone residues. Complete assignment with the carbon-detected strategy was achieved with a set of only two 3D, one 2D, and a HNCO measurement, which was necessary to translate the information to the HSQC spectrum.
机译:金黄色葡萄球菌分泌的葡萄球菌凝固酶的C末端重复域被认为与纤维蛋白原相互作用并促进血液凝结起着重要作用。为了通过NMR研究这种相互作用,需要对HSQC光谱中的每个酰胺残基进行完全分配。尽管重复序列的序列很短,但HSQC光谱仍包含大量重叠和交换加宽的共振,表明几乎没有二级或三级结构。在使用常规的基于酰胺的NMR方法进行主链分配时,这引起了严重的问题。随着人们对小型表观无序蛋白的兴趣日益浓厚,这些问题正日益面临。改善骨干分配能力的替代策略涉及碳直接检测方法。绕过酰胺质子检测可提供更大的信号分散度和更均匀的信号强度。对于更高浓度的肽,并结合新的低温探针的冷碳通道,更高的视野和足够长的弛豫时间,可以克服 13 C核灵敏度较低的缺点。该方法的另一个优点是脯氨酸主链残基的分配。仅通过一组两个3D,一个2D和一个HNCO测量就可以完成碳检测策略的完全分配,这对于将信息转换为HSQC光谱是必不可少的。

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