首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Unraveling the interface of signal recognition particle and its receptor by using chemical cross-linking and tandem mass spectrometry.
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Unraveling the interface of signal recognition particle and its receptor by using chemical cross-linking and tandem mass spectrometry.

机译:通过化学交联和串联质谱分析来揭示信号识别颗粒及其受体的界面。

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摘要

Among the methods used to unravel protein interaction surfaces, chemical cross-linking followed by identification of the cross-linked peptides by mass spectrometry has proven especially useful in dynamic and complex systems. During the signal recognition particle (SRP)-dependent targeting of proteins to the bacterial plasma membrane, the specific interaction between Ffh (the protein component of SRP) and FtsY (the SRP receptor) is known to be essential for the efficiency and fidelity of this process. In this work, we studied the Escherichia coli and Thermus aquaticus Ffh.FtsY complexes by using chemical cross-linking and tandem mass spectrometry to identify nine intermolecular cross-linked peptides. This information was used in conjunction with a previously undescribed model-building approach that combines geometric restraint optimization with macromolecular docking. The resulting model of the Ffh.FtsY complex is in good agreement with the crystal structure solved shortly thereafter. Intriguingly, fourof the cross-linked pairs involve the M domain of Ffh, which is absent from the crystal structure, providing previously undocumented experimental evidence that the M domain is positioned in close proximity to the Ffh.FtsY interface in the complex.
机译:在用于解开蛋白质相互作用表面的方法中,化学交联然后通过质谱鉴定交联的肽已被证明在动态和复杂的系统中特别有用。在依赖信号识别颗粒(SRP)的蛋白质靶向细菌质膜的过程中,已知Ffh(SRP的蛋白质成分)和FtsY(SRP受体)之间的特异性相互作用对于该蛋白质的效率和保真度至关重要处理。在这项工作中,我们通过使用化学交联和串联质谱法鉴定了9种分子间交联的肽,研究了大肠杆菌和水生栖热菌Ffh.FtsY复合物。该信息与先前未描述的模型构建方法结合使用,该方法将几何约束优化与高分子对接相结合。 Ffh.FtsY配合物的最终模型与此后不久解析的晶体结构非常吻合。有趣的是,四个交联对涉及Ffh的M结构域,该结构域不存在于晶体结构中,提供了以前未记录的实验证据,即M结构域位于复合物中的Ffh.FtsY界面附近。

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