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Nanoscale protein dynamics: A new frontier for neutron spin echo spectroscopy*

机译:纳米级蛋白质动力学:中子自旋回波谱学的新领域*

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Recent studies show that neutron spin echo spectroscopy (NSE) can reveal long-range protein domain motions on nanometer lengthscales and on nanosecond to microsecond timescales. This unique capability of NSE provides new opportunities to understand protein dynamics and functions, such as how binding signals are propagated in a protein to distal sites. Here we review our applications of NSE to the study of nanoscale protein domain motions in a set of cell signaling proteins. We summarize the theoretical framework we have developed, which allows one to interpret the NSE data (Biophys. J. 99, 3473 (2010) and Proc. Natl. Acad. Sci. USA 102, 17646 (2005)). Our theoretical framework uses simple concepts from nonequilibrium statistical mechanics, and does not require elaborate molecular dynamics simulations, complex fits to rotational motion, or elastic network models. It is thus more robust than multiparameter techniques that require untestable assumptions. We also demonstrate our experimental scheme involving deuterium labeling of a protein domain or a subunit in a protein complex. We show that our selective deuteration scheme can highlight and resolve specific domain dynamics from the abundant global translational and rotational motions in a protein. Our approach thus clears significant hurdles to the application of NSE for the study of protein dynamics in solution.
机译:最近的研究表明,中子自旋回波谱仪(NSE)可以揭示纳米级和纳米级至微秒级时间范围内的远距离蛋白质域运动。 NSE的这种独特功能为理解蛋白质动力学和功能提供了新的机会,例如结合信号如何在蛋白质中传播到远端部位。在这里,我们回顾了NSE在研究一组细胞信号蛋白中纳米级蛋白质结构域运动中的应用。我们总结了已开发的理论框架,该理论框架使人们可以解释NSE数据(Biophys。J. 99,3473(2010)和Proc。Natl。Acad。Sci。USA 102,17646(2005))。我们的理论框架使用非平衡统计力学中的简单概念,不需要复杂的分子动力学模拟,对旋转运动的复杂拟合或弹性网络模型。因此,它比要求不可检验的假设的多参数技术更强大。我们还演示了我们的实验方案,其中涉及氘标记蛋白质复合物中的蛋白质结构域或亚基。我们表明,我们的选择性氘代方案可以从蛋白质中丰富的全局平移和旋转运动中突出显示并解析特定的域动态。因此,我们的方法为NSE在溶液中蛋白质动力学研究中的应用扫清了重大障碍。

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