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Mesodynamics in the SARS nucleocapsid measured by NMR field cycling

机译:核磁共振场循环测量SARS核衣壳的介观动力学

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摘要

Protein motions on all timescales faster than molecular tumbling are encoded in the spectral density. The dissection of complex protein dynamics is typically performed using relaxation rates determined at high and ultra-high field. Here we expand this range of the spectral density to low fields through field cycling using the nucleocapsid protein of the SARS coronavirus as a model system. The field-cycling approach enables site-specific measurements of R (1) at low fields with the sensitivity and resolution of a high-field magnet. These data, together with high-field relaxation and heteronuclear NOE, provide evidence for correlated rigid-body motions of the entire beta-hairpin, and corresponding motions of adjacent loops with a time constant of 0.8 ns (mesodynamics). MD simulations substantiate these findings and provide direct verification of the time scale and collective nature of these motions.
机译:在所有时间尺度上,蛋白质运动都比分子翻转更快,以光谱密度编码。复杂蛋白质动力学的解剖通常使用在高场和超高场下确定的弛豫率进行。在这里,我们使用SARS冠状病毒的核衣壳蛋白作为模型系统,通过田间循环将光谱密度的范围扩展到低场。磁场循环方法可以在低磁场下以高磁场磁铁的灵敏度和分辨率对R(1)进行特定位置的测量。这些数据,加上高场弛豫和异核NOE,为整个β-发夹的刚体运动以及相邻环的相应运动(时间常数为0.8 ns)提供了证据(介动力学)。 MD模拟证实了这些发现,并提供了对这些运动的时标和集体性质的直接验证。

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