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Domain-elongation NMR spectroscopy yields new insights into RNA dynamics and adaptive recognition.

机译:域延伸NMR光谱学为RNA动力学和自适应识别提供了新的见解。

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摘要

By simplifying the interpretation of nuclear magnetic resonance spin relaxation and residual dipolar couplings data, recent developments involving the elongation of RNA helices are providing new atomic insights into the dynamical properties that allow RNA structures to change functionally and adaptively. Domain elongation, in concert with spin relaxation measurements, has allowed the detailed characterization of a hierarchical network of local and collective motional modes occurring at nanosecond timescale that mirror the structural rearrangements that take place following adaptive recognition. The combination of domain elongation with residual dipolar coupling measurements has allowed the experimental three-dimensional visualization of very large amplitude rigid-body helix motions in HIV-1 transactivation response element (TAR) that trace out a highly choreographed trajectory in which the helices twist and bend in a correlated manner. The dynamic trajectory allows unbound TAR to sample many of its ligand bound conformations, indicating that adaptive recognition occurs by conformational selection intrinsic flexibility plays essential roles directing RNA conformational changes along specific pathways.
机译:通过简化对核磁共振自旋弛豫和残余偶极耦合数据的解释,涉及RNA螺旋伸长的最新进展为允许RNA结构功能性和适应性改变的动力学性质提供了新的原子学见解。域伸长与自旋弛豫测量相结合,已允许对纳秒级时域发生的局部和集体运动模式的分层网络进行详细表征,该网络反映了自适应识别后发生的结构重排。域伸长与残余偶极耦合测量值的结合,使得在HIV-1反式激活反应元件(TAR)中非常大幅度的刚体螺旋运动的实验性三维可视化成为可能,该运动描绘出了编排高度较高的轨迹,其中螺旋扭曲并以相关的方式弯曲。动态轨迹允许未结合的TAR对其许多配体结合的构象进行采样,这表明通过构象选择进行的自适应识别内在灵活性在指导RNA构象沿着特定途径的变化中起着至关重要的作用。

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