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A toolkit and benchmark study for FRET-restrained high-precision structural modeling

机译:FRET约束的高精度结构建模的工具包和基准研究

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摘要

We present a comprehensive toolkit for F?rster resonance energy transfer (FRET)-restrained modeling of biomolecules and their complexes for quantitative applications in structural biology. A dramatic improvement in the precision of FRET-derived structures is achieved by explicitly considering spatial distributions of dye positions, which greatly reduces uncertainties due to flexible dye linkers. The precision and confidence levels of the models are calculated by rigorous error estimation. The accuracy of this approach is demonstrated by docking a DNA primer-template to HIV-1 reverse transcriptase. The derived model agrees with the known X-ray structure with an r.m.s. deviation of 0.5 ?. Furthermore, we introduce FRET-guided 'screening' of a large structural ensemble created by molecular dynamics simulations. We used this hybrid approach to determine the formerly unknown configuration of the flexible single-strand template overhang.
机译:我们提出了一种用于共振共振能量转移(FRET)约束的生物分子及其复合物建模的综合工具包,用于结构生物学中的定量应用。通过明确考虑染料位置的空间分布,可以极大地提高FRET衍生结构的精确度,这大大降低了由于柔性染料接头而引起的不确定性。通过严格的误差估计来计算模型的精度和置信度。通过将DNA引物模板与HIV-1逆转录酶对接可以证明这种方法的准确性。导出的模型与已知的X射线结构相符,其r.m.s.偏差为0.5?。此外,我们介绍了由分子动力学模拟创建的大型结构整体的FRET引导“筛选”。我们使用这种混合方法来确定灵活的单链模板突出端以前未知的配置。

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