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首页> 外文期刊>The Journal of Chemical Physics >Internal friction in an intrinsically disordered protein-Comparing Rouse-like models with experiments
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Internal friction in an intrinsically disordered protein-Comparing Rouse-like models with experiments

机译:内在摩擦在本质无序的蛋白质 - 比较rouse样模型的实验

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Internal friction is frequently found in protein dynamics. Its molecular origin however is difficult to conceptualize. Even unfolded and intrinsically disordered polypeptide chains exhibit signs of internal friction despite their enormous solvent accessibility. Here, we compare four polymer theories of internal friction with experimental results on the intrinsically disordered protein ACTR (activator of thyroid hormone receptor). Using nanosecond fluorescence correlation spectroscopy combined with single-molecule Forster resonance energy transfer (smFRET), we determine the time scales of the diffusive chain dynamics of ACTR at different solvent viscosities and varying degrees of compaction. Despite pronounced differences between the theories, we find that all models can capture the experimental viscosity-dependence of the chain relaxation time. In contrast, the observed slow-down upon chain collapse of ACTR is not captured by any of the theories and a mechanistic link between chain dimension and internal friction is still missing, implying that the current theories are incomplete. In addition, a discrepancy between early results on homopolymer solutions and recent single-molecule experiments on unfolded and disordered proteins suggests that internal friction is likely to be a composite phenomenon caused by a variety of processes. Published by AIP Publishing.
机译:在蛋白质动态中经常存在内部摩擦。然而,其分子来源难以概念化。甚至展开和本质上无序的多肽链均表现出内部摩擦的迹象,尽管其巨大的溶剂可用性。在这里,我们将内部摩擦的四个聚合物理论与实验结果进行了实验结果对本质无序的蛋白质ActR(甲状腺激素受体的活化剂)。使用纳秒荧光相关光谱与单分子福尔斯特共振能量转移(SMFRet)结合,我们确定了不同溶剂粘度和不同程度的压实的actr扩散链动态的时间尺度。尽管理论之间有明显的差异,但我们发现所有模型都可以捕获链弛豫时间的实验粘度依赖性。相比之下,观察到的缓慢下降在Actr的链崩溃时不会被任何理论和内部摩擦之间的机械链路捕获仍然缺失,这意味着当前的理论是不完整的。此外,在展开和无序蛋白质上的均聚物溶液和最近单分子实验的早期结果之间的差异表明,内部摩擦可能是由多种方法引起的复合现象。通过AIP发布发布。

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