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Passage through a sub-diffusing geometrical bottleneck

机译:通过次散射几何瓶颈

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The usual Kramers theory of reaction rates in condensed media predict the rate to have an inverse dependence on the viscosity of the medium, eta. However, experiments on ligand binding to proteins, performed long ago, showed the rate to have eta(-nu) dependence, with nu in the range of 0.4-0.8. Zwanzig [J. Chem. Phys. 97, 3587 (1992)] suggested a model in which the ligand has to pass through a fluctuating opening to reach the binding site. This fluctuating gate model predicted the rate to be proportional to eta(-1/2). More recently, experiments performed by Xie et al. [Phys. Rev. Lett. 93, 180603 (2004)] showed that the distance between two groups in a protein undergoes not normal diffusion, but subdiffusion. Hence, in this paper, we suggest and solve a generalization of the Zwanzig model, viz., passage through an opening, whose size undergoes subdiffusion. Our solution shows that the rate is proportional to eta(-nu) with. in the range of 0.5-1, and hence, the subdiffusion model can explain the experimental observations. Published under license by AIP Publishing.
机译:通常的克拉姆斯在缩合培养基中的反应速率理论预测了对介质ETA粘度的逆依赖性的速率。然而,长期进行的对与蛋白质结合的配体结合的实验表明,在0.4-0.8的范围内,Nu的依赖性的速率达到速率。 zwanzig [J.化学。物理。 97,3587(1992)]建议其中配体必须通过波动开口以进入结合位点的模型。这种波动门模型预测了与ETA(-1/2)成比例的速率。最近,谢等人进行的实验。 [物理。 rev. lett。 93,180603(2004)]显示蛋白质中两组之间的距离不正常扩散,但是脱灯。因此,在本文中,我们建议并解决了Zwanzig模型的概括,Zwanzig模型,viz,通过开口通道,其尺寸经历的低拐灯。我们的解决方案表明,该速率与ETA(-NU)成比例。在0.5-1的范围内,因此,子边域模型可以解释实验观察。通过AIP发布在许可证下发布。

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