计算配体-受体结合动力学的新方法。

New approaches for computing ligand-receptor binding kinetics.

机构信息

Molecular and Cellular Modeling Group, Heidelberg Institute for Theoretical Studies, Schloss-Wolfsbrunnenweg 35, 69118 Heidelberg, Germany.

Molecular and Cellular Modeling Group, Heidelberg Institute for Theoretical Studies, Schloss-Wolfsbrunnenweg 35, 69118 Heidelberg, Germany; Interdisciplinary Center for Scientific Computing (IWR), Heidelberg University, Im Neuenheimer Feld 205, 69120 Heidelberg, Germany.

出版信息

Curr Opin Struct Biol. 2018 Apr;49:1-10. doi: 10.1016/j.sbi.2017.10.001. Epub 2017 Nov 11.

DOI:10.1016/j.sbi.2017.10.001

PMID:29132080

Abstract

The recent and growing evidence that the efficacy of a drug can be correlated to target binding kinetics has seeded the development of a multitude of novel methods aimed at computing rate constants for receptor-ligand binding processes, as well as gaining an understanding of the binding and unbinding pathways and the determinants of structure-kinetic relationships. These new approaches include various types of enhanced sampling molecular dynamics simulations and the combination of energy-based models with chemometric analysis. We assess these approaches in the light of the varying levels of complexity of protein-ligand binding processes.

摘要

最近越来越多的证据表明，药物的疗效可以与靶标结合动力学相关联，这为开发多种旨在计算受体配体结合过程的速率常数的新方法奠定了基础，也有助于了解结合和解离途径以及结构动力学关系的决定因素。这些新方法包括各种类型的增强采样分子动力学模拟以及基于能量的模型与化学计量学分析的结合。我们根据蛋白质-配体结合过程的复杂程度的不同来评估这些方法。

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计算配体-受体结合动力学的新方法。

New approaches for computing ligand-receptor binding kinetics.

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