从笔记本电脑到台式机再到床边:基于结构的药物设计针对蛋白质靶标。
From laptop to benchtop to bedside: structure-based drug design on protein targets.
机构信息
University of Texas M. D. Anderson Cancer Center, Department of Experimental Therapeutics, Houston, TX 77054, USA.
出版信息
Curr Pharm Des. 2012;18(9):1217-39. doi: 10.2174/138161212799436386.
Abstract
As an important aspect of computer-aided drug design, structure-based drug design brought a new horizon to pharmaceutical development. This in silico method permeates all aspects of drug discovery today, including lead identification, lead optimization, ADMET prediction and drug repurposing. Structure-based drug design has resulted in fruitful successes drug discovery targeting proteinligand and protein-protein interactions. Meanwhile, challenges, noted by low accuracy and combinatoric issues, may also cause failures. In this review, state-of-the-art techniques for protein modeling (e.g. structure prediction, modeling protein flexibility, etc.), hit identification/ optimization (e.g. molecular docking, focused library design, fragment-based design, molecular dynamic, etc.), and polypharmacology design will be discussed. We will explore how structure-based techniques can facilitate the drug discovery process and interplay with other experimental approaches.
摘要
作为计算机辅助药物设计的一个重要方面,基于结构的药物设计为药物开发带来了新的视野。这种计算方法渗透到当今药物发现的各个方面,包括先导化合物的鉴定、先导化合物的优化、ADMET 预测和药物再利用。基于结构的药物设计在针对蛋白质配体和蛋白质-蛋白质相互作用的药物发现方面取得了丰硕的成功。同时,低准确性和组合问题等挑战也可能导致失败。在这篇综述中,将讨论蛋白质建模的最新技术(例如结构预测、建模蛋白质的柔性等)、命中鉴定/优化(例如分子对接、聚焦文库设计、基于片段的设计、分子动力学等)和多药理学设计。我们将探讨基于结构的技术如何促进药物发现过程,并与其他实验方法相互作用。
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