Drug Repurposing: A Paradigm Shift in Drug Discovery

S. Jayaram, Emdormi Rymbai, D. Sugumar, Divakar Selvaraj
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引用次数: 1

Abstract

The traditional methods of drug discovery and drug development are a tedious, complex, and costly process. Target identification, target validation; lead identification; and lead optimization are a lengthy and unreliable process that further complicates the discovery of new drugs. A study of more than 15 years reports that the success rate in the discovery of new drugs in the fields of ophthalmology, cardiovascular, infectious disease, and oncology to be 32.6%, 25.5%, 25.2% and 3.4%, respectively. A tedious and costly process coupled with a very low success rate makes the traditional drug discovery a less attractive option. Therefore, an alternative to traditional drug discovery is drug repurposing, a process in which already existing drugs are repurposed for conditions other than which were originally intended. Typical examples of repurposed drugs are thalidomide, sildenafil, memantine, mirtazapine, mifepristone, etc. In recent times, several databases have been developed to hasten drug repurposing based on the side effect profile, the similarity of chemical structure, and target site. This work reviews the pivotal role of drug repurposing in drug discovery and the databases currently available for drug repurposing.
药物再利用:药物发现的范式转变
传统的药物发现和开发方法是一个繁琐、复杂和昂贵的过程。目标识别、目标验证;领导识别;而先导优化是一个漫长而不可靠的过程,这进一步使新药的发现变得复杂。一项超过15年的研究报告显示,眼科、心血管、传染病和肿瘤学领域的新药发现成功率分别为32.6%、25.5%、25.2%和3.4%。繁琐而昂贵的过程加上极低的成功率使得传统的药物发现不那么有吸引力。因此,替代传统药物发现的一种方法是药物再利用,这是一种将现有药物用于与最初预期不同的条件的过程。典型的重新利用药物有沙利度胺、西地那非、美金刚、米氮平、米非司酮等。近年来,基于副作用、化学结构和靶点的相似性,已经开发了几个数据库来加速药物的再利用。这项工作回顾了药物再利用在药物发现中的关键作用,以及目前可用于药物再利用的数据库。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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