可药性
鉴定(生物学)
药品
小分子
药物发现
风险分析(工程)
计算机科学
计算生物学
药物开发
医学
纳米技术
药理学
生物信息学
生物
植物
基因
生物化学
遗传学
材料科学
作者
Tristan S. Maurer,Martin P. Edwards,David Hepworth,Patrick R. Verhoest,Charlotte Allerton
标识
DOI:10.1016/j.drudis.2021.09.017
摘要
Successful small-molecule drug design requires a molecular target with inherent therapeutic potential and a molecule with the right properties to unlock its potential. Present-day drug design strategies have evolved to leave little room for improvement in drug-like properties. As a result, inadequate safety or efficacy associated with molecular targets now constitutes the primary cause of attrition in preclinical development through Phase II. This finding has led to a deeper focus on target selection. In this current reality, design tactics that enable rapid identification of risk-balanced clinical candidates, translation of clinical experience into meaningful differentiation strategies, and expansion of the druggable proteome represent significant levers by which drug designers can accelerate the discovery of the next generation of medicines.
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