片段(逻辑)
生物信息学
化学
药物发现
配体效率
计算生物学
药品
组合化学
对接(动物)
立体化学
配体(生物化学)
药理学
生物化学
计算机科学
生物
受体
医学
算法
基因
护理部
作者
Osamu Takahashi,Yoshiaki Masuda,Ayumu Muroya,Toshio Furuya
出处
期刊:Journal of the Pharmaceutical Society of Japan
日期:2010-03-01
卷期号:130 (3): 349-354
被引量:1
标识
DOI:10.1248/yakushi.130.349
摘要
An important step to promote fragment-based drug design (FBDD) is to find high-quality fragment molecules. Therefore the design of the fragment library is the most crucial stage. In our fragment library, the main considerations are ligand efficiency (LE), diversity, and solubility with drug-like properties. We especially considered LE to raise hit probability in screening. We estimated LE of the fragment molecule based on known LE values of the active compounds. We also developed a docking program suitable for screening fragments rather than drug compounds. Furthermore, we explored fragment-linking program, which links together fragments that bind to adjacent sites on a target protein so as to promote FBDD in silico.
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