Abuhamdah Sawsan, Habash Maha, Taha Mutasem O
Department of Biopharmaceutics and Clinical Pharmacy, Faculty of Pharmacy, The University of Jordan, Amman, Jordan.
J Comput Aided Mol Des. 2013 Dec;27(12):1075-92. doi: 10.1007/s10822-013-9699-6. Epub 2013 Dec 12.
Inhibition of the enzyme acetylcholinesterase (AChE) has been shown to alleviate neurodegenerative diseases prompting several attempts to discover and optimize new AChE inhibitors. In this direction, we explored the pharmacophoric space of 85 AChE inhibitors to identify high quality pharmacophores. Subsequently, we implemented genetic algorithm-based quantitative structure-activity relationship (QSAR) modeling to select optimal combination of pharmacophoric models and 2D physicochemical descriptors capable of explaining bioactivity variation among training compounds (r2(68)=0.94, F-statistic=125.8, r2 LOO=0.92, r2 PRESS against 17 external test inhibitors = 0.84). Two orthogonal pharmacophores emerged in the QSAR equation suggesting the existence of at least two binding modes accessible to ligands within AChE binding pocket. The successful pharmacophores were comparable with crystallographically resolved AChE binding pocket. We employed the pharmacophoric models and associated QSAR equation to screen the national cancer institute list of compounds. Twenty-four low micromolar AChE inhibitors were identified. The most potent gave IC50 value of 1.0 μM.
抑制乙酰胆碱酯酶(AChE)已被证明可缓解神经退行性疾病,这促使人们多次尝试发现并优化新型AChE抑制剂。在此方向上,我们探索了85种AChE抑制剂的药效团空间,以识别高质量的药效团。随后,我们实施了基于遗传算法的定量构效关系(QSAR)建模,以选择能够解释训练化合物之间生物活性差异的药效团模型和二维物理化学描述符的最佳组合(r2(68)=0.94,F统计量=125.8,留一法交叉验证r2=0.92,对17种外部测试抑制剂的预测残差平方和r2=0.84)。QSAR方程中出现了两个正交药效团,表明AChE结合口袋内的配体至少可采用两种结合模式。成功的药效团与晶体学解析的AChE结合口袋相当。我们利用药效团模型和相关的QSAR方程筛选了美国国立癌症研究所的化合物列表。鉴定出了24种低微摩尔浓度的AChE抑制剂。其中最有效的抑制剂的IC50值为1.0 μM。
