Roy Subhajit, Narang Bawneet K, Gupta Manish K, Abbot Vikrant, Singh Virender, Rawal Ravindra K
Department of Pharmaceutical Chemistry, Indo-Soviet Friendship College of Pharmacy (ISFCP), Moga, India.
School of Pharmacy, Lloyd Institute of Management and Technology, Greater Noida, India.
Drug Res (Stuttg). 2018 Jul;68(7):395-402. doi: 10.1055/s-0043-125210. Epub 2018 Jan 17.
Flexible docking simulations were carried out on a series of isocytosine analogs as xanthine oxidase (XO) inhibitors. This was done by analysing the interaction of these compounds at the active site of XO. The binding free energies of the analogs were calculated using GoldScore. The binding modes of the best-fit conformation were studied, providing some handy important interactions. The results obtained henceforth provided an insight into the pharmacophoric structural requirements for XO inhibition for this class of molecules.
对一系列异胞嘧啶类似物作为黄嘌呤氧化酶(XO)抑制剂进行了柔性对接模拟。这是通过分析这些化合物在XO活性位点的相互作用来完成的。使用GoldScore计算类似物的结合自由能。研究了最佳拟合构象的结合模式,提供了一些方便的重要相互作用。此后获得的结果为这类分子抑制XO的药效团结构要求提供了深入了解。
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