化学学报 ›› 2009, Vol. 67 ›› Issue (8): 735-745. 上一篇    下一篇

研究论文

基于QSAR/QSSR的苯并三唑化合物选择性抑制PTP-1B的研究

梁娜娜 李艳妮 葛志强*

  

  1. (天津大学化工学院制药工程系 系统生物工程教育部重点实验室 天津 300072)

  • 投稿日期:2008-09-16 修回日期:2008-11-10 发布日期:2009-04-28
  • 通讯作者: 葛志强

Analyses Based on 3D-QSAR/QSSR of PTP-1B Selective Inhibitor—Benzotriazole Derivatives

Liang, Nana Li, Yanni Ge, Zhiqiang*   

  1. (Education Ministry Key Laboratory of Systems Bioengineering, School of Chemical Engineering,
    Tianjin University, Tianjin 300072)
  • Received:2008-09-16 Revised:2008-11-10 Published:2009-04-28
  • Contact: Ge, Zhiqiang

蛋白酪氨酸磷酸酶1B (PTP-1B)特异性抑制剂是近年来治疗II型糖尿病药物研发的热点. PTP-1B与T细胞蛋白酪氨酸磷酸酶(TCPTP)同源性很高, 为了避免在使用PTP-1B抑制剂过程中对TCPTP产生交叉抑制, 则需要设计开发对PTP-1B具有高活性和高特异选择性的小分子化合物. 苯并三唑类化合物对PTP-1B的抑制活性很高, 并且其中一些化合物对PTP-1B表现出了较好的特异选择性, 具有良好的药用开发前景. 通过CoMFA和CoMSIA两种方法分别对该类化合物进行了三维定量结构-活性关系(3D-QSAR)和三维定量结构-选择性关系(3D-QSSR)研究, 并建立了相关的预测模型. 计算结果表明PTP-1B中的Arg24与化合物的氢键相互作用是提高选择性的重要因素, 并且在R2位引入氢键供体且体积较大的强供电子基团, 将有利于化合物抑制活性的提高, 而在R2位取代基的末端引入氢键受体且体积较大的强吸电子基团, 将有利于化合物选择性的提高.

关键词: 苯并三唑, 蛋白酪氨酸磷酸酶1B, T细胞蛋白酪氨酸磷酸酶, 三维定量构效关系

Protein tyrosine phosphatase 1B (PTP-1B) has recently received much attention as a potential drug target in type 2 diabetes. T-cell protein tyrosine phosphatase (TCPTP) has an 80% homology to PTP-1B in the catalytic domains, and non-selective inhibition gives rise to severe side effects. Benzotriazole derivatives were found to be potent PTP-1B inhibitors, which provide a moderate degree of selectivity to PTP-1B over TCPTP. The 3D-QSAR and 3D-QSSR studies were conducted by comparative molecular field analysis (CoMFA) and comparative molecular similarity index analysis (CoMSIA), to obtain the best CoMFA and CoMSIA models. The result indicates that the hydrogen bond formed by Arg24 in PTP-1B and benzotriazole molecules is of great importance for the selectivity of the compounds. An enormous, negatively charged and hydrogen-bond donor group at R2 of benzotriazole skeleton would be beneficial for increasing the activity of the compounds, and an enormous, positively charged and hydrogen-bond acceptor group at the end of the R2 position would increase the selectivity of benzotriazole derivatives.

Key words: benzotriazole, protein tyrosine phosphatase 1B, T-cell protein tyrosine phosphatase, 3D- QSAR/QSSR

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