Xue Ping, Lu Huan-Huan, Zhu Yuan-Yuan, Ju Xiu-Lian, Pannecouque Christophe, Zheng Xiao-Jiao, Liu Gen-Yan, Zhang Xiu-Lan, Gu Shuang-Xi
Key Laboratory for Green Chemical Process of Ministry of Education, School of Chemical Engineering & Pharmacy, Wuhan Institute of Technology, Wuhan 430205, China.
School of Chemistry and Environmental Engineering, Wuhan Institute of Technology, Wuhan 430205, China.
Bioorg Med Chem Lett. 2017 Apr 15;27(8):1640-1643. doi: 10.1016/j.bmcl.2017.03.009. Epub 2017 Mar 7.
Based on the strategy of molecular hybridization, diketo acid fragment as a classical phamacophore of integrase inhibitors was introduced to reverse transcriptase inhibitors diarylpyrimidines to design a series of diarylpyrimidine-diketo acid hybrids (DAPY-DKAs). The target molecules 10b and 11b showed inhibitory activities against WT HIV-1 with EC values of 0.18μM and 0.14μM, respectively. And the results of molecular docking demonstrated the potential binding mode and revealed that the DKA moiety and its ester could both be tolerated in the nonnucleoside binding site (NNBS) of HIV-1 RT.
基于分子杂交策略,将二酮酸片段作为整合酶抑制剂的经典药效团引入逆转录酶抑制剂二芳基嘧啶中,设计了一系列二芳基嘧啶-二酮酸杂合物(DAPY-DKAs)。目标分子10b和11b对野生型HIV-1显示出抑制活性,其EC值分别为0.18μM和0.14μM。分子对接结果表明了潜在的结合模式,并揭示二酮酸部分及其酯在HIV-1逆转录酶的非核苷结合位点(NNBS)中均能被耐受。
