Literature DB >> 29606793

Quionolone carboxylic acid derivatives as HIV-1 integrase inhibitors: Docking-based HQSAR and topomer CoMFA analyses.

Jianbo Tong1, Pei Zhan1, Xiang Simon Wang2, Yingji Wu1.   

Abstract

Quionolone carboxylic acid derivatives as inhibitors of HIV-1 integrase were investigated as a potential class of drugs for the treatment of acquired immunodeficiency syndrome (AIDS). Hologram quantitative structure-activity relationships (HQSAR) and translocation comparative molecular field vector analysis (topomer CoMFA) were applied to a series of 48 quionolone carboxylic acid derivatives. The most effective HQSAR model was obtained using atoms and bonds as fragment distinctions: cross-validation q2 = 0.796, standard error of prediction SDCV = 0.36, the non-cross-validated r2 = 0.967, non-cross validated standard error SD = 0.17, the correlation coefficient of external validation Qext2 = 0.955, and the best hologram length HL = 180. topomer CoMFA models were built based on different fragment cutting models, with the most effective model of q2 = 0.775, SDCV = 0.37, r2 = 0.967, SD = 0.15, Qext2 = 0.915, and F = 163.255. These results show that the models generated form HQSAR and topomer CoMFA were able to effectively predict the inhibitory potency of this class of compounds. The molecular docking method was also used to study the interactions of these drugs by docking the ligands into the HIV-1 integrase active site, which revealed the likely bioactive conformations. This study showed that there are extensive interactions between the quionolone carboxylic acid derivatives and THR80, VAL82, GLY27, ASP29, and ARG8 residues in the active site of HIV-1 integrase. These results provide useful insights for the design of potent new inhibitors of HIV-1 integrase.

Entities:  

Keywords:  3D-QSAR; HQSAR; molecular docking; quionolone carboxylic acid derivatives; topomer CoMFA

Year:  2017        PMID: 29606793      PMCID: PMC5875935          DOI: 10.1002/cem.2934

Source DB:  PubMed          Journal:  J Chemom        ISSN: 0886-9383            Impact factor:   2.467


  21 in total

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Authors:  Jaroslaw Polanski; Fatima Zouhiri; Laurence Jeanson; Didier Desmaële; Jean d'Angelo; Jean-François Mouscadet; Rafal Gieleciak; Johann Gasteiger; Marc Le Bret
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10.  A central role for TRPS1 in the control of cell cycle and cancer development.

Authors:  Lele Wu; Yuzhi Wang; Yan Liu; Shiyi Yu; Hao Xie; Xingjuan Shi; Sheng Qin; Fei Ma; Tuan Zea Tan; Jean Paul Thiery; Liming Chen
Journal:  Oncotarget       Date:  2014-09-15
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