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首页> 外文期刊>Medicinal chemistry research: an international journal for rapid communications on design and mechanisms of action of biologically active agents >Discovery of a potent broad spectrum antimicrobial agent through pharmacophore modeling, virtual screening, in vitro antimicrobial evaluation and gastrointestinal permeation studies
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Discovery of a potent broad spectrum antimicrobial agent through pharmacophore modeling, virtual screening, in vitro antimicrobial evaluation and gastrointestinal permeation studies

机译:通过药效基团建模,虚拟筛选,体外抗菌评估和胃肠道渗透研究发现有效的广谱抗菌剂

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In view of the role of DHFR in design and development of antimicrobials, we have attempted to develop a rigorously validated structure-based pharmacophore model comprising of two hydrogen bond donors, one hydrogen bond acceptor and two hydrophobic features. The model was used as a query to screen the National Cancer Institute and Maybridge database leading to retrieval of many hits which were screened on the basis of estimated activity, fit value and Lipinski's violation. Three most potent hits with zero lipinski's violation were subjected to docking studies which resulted into visualization of potential interaction capabilities of compounds in line to pharmacophoric features. All the three hits were subjected to in vitro antimicrobial evaluation, and the order of activity against various microbial strains was found to be HTS00987 > NSC47793 > NSC5475. Since HTS00987 appeared to be most active, it was subjected to permeability studies using in vitro everted intestinal sac permeation method. The results revealed that HTS00987 has good permeability proving its potential as druggable antimicrobial agent.
机译:考虑到DHFR在抗菌剂的设计和开发中的作用,我们试图开发一种经过严格验证的基于结构的药效团模型,该模型包含两个氢键供体,一个氢键受体和两个疏水性特征。该模型用作查询以筛选国家癌症研究所和Maybridge数据库,从而检索许多命中,这些命中是根据估计的活性,拟合值和Lipinski违规进行筛选的。进行了对接研究,对三个最有效的零lipinski违例值进行了对接研究,结果显示了与药效学特征一致的化合物的潜在相互作用能力。所有三个命中均进行了体外抗菌评估,发现针对各种微生物菌株的活性顺序为:HTS00987> NSC47793> NSC5475。由于HTS00987似乎是最活跃的,因此使用体外翻肠肠囊渗透法对其进行了渗透性研究。结果表明,HTS00987具有良好的渗透性,证明了其作为可药用抗菌剂的潜力。

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