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Discovery of antimicrobial compounds targeting bacterial type FAD synthetases

机译:发现靶向细菌FAD合成酶的抗菌化合物

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Abstract The increase of bacterial strains resistant to most of the available antibiotics shows a need to explore novel antibacterial targets to discover antimicrobial drugs. Bifunctional bacterial FAD synthetases (FADSs) synthesise the flavin mononucleotide (FMN) and flavin adenine dinucleotide (FAD). These cofactors act in vital processes as part of flavoproteins, making FADS an essential enzyme. Bacterial FADSs are potential antibacterial targets because of differences to mammalian enzymes, particularly at the FAD producing site. We have optimised an activity-based high throughput screening assay targeting Corynebacterium ammoniagenes FADS (CaFADS) that identifies inhibitors of its different activities. We selected the three best high-performing inhibitors of the FMN:adenylyltransferase activity (FMNAT) and studied their inhibition mechanisms and binding properties. The specificity of the CaFADS hits was evaluated by studying also their effect on the Streptococcus pneumoniae FADS activities, envisaging differences that can be used to discover species-specific antibacterial drugs. The antimicrobial effect of these compounds was also evaluated on C. ammoniagenes, S. pneumoniae, and Mycobacterium tuberculosis cultures, finding hits with favourable antimicrobial properties.
机译:摘要对大多数可用抗生素产生耐药性的细菌菌株的增加表明需要探索新型的抗菌靶标以发现抗菌药物。双功能细菌FAD合成酶(FADS)合成黄素单核苷酸(FMN)和黄素腺嘌呤二核苷酸(FAD)。这些辅因子在生命过程中起黄素蛋白的作用,使FADS成为必不可少的酶。由于与哺乳动物酶的差异,尤其是在FAD产生部位,细菌FADS是潜在的抗菌靶标。我们优化了针对氨氮棒状杆菌FADS(CaFADS)的基于活性的高通量筛选测定方法,该方法可识别其不同活性的抑制剂。我们选择了FMN的三种最佳高性能抑制剂:腺苷酸转移酶活性(FMNAT),并研究了它们的抑制机制和结合特性。通过还研究其对肺炎链球菌FADS活性的影响,评估了CaFADS命中的特异性,并设想了可用于发现物种特异性抗菌药物的差异。还评估了这些化合物对氨氮梭菌,肺炎链球菌和结核分枝杆菌培养物的抗菌作用,发现了具有良好抗菌特性的产品。

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