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Phenylthiazole Antibacterial Agents Targeting Cell Wall Synthesis Exhibit Potent Activity in Vitro and in Vivo against Vancomycin-Resistant Enterococci

机译:靶向细胞壁合成的苯基噻唑抗菌剂在体外和体内对耐万古霉素肠球菌具有有效的活性

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摘要

The emergence of antibiotic-resistant bacterial species, such as vancomycin-resistant enterococci (VRE), necessitates the development of new antimicrobials: Here, we investigate the spectrum of antibacterial activity of three phenylthiazole-substituted aminoguanidines. These compounds possess potent activity against VRE, inhibiting growth of clinical isolates at concentrations as low as 0.5 mu g/mL. The compounds exerted a rapid bactericidal effect, targeting cell wall synthesis. Transposon mutagenesis suggested three possible targets: YubA, YubB (undecaprenyl diphosphate phosphatase (UPPP)), and YubD. Both UPPP as well as undecaprenyl diphosphate synthase were inhibited by compound 1. YubA and YubD are annotated as transporters and may also be targets because 1 collapsed the proton motive force in membrane vesicles. Using Caenorhabditis elegans, we demonstrate that two compounds (1, 3, at 20 mu g/mL) retain potent activity in vivo, significantly reducing the burden of VRE in infected worms. Taken altogether, the results indicate that compounds 1 and 3 warrant further investigation as novel antibacterial agents against drug-resistant enterococci.
机译:抗生素耐药细菌物种的出现,如耐万古霉素肠球菌(VRE),需要开发新的抗菌剂:在这里,我们研究了三种苯基噻唑取代的氨基胍的抗菌活性谱。这些化合物具有强大的抗VRE活性,抑制浓度低至0.5μ g/mL的临床分离株的生长。这些化合物发挥了快速的杀菌作用,靶向细胞壁合成。转座子诱变提出了三种可能的靶点:YubA、YubB(十一烯基二磷酸磷酸酶 (UPPP))和 YubD。UPPP和十一烯基二磷酸合酶均被化合物1抑制。YubA 和 YubD 被注释为转运蛋白,也可能是靶标,因为 1 折叠了膜囊泡中的质子动力。使用秀丽隐杆线虫,我们证明两种化合物(1,3,20μ g / mL)在体内保持有效的活性,显着降低了受感染蠕虫中VRE的负担。综上所述,结果表明化合物1和3作为抗耐药肠球菌的新型抗菌剂值得进一步研究。

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