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首页> 外文期刊>Infectious Disorders - Drug Targets >Combating Vancomycin Resistance in Bacteria: Targeting the D-ala-D-ala Dipeptidase VanX
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Combating Vancomycin Resistance in Bacteria: Targeting the D-ala-D-ala Dipeptidase VanX

机译:对抗细菌中的万古霉素耐药性:靶向D-ala-D-ala二肽酶VanX

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摘要

In the past 20 years, vancomycin and other glycopeptide antibiotics have been administered to patients with Streptococcal and Staphylococcal infections that were resistant to all other antibiotics or to patients who were allergic to penicillins and cephalosporins. After extensive use of vancomycin and other glycopeptide antibiotics in humans, several strains of Enterococcus have developed high-level vancomycin resistance (collectively called VRE, vancomycin-resistant Enterococcus), and this resistance phenotype has spread to other organisms. The spread of vancomycin resistance to other pathogens and, potentially, to bacterial strains on the CDC's bioterrorism watch list is a major biomedical concern. Bacteria most often become resistant to vancomycin by acquiring a transposon containing genes that encode for a number of proteins, five of which are essential for the high-level resistance phenotype. The five essential gene products are called VanR, VanS, VanH, VanA, and VanX. Previous studies have shown that the inactivation of VanX results in an organism that is sensitive to vancomycin and that VanX is an excellent inhibitor target. In this review the known inhibitors and structural and mechanistic properties of VanX will be discussed. These data will be used to offer suggestions for novel, rationally-designed or -redesigned inhibitors, which could potentially be used in combination with existing glycopeptide antibiotics as a treatment for vancomycin-resistant bacterial infections.
机译:在过去的20年中,万古霉素和其他糖肽类抗生素已被施用于对所有其他抗生素具有抗药性的链球菌和葡萄球菌感染的患者,或对青霉素和头孢菌素过敏的患者。在人类中广泛使用万古霉素和其他糖肽抗生素后,数种肠球菌菌株已发展出高水平的万古霉素耐药性(统称为VRE,耐万古霉素肠球菌),并且这种耐药性表型已经传播到其他生物。万古霉素对其他病原体的耐药性以及对CDC生物恐怖主义监视名单上的细菌菌株的耐药性传播是一个主要的生物医学问题。细菌通常会通过获得含有编码多种蛋白质的基因的转座子而变得对万古霉素具有抗性,其中五种对于高水平抗性表型至关重要。这五个必需的基因产物称为VanR,VanS,VanH,VanA和VanX。先前的研究表明,VanX的失活会导致对万古霉素敏感的生物,而VanX是出色的抑制剂靶标。在这篇综述中,将讨论VanX的已知抑制剂以及结构和机械性能。这些数据将用于为新型,合理设计或重新设计的抑制剂提供建议,这些抑制剂可潜在地与现有糖肽抗生素联合使用,以治疗耐万古霉素的细菌感染。

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