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Patents on glycopeptides of the vancomycin family and their derivatives as antimicrobials: January 1999 - June 2003

机译:万古霉素家族糖肽及其衍生物作为抗微生物剂的专利:1999年1月-2003年6月

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摘要

The review summarises patents claiming novel glycopeptides of vancomycin and teicoplanin families published from January 1999 to June 2003. A brief overview of the structures of the most important natural antibacterial glycopeptides, the mode of action and resistance mechanism is presented. Struc-ture-activity relationships for semisynthetic antibiotics are discussed and the structures and properties of novel clinically important compounds are presented. Semisynthetic derivatives containing various hydrophobic moieties were found to be active against glycopeptide-resistant bacteria. These compounds use a different or additional mechanism for antibacterial action to the parent antibiotics. These are not based on the interaction with Acyl-D-Ala-D-Ala or Acyl-D-Ala-D-lactate of the nascent bacterial peptidoglycan. Recently discovered antiviral activities of modified glycopeptides based on the interaction with viral receptors shows that glycopeptide derivatives are capable of interacting with membrane structures through mechanism(s) unrelated to -D-Ala-D-Ala or -D-Ala-D-lactate binding. Understanding the structural demands and the mechanics of this binding represents a challenge for researchers in this field.
机译:该综述总结了自1999年1月至2003年6月发表的声称具有万古霉素和替考拉宁家族新糖肽的专利。简要概述了最重要的天然抗菌糖肽的结构,作用方式和耐药机制。讨论了半合成抗生素的结构活性关系,并提出了具有临床意义的新型化合物的结构和性质。发现含有各种疏水部分的半合成衍生物对糖肽抗性细菌具有活性。这些化合物对母体抗生素使用不同或其他的抗菌作用机理。这些不是基于与新生细菌肽聚糖的酰基-D-丙氨酸-D-丙氨酸或酰基-D-丙氨酸-D-乳酸酯的相互作用。最近发现的基于与病毒受体相互作用的修饰糖肽的抗病毒活性表明,糖肽衍生物能够通过与-D-Ala-D-Ala或-D-Ala-D-乳酸酯结合无关的机制与膜结构相互作用。 。理解这种结合的结构要求和机理是该领域研究人员的挑战。

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