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Bacterial lipid membranes as promising targets to fight antimicrobial resistance, molecular foundations and illustration through the renewal of aminoglycoside antibiotics and emergence of amphiphilic aminoglycosides

机译:通过更新氨基糖苷类抗生素和出现两亲性氨基糖苷类,细菌脂质膜有望成为抗药性,分子基础和例证的有力靶标

摘要

Hereunder, we highlight bacterial membrane anionic lipids as attractive targets in the design of antibacterial drugs which can be effective against both Gram-positive and Gram-negative resistant bacteria. In this approach, first, molecular foundations and structure–activity relationships are laid out for membrane-targeting drugs and drug candidates from the structure and physicochemical properties of the main membrane targets, describing, as well, the corresponding identified resistances. Second, this approach is illustrated by the history of the emergence of antibacterial and antifungal amphiphilic aminoglycosides (AAGs) which are active against Gram-positive and Gram-negative resistant bacteria. AAGs have resulted from intensive medicinal chemistry development of a group of old antibiotic drugs known as aminoglycosides (AGs), which target ribosomal RNA. The aforementioned AAG's are being used towards discovering new antibiotics which are less toxic and less susceptible to resistance. The recent results in the field of AAGs are described and discussed in terms of structure–activity relationships and mechanism of action.
机译:在下文中,我们突出了细菌膜阴离子脂质作为抗菌药物设计中的诱人靶标,该抗菌药物可以有效抵抗革兰氏阳性和革兰氏阴性细菌。在这种方法中,首先,通过主要膜靶的结构和理化特性,为膜靶向药物和候选药物奠定了分子基础和结构-活性关系,并描述了相应的已确定的耐药性。其次,这种方法通过对革兰氏阳性和革兰氏阴性细菌具有活性的抗菌和抗真菌两亲性氨基糖苷(AAG)的出现来说明。 AAG是由一组针对核糖体RNA的称为氨基糖苷(AGs)的旧抗生素药物的密集化学化学开发产生的。前面提到的AAG被用于发现毒性较小,抗药性较弱的新抗生素。从结构-活动关系和作用机制方面描述和讨论了AAGs领域的最新成果。

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