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利用当前对抗生素作用的认识来发现新药。

Exploiting current understanding of antibiotic action for discovery of new drugs.

作者信息

Chopra I, Hesse L, O'Neill A J

机构信息

Antimicrobial Research Centre and Division of Microbiology, School of Biochemistry and Molecular Biology, University of Leeds, Leeds, UK.

出版信息

Symp Ser Soc Appl Microbiol. 2002(31):4S-15S.

Abstract

The introduction of antibiotics for the chemotherapy of bacterial infections has been one of the most important medical achievements of the past 50 years. However, the emergence of bacterial resistance to antibiotics undermines the therapeutic utility of existing agents, creating a requirement for the discovery of new antibacterial drugs. Several drug discovery strategies have emerged, including incremental improvements to existing antibiotics by chemical manipulation and the search for novel drug targets based on genomic approaches. An alternative strategy seeks to exploit opportunities for drug discovery arising from an understanding of the mode of action of existing antibiotics. Thus biochemical pathways or processes inhibited by antibiotics already in clinical use may nevertheless contain key functions that represent unexploited targets for further drug discovery. A major benefit of employing pathways or processes that are already known to contain drug targets is that proof of principle for drug intervention is already established. This approach to drug discovery is illustrated by reviewing target sites for existing antibiotics and considering how this information might be applied for the discovery of new agents inhibiting peptidoglycan synthesis, tRNA synthesis, transcription and DNA replication.

摘要

抗生素用于细菌感染的化疗是过去50年最重要的医学成就之一。然而,细菌对抗生素产生耐药性削弱了现有药物的治疗效用,这就需要发现新的抗菌药物。已经出现了几种药物发现策略,包括通过化学操作对现有抗生素进行逐步改进,以及基于基因组方法寻找新的药物靶点。另一种策略试图利用因了解现有抗生素的作用方式而产生的药物发现机会。因此,临床使用的抗生素所抑制的生化途径或过程可能仍包含关键功能,这些功能代表了尚未开发的进一步药物发现靶点。采用已知含有药物靶点的途径或过程的一个主要好处是,药物干预的原理证明已经确立。通过回顾现有抗生素的靶点部位,并考虑如何将这些信息应用于发现抑制肽聚糖合成、tRNA合成、转录和DNA复制的新药物,来说明这种药物发现方法。

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