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Targeting Bacterial Dsb Proteins for the Development of Anti-Virulence Agents

机译:靶向细菌Dsb蛋白以开发抗毒力剂

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Recent years have witnessed a dramatic increase in bacterial antimicrobial resistance and a decline in the development of novel antibiotics. New therapeutic strategies are urgently needed to combat the growing threat posed by multidrug resistant bacterial infections. The Dsb disulfide bond forming pathways are potential targets for the development of antimicrobial agents because they play a central role in bacterial pathogenesis. In particular, the DsbA/DsbB system catalyses disulfide bond formation in a wide array of virulence factors, which are essential for many pathogens to establish infections and cause disease. These redox enzymes are well placed as antimicrobial targets because they are taxonomically widespread, share low sequence identity with human proteins, and many years of basic research have provided a deep molecular understanding of these systems in bacteria. In this review, we discuss disulfide bond catalytic pathways in bacteria and their significance in pathogenesis. We also review the use of different approaches to develop inhibitors against Dsb proteins as potential anti-virulence agents, including fragment-based drug discovery, high-throughput screening and other structure-based drug discovery methods.
机译:近年来,细菌的抗菌素耐药性急剧增加,新型抗生素的发展下降。迫切需要新的治疗策略来对抗由多药耐药性细菌感染引起的日益严重的威胁。 Dsb二硫键形成途径是抗菌剂开发的潜在目标,因为它们在细菌发病机理中起着核心作用。尤其是,DsbA / DsbB系统在多种毒力因子中催化二硫键的形成,这对于许多病原体建立感染并引起疾病至关重要。这些氧化还原酶在分类学上很普遍,与人类蛋白质具有低序列同一性,因此被定位为抗菌目标,并且多年的基础研究已经为细菌中的这些系统提供了深刻的分子理解。在这篇综述中,我们讨论了细菌中的二硫键催化途径及其在发病中的意义。我们还回顾了使用不同方法开发针对Dsb蛋白的抑制剂作为潜在抗毒剂的方法,包括基于片段的药物发现,高通量筛选和其他基于结构的药物发现方法。

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