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首页> 外文期刊>Current drug targets-The International journal for timely in-depth reviews on drug targets >Molecular mechanisms of host-pathogen interactions and their potential for the discovery of new drug targets.
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Molecular mechanisms of host-pathogen interactions and their potential for the discovery of new drug targets.

机译:宿主病原体相互作用的分子机制及其发现新药物靶标的潜力。

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Vaccines and chemotherapy have undeniably been the discoveries in the field of biomedical research that have exerted the biggest impact on the improvement of public health. Nevertheless, the development of bacterial resistance to antibiotics has co-evolved over time with the discovery of new drugs. This entails the necessity for continuous research on new anti-infectious agents.The current review highlights recent discoveries in the molecular mechanisms of specific host pathogen interactions and their potential for drug discovery. The focus is on facultative and obligate intracellular pathogens (Mycobacterium, Chlamydia and Legionella) and their manipulation of host cells in regard to inhibition of phagosome maturation and cell death. Furthermore, the composition and role of the SecA2 and the ESX-1 secretion pathways in bacterial virulence and manipulation of infected host cells is discussed. The central hypothesis proposed in this review is that the characterization of bacterial proteins and lipids involved in host cell manipulation (modulins) will provide an abundance of new drug targets. One advantage of targeting such bacterial modulins for drug development is that these anti-modulin drugs will not disrupt the beneficial host microflora and therefore have fewer side effects.
机译:疫苗和化学疗法无可否认是生物医学研究领域的发现,这施加了对改善公共卫生的影响。然而,随着新药的发现,对抗生素的细菌性抗性的发展已经共同进化。这需要持续研究新的抗传染性药物的必要性。目前的审查突出了特定宿主病原体相互作用的分子机制及其药物发现潜力的发现。重点是兼表性的,迫使细胞内病原体(分枝杆菌,衣原体和军团菌)及其在吞咽植物成熟和细胞死亡的抑制方面操纵宿主细胞。此外,讨论了SECA2和ESX-1分泌途径的组成和作用在细菌毒力和感染宿主细胞的操纵中。在本综述中提出的中央假设是,参与宿主细胞操纵(调节蛋白)的细菌蛋白和脂质的表征将提供丰富的新药物靶标。针对这种药物发育的这种细菌调制蛋白的一个优点是这些抗模型药物不会破坏有益宿主微生物或因此具有更少的副作用。

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