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Exploring the potential of adjunct therapy in tuberculosis

机译:探索结核病辅助治疗的潜力

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A critical unmet need for treatment of drug-resistant tuberculosis (TB) is to find novel therapies that are efficacious, safe, and shorten the duration of treatment. Drug discovery approaches for TB primarily target essential genes of the pathogen Mycobacterium tuberculosis (Mtb) but novel strategies such as host-directed therapies and nonmicrobicidal targets are necessary to bring about a paradigm shift in treatment. Drugs targeting the host pathways and nonmicrobicidal proteins can be used only in conjunction with existing drugs as adjunct therapies. Significantly, host-directed adjunct therapies have the potential to decrease duration of treatment, as they are less prone to drug resistance, target the immune responses, and act via novel mechanism of action. Recent advances in targeting host-pathogen interactions have implicated pathways such as eicosanoid regulation and angiogenesis. Furthermore, several approved drugs such as metformin and verapamil have been identified that appear suitable for repurposing for the treatment of TB. These findings and the challenges in the area of host- and/or pathogen-directed adjunct therapies and their implications for TB therapy are discussed.
机译:耐药结核病(TB)的未满足的关键需求是找到有效,安全且能缩短治疗时间的新疗法。结核病的药物发现方法主要针对病原体结核分枝杆菌(Mtb)的必需基因,但诸如宿主定向疗法和非杀菌目标等新颖策略对于实现治疗范式的转变是必不可少的。靶向宿主途径的药物和非杀微生物蛋白只能与现有药物一起用作辅助疗法。重要的是,针对宿主的辅助疗法具有减少治疗时间的潜力,因为它们不易产生耐药性,靶向免疫反应并通过新的作用机制起作用。靶向宿主-病原体相互作用的最新进展涉及诸如类花生酸调节和血管生成的途径。此外,已经确定了几种批准的药物,如二甲双胍和维拉帕米,似乎适合用于治疗结核病。讨论了这些发现以及在宿主和/或病原体指导的辅助治疗领域中的挑战及其对结核病治疗的意义。

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