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Antimicrobial peptides and proteins in mycobacterial therapy: Current status and future prospects

机译:分枝杆菌治疗中的抗菌肽和蛋白质:现状和未来展望

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Tuberculosis (TB), an infectious disease caused by the pathogen Mycobacterium tuberculosis (Mtb), kills about 1.5 million people every year worldwide. An increase in the prevalence of drug-resistant strains of Mtb in the last few decades now necessitates the development of novel drugs that combat infections by both drug-sensitive and resistant Mtb. Moreover, as Mtb can persist in host cells by modulating their immune responses, it is essential that anti-TB agents be able to penetrate macrophages and kill the pathogen intracellularly without harming the host cells. In this context, antimicrobial peptides (AMPs) and proteins are being harnessed as anti-infective agents for the treatment of various diseases. Due to their direct and rapid bactericidal activity it is unlikely that pathogens acquire resistance against AMPs. Several short and potent AMP derivatives have been prepared by peptide engineering, and several of them are currently evaluated in clinical trials. The present review summarizes the role of endogenously expressed AMPs and proteins in the treatment of tuberculosis infections. In addition, mechanisms of direct anti-mycobacterial activity, manipulation of host immune responses, and future prospects of AMPs as therapeutic agents are discussed.
机译:结核病(TB)是一种由病原体结核分枝杆菌(Mtb)引起的传染病,全世界每年造成150万人死亡。在过去的几十年中,耐药结核菌的流行率上升,现在有必要开发出新药来对抗由药敏和耐药菌引起的感染。此外,由于Mtb可以通过调节其免疫反应而在宿主细胞中持续存在,因此至关重要的是,抗TB剂必须能够穿透巨噬细胞并在细胞内杀死病原体而不会损害宿主细胞。在这种情况下,抗微生物肽(AMPs)和蛋白质被用作抗感染剂,用于治疗各种疾病。由于其直接和快速的杀菌活性,病原体不太可能获得对AMP的抗性。通过肽工程已经制备了几种短而有效的AMP衍生物,其中一些目前正在临床试验中进行评估。本综述总结了内源性表达的AMPs和蛋白在结核感染治疗中的作用。此外,还讨论了直接抗分枝杆菌活性的机制,宿主免疫应答的操纵以及AMPs作为治疗剂的未来前景。

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