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Understanding anti-tuberculosis drug efficacy: rethinking bacterial populations and how we model them

机译:了解抗结核药的功效:重新思考细菌种群及其建模方法

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Tuberculosis still remains a global health emergency, claiming 1.5 million lives in 2013. The bacterium responsible for this disease, Mycobacterium tuberculosis (M.tb), has successfully survived within hostile host environments, adapting to immune defence mechanisms, for centuries. This has resulted in a disease that is challenging to treat, requiring lengthy chemotherapy with multi-drug regimens. One explanation for this difficulty in eliminating M.tb bacilli in vivo is the disparate action of antimicrobials on heterogeneous populations of M.tb, where mycobacterial physiological state may influence drug efficacy. In order to develop improved drug combinations that effectively target diverse mycobacterial phenotypes, it is important to understand how such subpopulations of M.tb are formed during human infection. We review here the in vitro and in vivo systems used to model M.tb subpopulations that may persist during drug therapy, and offer aspirations for future research in this field.
机译:结核病仍然是全球卫生紧急状况,2013年有150万人死亡。造成这种疾病的细菌结核分枝杆菌(M.tb)在适应宿主的免疫环境中成功存活了数百年,适应了免疫防御机制。这导致了一种难以治疗的疾病,需要长期采用多种药物方案进行化疗。体内消除结核分枝杆菌这种困难的一种解释是,抗菌剂对结核分枝杆菌异种群体的不同作用,其中分枝杆菌的生理状态可能会影响药物疗效。为了开发有效靶向多种分枝杆菌表型的改良药物组合,重要的是要了解在人类感染过程中M.tb的这些亚群是如何形成的。我们在这里回顾了用于模拟可能在药物治疗期间持续存在的M.tb亚群的体外和体内系统,并为该领域的未来研究提供了希望。

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