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Consequences of Noncompliance for Therapy Efficacy and Emergence of Resistance in Murine Tuberculosis Caused by the Beijing Genotype of Mycobacterium tuberculosis

机译:北京结核分枝杆菌基因型引起的鼠结核的治疗功效和耐药性产生的不合规后果

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摘要

Despite great effort by health organizations worldwide in fighting tuberculosis (TB), morbidity and mortality are not declining as expected. One of the reasons is related to the evolutionary development of Mycobacterium tuberculosis, in particular the Beijing genotype strains. In a previous study, we showed the association between the Beijing genotype and an increased mutation frequency for rifampin resistance. In this study, we use a Beijing genotype strain and an East-African/Indian genotype strain to investigate with our mouse TB model whether the higher mutation frequency observed in a Beijing genotype strain is associated with treatment failure particularly during noncompliance therapy. Both genotype strains showed high virulence in comparison to that of M. tuberculosis strain H37Rv, resulting in a highly progressive infection with a rapid lethal outcome in untreated mice. Compliance treatment was effective without relapse of TB irrespective of the infecting strain, showing similar decreases in the mycobacterial load in infected organs and similar histopathological changes. Noncompliance treatment, simulated by a reduced duration and dosing frequency, resulted in a relapse of infection. Relapse rates were correlated with the level of noncompliance and were identical for Beijing infection and East African/Indian infection. However, only in Beijing-infected mice, isoniazid-resistant mutants were selected at the highest level of noncompliance. This is in line with the substantial selection of isoniazid-resistant mutants in vitro in a wide isoniazid concentration window observed for the Beijing strain and not for the EAI strain. These results suggest that genotype diversity of M. tuberculosis may be involved in emergence of resistance and indicates that genotype-tailor-made treatment should be investigated.
机译:尽管全球卫生组织在抗击结核病方面做出了巨大努力,但发病率和死亡率并未如预期的那样下降。原因之一与结核分枝杆菌特别是北京基因型菌株的进化发展有关。在先前的研究中,我们显示了北京基因型与利福平耐药性的突变频率增加之间的关联。在这项研究中,我们使用北京基因型菌株和东非/印度基因型菌株,通过我们的小鼠TB模型调查北京基因型菌株中观察到的较高突变频率是否与治疗失败相关,尤其是在不依从治疗期间。与结核分枝杆菌菌株H37Rv相比,两种基因型菌株均显示出高毒力,在未经治疗的小鼠中导致高度进行性感染,并具有快速致死性。顺应性治疗是有效的,无论感染菌株如何,都不会结核病复发,在受感染器官中分枝杆菌载量下降相似,组织病理学变化也相似。通过减少持续时间和给药频率模拟的不合规治疗导致感染复发。复发率与不依从程度相关,北京感染和东非/印度感染也相同。但是,仅在北京感染的小鼠中,异烟肼抗性突变体的违规程度最高。这与在北京菌株而非EAI菌株中观察到的广泛的异烟肼浓度范围内在体外大量选择耐异烟肼的突变体是一致的。这些结果表明结核分枝杆菌的基因型多样性可能与耐药性的产生有关,并表明应研究基因型量身定制的治疗方法。

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