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In-host population dynamics of

机译:宿主人口动态

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摘要

Tuberculosis (TB) is a leading cause of death globally. Understanding the population dynamics of TB’s causative agent Mycobacterium tuberculosis complex (Mtbc) in-host is vital for understanding the efficacy of antibiotic treatment. We use longitudinally collected clinical Mtbc isolates that underwent Whole-Genome Sequencing from the sputa of 200 patients to investigate Mtbc diversity during the course of active TB disease after excluding 107 cases suspected of reinfection, mixed infection or contamination. Of the 178/200 patients with persistent clonal infection >2 months, 27 developed new resistance mutations between sampling with 20/27 occurring in patients with pre-existing resistance. Low abundance resistance variants at a purity of ≥19% in the first isolate predict fixation in the subsequent sample. We identify significant in-host variation in 27 genes, including antibiotic resistance genes, metabolic genes and genes known to modulate host innate immunity and confirm several to be under positive selection by assessing phylogenetic convergence across a genetically diverse sample of 20,352 isolates.
机译:结核病(TB)是全球死亡的主要原因。了解TB的致病剂的人口动态分枝杆菌结核分枝杆菌复合物(MTBC)的宿主对患者对抗生素治疗的疗效至关重要。我们使用纵向收集的临床MTBC分离物,该分离物从200名患者的30例患者的SPUTA中进行了全基因组测序,以在涉嫌重新感染,混合感染或污染的107例患者中探讨了MTBC多样性。在持续克隆感染患者的178/200名患者中> 2个月,27例在具有预先存在的抗性的患者中产生了20/27的取样之间的新电阻突变。在第一种分离物中纯度≥19%的低丰度抗性变体预测后续样品中的固定。我们鉴定了27个基因的显着的宿主变异,包括抗生素抗性基因,已知调节宿主先天免疫的代谢基因和基因,并通过评估20,352个分离物的遗传多样化样品中的系统发育收敛来确认几种阳性选择。

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