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  4. The within-host population dynamics of Mycobacterium tuberculosis vary with treatment efficacy
 
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The within-host population dynamics of Mycobacterium tuberculosis vary with treatment efficacy

Date Issued
2017-01-01
Author(s)
Trauner, Andrej
Liu, Qingyun
Via, Laura E.
Liu, Xin
Ruan, Xianglin
Liang, Lili
Shi, Huimin
Chen, Ying
Wang, Ziling
Liang, Ruixia
Zhang, Wei
Wei, Wang
Gao, Jingcai
Sun, Gang
Brites, Daniela  
England, Kathleen
Zhang, Guolong
Gagneux, Sebastien  
Barry, Clifton E.
Gao, Qian
DOI
10.1186/s13059-017-1196-0
Abstract
Combination therapy is one of the most effective tools for limiting the emergence of drug resistance in pathogens. Despite the widespread adoption of combination therapy across diseases, drug resistance rates continue to rise, leading to failing treatment regimens. The mechanisms underlying treatment failure are well studied, but the processes governing successful combination therapy are poorly understood. We address this question by studying the population dynamics of Mycobacterium tuberculosis within tuberculosis patients undergoing treatment with different combinations of antibiotics.; By combining very deep whole genome sequencing (~1000-fold genome-wide coverage) with sequential sputum sampling, we were able to detect transient genetic diversity driven by the apparently continuous turnover of minor alleles, which could serve as the source of drug-resistant bacteria. However, we report that treatment efficacy has a clear impact on the population dynamics: sufficient drug pressure bears a clear signature of purifying selection leading to apparent genetic stability. In contrast, M. tuberculosis populations subject to less drug pressure show markedly different dynamics, including cases of acquisition of additional drug resistance.; Our findings show that for a pathogen like M. tuberculosis, which is well adapted to the human host, purifying selection constrains the evolutionary trajectory to resistance in effectively treated individuals. Nonetheless, we also report a continuous turnover of minor variants, which could give rise to the emergence of drug resistance in cases of drug pressure weakening. Monitoring bacterial population dynamics could therefore provide an informative metric for assessing the efficacy of novel drug combinations.
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