Clinically prevalent mutations in Mycobacterium tuberculosis alter propionate metabolism and mediate multidrug tolerance.
Nathan D HicksJian YangXiaobing ZhangBing ZhaoYonatan Hagai GradLiguo LiuXichao OuZhili ChangHui XiaYang ZhouShengfen WangJie DongLilian SunYafang ZhuYan-Lin ZhaoQi JinSarah M FortunePublished in: Nature microbiology (2018)
The global epidemic of drug-resistant tuberculosis is a catastrophic example of how antimicrobial resistance is undermining the public health gains made possible by combination drug therapy. Recent evidence points to unappreciated bacterial factors that accelerate the emergence of drug resistance. In a genome-wide association study of Mycobacterium tuberculosis isolates from China, we find mutations in the gene encoding the transcription factor prpR enriched in drug-resistant strains. prpR mutations confer conditional drug tolerance to three of the most effective classes of antibiotics by altering propionyl-CoA metabolism. prpR-mediated drug tolerance is carbon-source dependent, and while readily detectable during infection of human macrophages, is not captured by standard susceptibility testing. These data define a previously unrecognized and clinically prevalent class of M. tuberculosis variants that undermine antibiotic efficacy and drive drug resistance.
Keyphrases
- drug resistant
- mycobacterium tuberculosis
- multidrug resistant
- antimicrobial resistance
- acinetobacter baumannii
- public health
- pulmonary tuberculosis
- transcription factor
- genome wide association study
- adverse drug
- copy number
- endothelial cells
- emergency department
- electronic health record
- genome wide
- machine learning
- gene expression
- deep learning
- dna methylation
- mesenchymal stem cells
- genome wide identification
- human immunodeficiency virus
- cell therapy
- global health