Transcriptional Adaptation of Drug-tolerant Mycobacterium tuberculosis During Treatment of Human Tuberculosis.

نویسندگان

  • Nicholas D Walter
  • Gregory M Dolganov
  • Benjamin J Garcia
  • William Worodria
  • Alfred Andama
  • Emmanuel Musisi
  • Irene Ayakaka
  • Tran T Van
  • Martin I Voskuil
  • Bouke C de Jong
  • Rebecca M Davidson
  • Tasha E Fingerlin
  • Katerina Kechris
  • Claire Palmer
  • Payam Nahid
  • Charles L Daley
  • Mark Geraci
  • Laurence Huang
  • Adithya Cattamanchi
  • Michael Strong
  • Gary K Schoolnik
  • John Lucian Davis
چکیده

BACKGROUND Treatment initiation rapidly kills most drug-susceptible Mycobacterium tuberculosis, but a bacterial subpopulation tolerates prolonged drug exposure. We evaluated drug-tolerant bacilli in human sputum by comparing messenger RNA (mRNA) expression of drug-tolerant bacilli that survive the early bactericidal phase with treatment-naive bacilli. METHODS M. tuberculosis gene expression was quantified via reverse-transcription polymerase chain reaction in serial sputa from 17 Ugandans treated for drug-susceptible pulmonary tuberculosis. RESULTS Within 4 days, bacterial mRNA abundance declined >98%, indicating rapid killing. Thereafter, the rate of decline slowed >94%, indicating drug tolerance. After 14 days, 16S ribosomal RNA transcripts/genome declined 96%, indicating slow growth. Drug-tolerant bacilli displayed marked downregulation of genes associated with growth, metabolism, and lipid synthesis and upregulation in stress responses and key regulatory categories-including stress-associated sigma factors, transcription factors, and toxin-antitoxin genes. Drug efflux pumps were upregulated. The isoniazid stress signature was induced by initial drug exposure, then disappeared after 4 days. CONCLUSIONS Transcriptional patterns suggest that drug-tolerant bacilli in sputum are in a slow-growing, metabolically and synthetically downregulated state. Absence of the isoniazid stress signature in drug-tolerant bacilli indicates that physiological state influences drug responsiveness in vivo. These results identify novel drug targets that should aid in development of novel shorter tuberculosis treatment regimens.

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عنوان ژورنال:
  • The Journal of infectious diseases

دوره 212 6  شماره 

صفحات  -

تاریخ انتشار 2015