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The perceived impact of isoniazid resistance on outcome of first-line rifampicin-throughout regimens is largely due to missed rifampicin resistance

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Listed:
  • Armand Van Deun
  • Tom Decroo
  • Aung Kya Jai Maug
  • Mohamed Anwar Hossain
  • Murid Gumusboga
  • Wim Mulders
  • Nimer Ortuño-Gutiérrez
  • Lutgarde Lynen
  • Bouke C de Jong
  • Hans L Rieder

Abstract

Background: Meta-analyses on impact of isoniazid-resistant tuberculosis informed the World Health Organization recommendation of a levofloxacin-strengthened rifampicin-based regimen. Methods: Retrospective analysis of 7291 treatment episodes with known initial isoniazid and rifampicin status obtained from individual patient databases maintained by the Damien Foundation Bangladesh over 20 years. Drug susceptibility test results were confirmed by the programme’s designated supra-national tuberculosis laboratory. To detect missed Rr among isolates routinely classified as Hr, rpoB gene sequencing was done randomly and on a sample selected for suspected missed Rr. Results: Initial Hr caused a large recurrence excess after the 8-month regimen for new cases (rifampicin for two months), but had little impact on rifampicin-throughout regimens: (6 months, new cases; 3.8%; OR 0.8, 95%CI:0.3,2.8; 8 months, retreatment cases: 7.3%, OR 1.8; 95%CI:1.3,2.6). Rr was missed in 7.6% of randomly selected "Hr" strains. Acquired Rr was frequent among recurrences on rifampicin-throughout regimens, particularly after the retreatment regimen (31.9%). It was higher in mono-Hr (29.3%; aOR 3.5, 95%CI:1.5,8.5) and poly-Hr (53.3%; aOR 10.2, 95%CI 4.4,23.7) than in susceptible tuberculosis, but virtually absent after the 8-month new case regimen. Comparing Bangladesh (low Rr prevalence) with a high Rr prevalence setting,true Hr corrected for missed Rr caused only 2–3 treatment failures per 1000 TB cases (of whom 27% were retreatments) in both. Conclusions: Our analysis reveals a non-negligible extent of misclassifying as isoniazid resistance of what is actually missed multidrug-resistant tuberculosis. Recommending for such cases a “strengthened” regimen containing a fluoroquinolone provokes a direct route to extensive resistance while offering little benefit against the minor role of true Hr tuberculosis in rifampicin-throughout first-line regimen.

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  • Armand Van Deun & Tom Decroo & Aung Kya Jai Maug & Mohamed Anwar Hossain & Murid Gumusboga & Wim Mulders & Nimer Ortuño-Gutiérrez & Lutgarde Lynen & Bouke C de Jong & Hans L Rieder, 2020. "The perceived impact of isoniazid resistance on outcome of first-line rifampicin-throughout regimens is largely due to missed rifampicin resistance," PLOS ONE, Public Library of Science, vol. 15(5), pages 1-18, May.
  • Handle: RePEc:plo:pone00:0233500
    DOI: 10.1371/journal.pone.0233500
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    1. Anonymous, 1964. "World Health Organization," International Organization, Cambridge University Press, vol. 18(4), pages 859-870, October.
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