Pharmacogenetics of tuberculosis treatment toxicity and effectiveness in a large Brazilian cohort

  1. Gustavo Amorim
  2. James Jaworski
  3. Jing Yang
  4. Marcelo Cordeiro-Santos
  5. Afrânio L. Kritski
  6. Marina C. Figueiredo
  7. Megan Turner
  8. Bruno B. Andrade
  9. Digna R. Velez Edwards
  10. Adalberto R. Santos
  11. Valeria C. Rolla
  12. Timothy R. Sterling
  13. David W. Haas
  14. the Regional Prospective Observational Research in Tuberculosis (RePORT)-Brazil network
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Abstract

Genetic polymorphisms have been associated with risk of antituberculosis treatment toxicity. We characterized associations with adverse events and treatment failure/recurrence among adults treated for tuberculosis in Brazil.

Methods

Participants were followed in Regional Prospective Observational Research in Tuberculosis (RePORT)-Brazil. We included persons with culture-confirmed drug-susceptible pulmonary tuberculosis who started treatment between 2015 and 2019, and who were eligible for pharmacogenetics. Treatment included 2 months of isoniazid, rifampin or rifabutin, pyrazinamide, and ethambutol, then 4 months of isoniazid and rifampin or rifabutin, with 24-month follow-up. Analyses included 43 polymorphisms in 20 genes related to antituberculosis drug hepatotoxicity or pharmacokinetics. Whole exome sequencing was done in a case-control toxicity subset.

Results

Among 903 participants in multivariable genetic association analyses, NAT2 slow acetylator status was associated with increased risk of treatment-related grade 2 or greater adverse events, including hepatotoxicity. Treatment failure/recurrence was more likely among NAT2 rapid acetylators, but not statistically significant at the 5% level. A GSTM1 polymorphism (rs412543) was associated with increased risk of treatment-related adverse events, including hepatotoxicity. SLCO1B1 polymorphisms were associated with increased risk of treatment-related hepatoxicity and treatment failure/recurrence. Polymorphisms in NR1/2 were associated with decreased risk of adverse events and increased risk of failure/recurrence. In whole exome sequencing, hepatotoxicity was associated with a polymorphism in VTI1A , and the genes METTL17 and PRSS57 , but none achieved genome-wide significance.

Conclusion

In a clinical cohort representing three regions of Brazil, NAT2 acetylator status was associated with risk for treatment-related adverse events. Additional significant polymorphisms merit investigation in larger study populations, particularly regarding risk of treatment failure/recurrence.

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  1. Version published to 10.1097/fpc.0000000000000552
  2. Version published to 10.1101/2023.08.30.23294860v1 on medRxiv