BMC Infectious Diseases (Jul 2024)

Drug-induced hepatotoxicity and association with slow acetylation variants NAT2*5 and NAT2*6 in Cameroonian patients with tuberculosis and HIV co-infection

  • Frederick Nchang Cho,
  • Eric A. Achidi,
  • Jude Eteneneng Enoh,
  • Srinivas Reddy Pallerla,
  • Le Thi Kieu Linh,
  • Hoang Van Tong,
  • Joseph Kamgno,
  • Véronique Beng Penlap,
  • Ayola Akim Adegnika,
  • Jean-Bernard Lekana-Douki,
  • Marielle Karine Bouyou-Akotet,
  • Gauthier Mesia Kahunu,
  • Gaston Tona Lutete,
  • Mathew Bates,
  • John Tembo,
  • Linzy Elton,
  • Timothy D McHugh,
  • Martin P Grobusch,
  • Alimuddin Zumla,
  • Francine Ntoumi,
  • Thirumalaisamy P. Velavan

DOI
https://doi.org/10.1186/s12879-024-09638-w
Journal volume & issue
Vol. 24, no. 1
pp. 1 – 13

Abstract

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Abstract Background Human immunodeficiency virus (HIV) and tuberculosis (TB) are major contributors to morbidity and mortality in sub-Saharan Africa including Cameroon. Pharmacogenetic variants could serve as predictors of drug-induced hepatotoxicity (DIH), in patients with TB co-infected with HIV. We evaluated the occurrence of DIH and pharmacogenetic variants in Cameroonian patients. Methods Treatment-naïve patients with HIV, TB or TB/HIV co-infection were recruited at three hospitals in Cameroon, between September 2018 and November 2019. Appropriate treatment was initiated, and patients followed up for 12 weeks to assess DIH. Pharmacogenetic variants were assessed by allele discrimination TaqMan SNP assays. Results Of the 141 treatment naïve patients, the overall incidence of DIH was 38% (53/141). The highest incidence of DIH, 52% (32/61), was observed among HIV patients. Of 32 pharmacogenetic variants, the slow acetylation variants NAT2*5 was associated with a decreased risk of DIH (OR: 0.4; 95%CI: 0.17–0.96; p = 0.038), while NAT2*6 was found to be associated with an increased risk of DIH (OR: 4.2; 95%CI: 1.1–15.2; p = 0.017) among patients treated for TB. Up to 15 SNPs differed in ≥ 5% of allele frequencies among African populations, while 25 SNPs differed in ≥ 5% of the allele frequencies among non-African populations, respectively. Conclusions DIH is an important clinical problem in African patients with TB and HIV. The NAT2*5 and NAT2*6 variants were found to be associated with DIH in the Cameroonian population. Prior screening for the slow acetylation variants NAT2*5 and NAT2*6 may prevent DIH in TB and HIV-coinfected patients.

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