Publication | Closed Access
NAT2 Slow Acetylator is Associated with Anti-tuberculosis Drug-induced Liver injury Severity in Indonesian Population
25
Citations
24
References
2019
Year
<b>Aim:</b> We investigated the contribution of NAT2 variants and acetylator status to anti-tuberculosis drug-induced liver injury (AT-DILI) severity. <b>Materials & methods:</b> 100 patients with clinically severe AT-DILI and 210 non-AT-DILI controls were subjected to NAT2 genotyping by direct DNA sequencing. <b>Results:</b> NAT2 slow acetylator was significantly associated with AT-DILI risk (p = 2.7 × 10<sup>-7</sup>; odds ratio [95% CI] = 3.64 [2.21-6.00]). Subgroup analysis of NAT2 ultra-slow acetylator revealed a stronger association with AT-DILI risk (p = 4.3 × 10<sup>-6</sup>; odds ratio [95% CI] = 3.37 [2.00-5.68]). Subset analysis of NAT2 acetylator status and severity grade confirmed these results in AT-DILI patients with more severe disease whereas fast and intermediate acetylator phenotypes were associated with a decreased AT-DILI risk. <b>Conclusion:</b> We elucidated the role of NAT2 phenotypes in AT-DILI in Indonesian population, suggesting that NAT2 genotype and phenotype determination are important to reduce AT-DILI risk.
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