喀麦隆结核病与艾滋病毒合并感染患者中药物性肝毒性及其与慢乙酰化变体NAT25和NAT26的关联。

Drug-induced hepatotoxicity and association with slow acetylation variants NAT25 and NAT26 in Cameroonian patients with tuberculosis and HIV co-infection.

作者信息

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

机构信息

Institute of Tropical Medicine, University of Tübingen, Wilhelmstrasse 27, 72074, Tübingen, Germany.

Faculty of Sciences, University of Buea, Buea, Cameroon.

出版信息

BMC Infect Dis. 2024 Jul 31;24(1):759. doi: 10.1186/s12879-024-09638-w.

DOI:10.1186/s12879-024-09638-w

PMID:39085767

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11293078/

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 NAT25 was associated with a decreased risk of DIH (OR: 0.4; 95%CI: 0.17-0.96; p = 0.038), while NAT26 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 NAT25 and NAT26 variants were found to be associated with DIH in the Cameroonian population. Prior screening for the slow acetylation variants NAT25 and NAT26 may prevent DIH in TB and HIV-coinfected patients.

摘要

背景

人类免疫缺陷病毒（HIV）和结核病（TB）是包括喀麦隆在内的撒哈拉以南非洲地区发病和死亡的主要原因。药物遗传学变异可能是HIV合并感染TB患者药物性肝毒性（DIH）的预测指标。我们评估了喀麦隆患者中DIH和药物遗传学变异的发生情况。

方法

2018年9月至2019年11月期间，在喀麦隆的三家医院招募了未接受过治疗的HIV、TB或TB/HIV合并感染患者。开始进行适当治疗，并对患者进行12周的随访以评估DIH。通过等位基因鉴别TaqMan SNP分析评估药物遗传学变异。

结果

在141例未接受过治疗的患者中，DIH的总体发生率为38%（53/141）。在HIV患者中观察到最高的DIH发生率，为52%（32/61）。在32种药物遗传学变异中，慢乙酰化变异NAT25与DIH风险降低相关（OR：0.4；95%CI：0.17 - 0.96；p = 0.038），而在接受TB治疗的患者中，NAT26与DIH风险增加相关（OR：4.2；95%CI：1.1 - 15.2；p = 0.017）。分别有多达15个单核苷酸多态性（SNP）在非洲人群中等位基因频率差异≥5%，而25个SNP在非非洲人群中等位基因频率差异≥5%。

结论

DIH是非洲TB和HIV患者的一个重要临床问题。在喀麦隆人群中发现NAT25和NAT26变异与DIH相关。预先筛查慢乙酰化变异NAT25和NAT26可能预防TB和HIV合并感染患者发生DIH。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7669/11293078/6ccf4efad536/12879_2024_9638_Fig1_HTML.jpg

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喀麦隆结核病与艾滋病毒合并感染患者中药物性肝毒性及其与慢乙酰化变体NAT2*5和NAT2*6的关联。

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

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喀麦隆结核病与艾滋病毒合并感染患者中药物性肝毒性及其与慢乙酰化变体NAT25和NAT26的关联。

Drug-induced hepatotoxicity and association with slow acetylation variants NAT25 and NAT26 in Cameroonian patients with tuberculosis and HIV co-infection.