Clofazimine and QT prolongation in the treatment of rifampicin-resistant tuberculosis: Findings of aDSM in Taiwan

IF 4.5 2区 医学 Q2 IMMUNOLOGY Journal of Microbiology Immunology and Infection Pub Date : 2024-08-08 DOI:10.1016/j.jmii.2024.08.002
Chou-Jui Lin , Jin-Hua Chen , Shun-Tien Chien , Yi-Wen Huang , Chih-Bin Lin , Jen-Jyh Lee , Chih-Hsin Lee , Ming-Chih Yu , Chen-Yuan Chiang
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Abstract

Background

Bedaquiline, delamanid and fluoroquinolones are associated with increased QTcF. Whether clofazimine is associated with QTcF prolongation is less clear.

Methods

All patients with rifampicin-resistant TB enrolled between May 2017 and Dec 2019 were included. ECGs were performed at baseline, month 1, month 3 and month 6 for patients treated with conventional regimens, and at additional timepoint for patients treated with bedaquiline, delamanid and short regimen. We estimated the maximum increase of QTcF and constructed cox proportional hazards models to assess factors associated with QTcF≥501ms.

Results

Among 321 patients, 59 (18.4%) patients had QTcF≥501ms during a mean follow-up of 242 days (median 189, range 4–1091). The median maximum increase of QTcF was 43.4 ms (IQR 31.3–65.9) in patients treated with clofazimine. Treatment with clofazimine was significantly associated with QTcF≥501ms as compared to without clofazimine (adjusted hazards ratio (adjHR) 4.35, 95% confidence interval (CI) 2.01–9.44). Among patients not treated with bedaquiline and delamanid, those treated with clofazimine and a fluoroquinolone (adjHR 3.43, 95% CI 1.61–7.34) and those treated with clofazimine and high dose moxifloxacin (adjHR 6.54, 95% CI 2.43–17.60) had a significantly higher risk of QTcF≥501ms as compared to those treated with a fluoroquinolone without other QTcF prolonging agents. Four (1.6%) patients had documented ventricular tachycardia, in which one was Torsade de pointes. One patient was found to have sudden death during hospitalization.

Conclusions

Clofazimine was significantly associated with an increased risk of QTcF prolongation. QTcF≥501ms was potentially associated with fatal event and needed to be managed cautiously.

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治疗耐利福平结核病时氯苯胍与 QT 间期延长:台湾 aDSM 的研究结果。
背景:贝达喹啉、delamanid和氟喹诺酮类药物与QTcF延长有关。氯法齐明是否与QTcF延长有关尚不清楚:纳入2017年5月至2019年12月期间入组的所有耐利福平肺结核患者。对接受常规方案治疗的患者在基线、第1个月、第3个月和第6个月进行心电图检查,对接受贝达喹啉、地拉那米德和短方案治疗的患者在额外的时间点进行心电图检查。我们估算了 QTcF 的最大增幅,并构建了 cox 比例危险模型来评估与 QTcF≥501ms 相关的因素:在 321 名患者中,有 59 名(18.4%)患者在平均 242 天(中位数 189 天,范围 4-1091 天)的随访期间 QTcF≥501ms 。在接受氯法齐明治疗的患者中,QTcF的最大增幅中位数为43.4毫秒(IQR为31.3-65.9)。与不使用氯唑明相比,使用氯唑明治疗与 QTcF≥501ms 显著相关(调整危险比 (adjHR) 4.35,95% 置信区间 (CI) 2.01-9.44)。在未接受贝达喹啉和地拉马尼治疗的患者中,接受氯法齐明和氟喹诺酮治疗的患者(adjHR为3.43,95% CI为1.61-7.34)和接受氯法齐明和大剂量莫西沙星治疗的患者(adjHR为6.54,95% CI为2.43-17.60)与接受氟喹诺酮治疗且未使用其他QTcF延长药物的患者相比,QTcF≥501ms的风险明显更高。4例(1.6%)患者有室性心动过速记录,其中1例为室性心动过速。一名患者在住院期间猝死:结论:氯法齐明与 QTcF 延长风险的增加有显著相关性。QTcF≥501ms可能与致命事件有关,需要谨慎处理。
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来源期刊
Journal of Microbiology Immunology and Infection
Journal of Microbiology Immunology and Infection IMMUNOLOGY-INFECTIOUS DISEASES
CiteScore
15.90
自引率
5.40%
发文量
159
审稿时长
67 days
期刊介绍: Journal of Microbiology Immunology and Infection is an open access journal, committed to disseminating information on the latest trends and advances in microbiology, immunology, infectious diseases and parasitology. Article types considered include perspectives, review articles, original articles, brief reports and correspondence. With the aim of promoting effective and accurate scientific information, an expert panel of referees constitutes the backbone of the peer-review process in evaluating the quality and content of manuscripts submitted for publication.
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