耐多药结核病中注射用阿米卡星和卷曲霉素的不良反应与选择。
Adverse Effects and Choice between the Injectable Agents Amikacin and Capreomycin in Multidrug-Resistant Tuberculosis.
机构信息
Institute for Infection and Immunity, St. George's University of London, London, United Kingdom
Division of Medicine, Imperial College London, London, United Kingdom.
出版信息
Antimicrob Agents Chemother. 2017 Aug 24;61(9). doi: 10.1128/AAC.02586-16. Print 2017 Sep.
The prolonged use of injectable agents in a regimen for the treatment of multidrug-resistant tuberculosis (MDR-TB) is recommended by the World Health Organization, despite its association with ototoxicity and nephrotoxicity. We undertook this study to look at the relative adverse effects of capreomycin and amikacin. We reviewed the case notes of 100 consecutive patients treated at four MDR-TB treatment centers in the United Kingdom. The median total duration of treatment with an injectable agent was 178 days (interquartile range [IQR], 109 to 192 days; = 73) for those with MDR-TB, 179 days (IQR, 104 to 192 days; = 12) for those with MDR-TB plus fluoroquinolone resistance, and 558 days (IQR, 324 to 735 days; = 8) for those with extensively drug-resistant tuberculosis (XDR-TB). Injectable use was longer for those started with capreomycin (183 days; IQR, 123 to 197 days) than those started with amikacin (119 days; IQR, 83 to 177 days) ( = 0.002). Excluding patients with XDR-TB, 51 of 85 (60%) patients were treated with an injectable for over 6 months and 12 of 85 (14%) were treated with an injectable for over 8 months. Forty percent of all patients discontinued the injectable due to hearing loss. Fifty-five percent of patients experienced ototoxicity, which was 5 times (hazard ratio [HR], 5.2; 95% confidence interval [CI], 1.2 to 22.6; = 0.03) more likely to occur in those started on amikacin than in those treated with capreomycin only. Amikacin was associated with less hypokalemia than capreomycin (odds ratio, 0.28; 95% CI, 0.11 to 0.72), with 5 of 37 (14%) patients stopping capreomycin due to recurrent electrolyte loss. There was no difference in the number of patients experiencing a rise in the creatinine level of >1.5 times the baseline level. Hearing loss is frequent in this cohort, though its incidence is significantly lower in those starting capreomycin, which should be given greater consideration as a first-line agent.
尽管注射用药物与耳毒性和肾毒性相关联,但世界卫生组织仍建议在治疗耐多药结核病(MDR-TB)的方案中长期使用注射用药物。我们开展这项研究旨在观察卷曲霉素和阿米卡星的相对不良反应。我们对英国四个 MDR-TB 治疗中心的 100 例连续患者的病历进行了回顾。对于 MDR-TB 患者,注射用药物的中位总治疗时间为 178 天(四分位距[IQR],109 至 192 天; = 73),对于 MDR-TB 加氟喹诺酮耐药患者为 179 天(IQR,104 至 192 天; = 12),对于广泛耐药结核病(XDR-TB)患者为 558 天(IQR,324 至 735 天; = 8)。与起始使用阿米卡星(119 天;IQR,83 至 177 天)的患者相比,起始使用卷曲霉素(183 天;IQR,123 至 197 天)的患者注射用药物使用时间更长( = 0.002)。排除 XDR-TB 患者后,85 例患者中有 51 例(60%)接受了 6 个月以上的注射治疗,12 例(14%)接受了 8 个月以上的注射治疗。由于听力损失,40%的所有患者停止使用注射用药物。55%的患者出现耳毒性,起始使用阿米卡星的患者发生耳毒性的可能性是仅使用卷曲霉素的患者的 5 倍(风险比[HR],5.2;95%置信区间[CI],1.2 至 22.6; = 0.03)。与卷曲霉素相比,阿米卡星导致低钾血症的可能性较小(比值比,0.28;95%CI,0.11 至 0.72),有 5 例(14%)患者因反复电解质丢失而停止使用卷曲霉素。肌酐水平升高超过基线水平 1.5 倍的患者人数没有差异。在本队列中,听力损失很常见,但起始使用卷曲霉素的患者发生率明显较低,卷曲霉素应作为一线药物给予更多考虑。
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