非小细胞肺癌肥胖患者因阿那莫瑞林诱发 QT 间期延长的病例报告。

IF 1.2 Q4 PHARMACOLOGY & PHARMACY
Hayato Yokota, Ruriko Asahi, Yumiko Akamine, Mizuki Kobayashi, Hiyu Wakabayashi, Sho Sakamoto, Yuji Okuda, Kazuhiro Sato, Katsutoshi Nakayama, Masafumi Kikuchi
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引用次数: 0

摘要

背景:阿那莫林是一种治疗癌症恶病质的药物,能与胃泌素受体结合,改善体重和食欲。在日本的临床试验中,患者出现刺激传导系统抑制这一严重副作用的频率为 10.7%。阿那莫瑞林虽然罕见,但有时会导致致命性心律失常。由于癌症恶病质患者通常体重过轻,因此缺乏有关肥胖患者服用阿那莫瑞林安全性的数据。我们报告了一例非小细胞肺癌肥胖患者服用阿莫瑞林后出现 QT 间期延长的病例:一名体重指数为 30 kg/m2 的女性患者接受了肺腺癌免疫治疗。她出现了严重的体重减轻、厌食和乏力。她没有心脏病史。在服用阿那莫瑞林 100 毫克、每天一次后的第 12 天,患者出现了恶心、腹泻和厌食,这被认为是癌症免疫疗法引起的免疫相关不良事件,于是她被送进了医院。入院时的心电图(ECG)显示QTc间期为502毫秒。入院时,她的肝功能为 Child-Pugh B 级,第二天停用了阿莫瑞林。停用阿莫瑞林后的第 3 天,QTc 间期延长达 557 毫秒,第 6 天降至 490 毫秒,第 16 天改善至 450 毫秒。避免了再次使用阿莫瑞林:结论:在对肥胖患者施用阿莫瑞林时,我们应注意刺激传导系统抑制的可能性,就像对体重不足的患者一样。因此,我们应该在使用阿那莫瑞林的早期阶段就通过心电图对患者进行监测。阿那莫瑞林具有亲脂性,其在肥胖患者体内的分布容积会增加。因此,肥胖患者在停用阿那莫瑞林后可能会继续出现 QT 间期延长,需要长期监测其副作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Case report of QT interval prolongation induced by anamorelin in an obese patient with non-small cell lung cancer.

Background: Anamorelin, a drug to treat cancer cachexia, binds to ghrelin receptors and improves body weight and appetite. In clinical trials in Japan, patients experienced a 10.7% frequency of stimulant conduction system depression as a severe side effect. Although rare, anamorelin sometimes causes fatal arrhythmias. Because patients with cancer cachexia are often underweight, data on the safety of anamorelin in obese patients are lacking. We report a case of QT interval prolongation after anamorelin administration to an obese patient with non-small cell lung cancer.

Case presentation: A female patient with a body mass index of 30 kg/m2 underwent immunotherapy for lung adenocarcinoma. She presented with severe weight loss, anorexia, and fatigue. She had no history of heart disease. On day 12, after administration of anamorelin 100 mg once daily, the patient developed nausea, diarrhea, and anorexia, which were considered cancer immunotherapy-induced immune-related adverse events, and she was admitted to the hospital. An electrocardiogram (ECG) on admission showed a QTc interval of 502 ms. On admission, her hepatic function was Child-Pugh class B, and anamorelin was discontinued the next day. On day 3 after anamorelin discontinuation, the QTc interval was prolonged by up to 557 ms, then decreased to 490 ms on day 6, and improved to 450 ms on day 16. Re-administration of anamorelin was avoided.

Conclusions: When administering anamorelin to obese patients, we should be aware of the potential for stimulatory conduction system depression, as in underweight patients. Therefore, we should monitor patients by ECG from the early stages of anamorelin administration. Anamorelin is lipophilic, and its volume of distribution is increased in obese patients. Consequently, obese patients may continue to have QT interval prolongation after discontinuation of anamorelin, requiring long-term side-effect monitoring.

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来源期刊
CiteScore
1.80
自引率
0.00%
发文量
29
审稿时长
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