A case of hepatic dysfunction from crizotinib followed by treatment with entrectinib

IF 0.2 Q4 ONCOLOGY
Takahito Mizuno , Satoshi Hagimoto , Takumi Umemura , Mariko Higashikawa , Takamasa Sakai , Kouichi Tanabe , Fumiko Ohtsu , Tetsuya Yamada , Tomoki Kimura
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引用次数: 0

Abstract

Background

Information regarding the safety of entrectinib for previously treated patients and patients with hepatic dysfunction is limited. This is the first case report of treatment modification attributable to hepatic dysfunction caused by crizotinib.

Patients

A 76-year-old Japanese woman was referred to the Department of Respiratory Medicine and Allergy after a computed tomography (CT) scan at the time of thyroid surgery. The CT scan revealed an enlarged right upper lobe nodule. After careful examination, she was diagnosed with T3N2M1c stage IV ROS1-positive lung adenocarcinoma; therefore, crizotinib (500 mg/day) was prescribed. On day 861 of treatment, crizotinib was discontinued because of repeatedly observed increased aspartate aminotransferase (AST) and alanine aminotransferase (ALT) levels. Approximately 2 weeks after crizotinib was discontinued, treatment was restarted with entrectinib 600 mg/day.

Conclusions

Entrectinib was prescribed because crizotinib caused hepatic dysfunction; however, the patient experienced grade 3 neutropenia and the creatinine phosphokinase (CPK) levels increased. After the dose reduction, she was able to continue treatment safely, without further worsening of the primary tumor or hepatic dysfunction. Therefore, entrectinib may be an option for patients who need treatment modification because of crizotinib-induced hepatic dysfunction. Increased CPK is a previously unknown adverse event occurring with entrectinib. This information is essential to risk management plans involving this drug. Further information regarding increased CPK and rhabdomyolysis occurring in patients treated with entrectinib is needed.

克唑替尼治疗肝功能障碍1例
背景关于恩曲替尼对既往接受治疗的患者和肝功能障碍患者的安全性的信息有限。这是第一例因克唑替尼引起肝功能不全而改变治疗的病例报告。患者一名76岁的日本妇女在甲状腺手术时进行了计算机断层扫描(CT)后,被转诊至呼吸医学和过敏科。CT扫描显示右上叶结节增大。经过仔细检查,她被诊断为T3N2M1c IV期ROS1阳性肺腺癌;因此,处方为克唑替尼(500mg/天)。治疗第861天,由于反复观察到天冬氨酸转氨酶(AST)和丙氨酸转氨酶(ALT)水平升高,克唑替尼停用。克唑替尼停药约2周后,用恩曲替尼600mg/天重新开始治疗;然而,患者出现3级中性粒细胞减少症,肌酸酐磷酸激酶(CPK)水平升高。在剂量减少后,她能够安全地继续治疗,而不会进一步恶化原发性肿瘤或肝功能障碍。因此,对于因克唑替尼诱导的肝功能不全而需要修改治疗的患者,恩替尼可能是一种选择。CPK升高是一种以前未知的因替尼引起的不良事件。这些信息对于涉及该药物的风险管理计划至关重要。需要更多关于恩曲替尼治疗患者CPK增加和横纹肌溶解症的信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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