体外膜肺氧合联合主动脉内球囊反搏治疗肺腺癌靶向药物恩曲替尼所致暴发性心肌炎:一例报告
ECMO combined with IABP for the treatment of fulminant myocarditis caused by the targeted drug entrectinib for lung adenocarcinoma: a case report.
作者信息
Yujuan Qi, Xiaozhong Ma, Zhenhua Wu, Yunpeng Bai
机构信息
Department of Intensive Care Unit, Chest Hospital Affiliated to Tianjin University, Tianjin, China.
Department of Intensive Care Unit, Tianjin Chest Hospital, Tianjin, China.
出版信息
Front Cardiovasc Med. 2025 Aug 1;12:1626318. doi: 10.3389/fcvm.2025.1626318. eCollection 2025.
BACKGROUND
Entrectinib, a recently approved multikinase inhibitor indicated for advanced ROS1-positive non-small cell lung cancer (NSCLC), has demonstrated significant survival benefits in metastatic disease. However, it carries risks of severe cardiotoxicity. We report the successful management of entrectinib-induced fulminant myocarditis using integrated venoarterial extracorporeal membrane oxygenation (V-A ECMO) and intra-aortic balloon pump (IABP) circulatory support.
CASE SUMMARY
A 71-year-old male diagnosed with lung adenocarcinoma three years ago (ROS1-positive on genetic testing) initiated crizotinib therapy. One week prior to admission, surveillance chest computed tomography(CT) revealed disease progression with increased tumor burden, prompting transition to entrectinib. Seven days post-treatment initiation, he presented to our emergency department with acute-onset palpitations, dyspnea, dizziness, and nausea. Emergent coronary angiography excluded significant stenosis. The patient subsequently developed frequent ventricular premature complexes(VPCs), cardiogenic shock (serum lactate 2.6 mmol/L), and acute heart failure. Absent cardiac history and negative viral serology supported a diagnosis of drug-induced fulminant myocarditis. V-A ECMO with IABP support was emergently instituted. Remarkable recovery ensued: cardiac function normalized by day 3 (ECMO decannulation), followed by extubation and IABP removal on day 5.After 12 days of hospitalization, the patient was discharged. Ejection fraction (EF) recovered from 10% at admission to 61% at discharge. Follow-up demonstrates sustained cardiac function comparable to discharge status.
CONCLUSION
Entrectinib demonstrates potential cardiotoxicity in lung adenocarcinoma therapy, necessitating prospective studies to quantify this risk. During treatment, multidisciplinary team (MDT) collaboration is essential for rigorous cardiac function surveillance. This case establishes V-A ECMO with IABP as an effective salvage therapy for drug-induced fulminant myocarditis.
背景
恩曲替尼是一种最近获批用于治疗晚期ROS1阳性非小细胞肺癌(NSCLC)的多激酶抑制剂,已在转移性疾病中显示出显著的生存获益。然而,它存在严重心脏毒性风险。我们报告了使用静脉-动脉体外膜肺氧合(V-A ECMO)和主动脉内球囊泵(IABP)循环支持成功治疗恩曲替尼诱发的暴发性心肌炎的病例。
病例摘要
一名71岁男性,三年前被诊断为肺腺癌(基因检测为ROS1阳性),开始使用克唑替尼治疗。入院前一周,胸部计算机断层扫描(CT)监测显示疾病进展,肿瘤负荷增加,促使其改用恩曲替尼。治疗开始7天后,他因急性发作的心悸、呼吸困难、头晕和恶心就诊于我院急诊科。急诊冠状动脉造影排除了严重狭窄。患者随后出现频发室性早搏(VPC)、心源性休克(血清乳酸2.6 mmol/L)和急性心力衰竭。无心脏病史且病毒血清学阴性支持药物性暴发性心肌炎的诊断。紧急实施了V-A ECMO联合IABP支持。随后出现显著恢复:第3天心脏功能恢复正常(ECMO撤管),第5天拔管并移除IABP。住院12天后,患者出院。射血分数(EF)从入院时的10%恢复至出院时的61%。随访显示心脏功能持续维持在与出院时相当的水平。
结论
恩曲替尼在肺腺癌治疗中显示出潜在的心脏毒性,需要进行前瞻性研究以量化这种风险。在治疗期间,多学科团队(MDT)协作对于严格监测心脏功能至关重要。本病例证实V-A ECMO联合IABP是药物性暴发性心肌炎的有效挽救治疗方法。
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