Yanmei Peng, Dong Li, Jason A Wampfler, Yung-Hung Luo, Ashok V Kumar, Zhong Gu, Nikhila Kosuru, Nathan Y Yu, Zhichao Wang, Konstantinos Leventakos, Vinicius Ernani, Ping Yang
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In the prospectively followed 3,767 patients with stage‑IV NSCLC, 701 received targeted therapy; of which 133 (19.0%) had cardiac comorbidity, 504 (71.9%) had other comorbidities and 64 (9.1%) had none. In total, 15 patients (2.1%) developed cardiotoxicity after taking drugs targeting epidermal growth factor receptor, anaplastic lymphoma kinase (<i>ALK</i>), c‑ros oncogene 1 (<i>ROS1</i>) or vascular endothelial growth factor/receptor (<i>VEGF</i>)/<i>VEGFR</i>, and all 15 had comorbidities: 10 cardiac and 5 other comorbidities. Cardiac comorbidity was associated with a 7.5‑fold higher risk of targeted therapy‑related cardiotoxicity than other comorbidities (7.5 vs. 1.0%; P<0.001). Patients with or without cardiotoxicity had a median survival time of 4.7 or 1.9 years, respectively, and patients with cardiotoxicity had a lower risk of death (hazard ratio, 0.45; 95% confidence interval, 0.25‑0.81) than those without (P=0.003), when adjusting for comorbidities. 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引用次数: 0
摘要
靶向药物已经彻底改变了晚期非小细胞肺癌(NSCLC)的治疗。然而,对心脏合并症和毒性如何影响靶向治疗后患者临床结果的理解仍然有限。在一项为期14年的队列研究中,确定了接受靶向治疗的IV期非小细胞肺癌患者的心脏合并症和毒性。比较三组患者的心脏毒性:心脏毒性、其他毒性和无合并症。生存分析采用Cox比例风险模型。在前瞻性随访的3767例IV期NSCLC患者中,701例接受了靶向治疗;其中133例(19.0%)有心脏合并症,504例(71.9%)有其他合并症,64例(9.1%)无合并症。总共有15例(2.1%)患者在服用靶向表皮生长因子受体、间变性淋巴瘤激酶(ALK)、c - ros癌基因1 (ROS1)或血管内皮生长因子/受体(VEGF)/VEGFR的药物后发生心脏毒性,且所有15例患者均有合并症:10例心脏合并症和5例其他合并症。心脏合并症与靶向治疗相关心脏毒性的风险比其他合并症高7.5倍(7.5 vs 1.0%;PALK/ROS1抑制剂的心脏毒性在心脏病患者中(30.0%)比无抑制剂的患者(2.1%)多14倍(P=0.001)。心脏毒性在靶向药物治疗的IV期非小细胞肺癌患者中并不常见,但在有心脏合并症的患者中更为普遍,似乎是延长生存期的保护因素。然而,在接受奥西替尼治疗的患者中,心脏合并症增加了死亡率。
Targeted therapy‑associated cardiotoxicity in patients with stage‑IV lung cancer with or without cardiac comorbidities.
Targeted drugs have revolutionized the treatment of advanced non‑small cell lung cancer (NSCLC). However, the understanding of how cardiac comorbidity and toxicity affect the clinical outcomes of patients following targeted therapy remains limited. In a 14‑year cohort, cardiac comorbidities and toxicities among patients with stage‑IV NSCLC treated with targeted therapy were identified. The cardiotoxicities were compared in three patient groups: Cardiac, other and no comorbidities. Survival analysis employed Cox Proportional Hazard Models. In the prospectively followed 3,767 patients with stage‑IV NSCLC, 701 received targeted therapy; of which 133 (19.0%) had cardiac comorbidity, 504 (71.9%) had other comorbidities and 64 (9.1%) had none. In total, 15 patients (2.1%) developed cardiotoxicity after taking drugs targeting epidermal growth factor receptor, anaplastic lymphoma kinase (ALK), c‑ros oncogene 1 (ROS1) or vascular endothelial growth factor/receptor (VEGF)/VEGFR, and all 15 had comorbidities: 10 cardiac and 5 other comorbidities. Cardiac comorbidity was associated with a 7.5‑fold higher risk of targeted therapy‑related cardiotoxicity than other comorbidities (7.5 vs. 1.0%; P<0.001). Patients with or without cardiotoxicity had a median survival time of 4.7 or 1.9 years, respectively, and patients with cardiotoxicity had a lower risk of death (hazard ratio, 0.45; 95% confidence interval, 0.25‑0.81) than those without (P=0.003), when adjusting for comorbidities. In the 164 patients that received osimertinib, 32 (19.5%) had cardiac comorbidity and a 1.7‑fold higher risk of death than the 121 (73.8%) patients with other comorbidities. In the 74 patients treated with ALK/ROS1 inhibitors, cardiotoxicity was 14 times more common in patients with heart disease (30.0%) than those without (2.1%) (P=0.001). Cardiotoxicity was uncommon in patients with targeted drug‑treated stage‑IV NSCLC but was more prevalent in those with cardiac comorbidity and appeared to be a protector for longer survival. However, in osimertinib‑treated patients, cardiac comorbidity increased mortality.
期刊介绍:
Oncology Reports is a monthly, peer-reviewed journal devoted to the publication of high quality original studies and reviews concerning a broad and comprehensive view of fundamental and applied research in oncology, focusing on carcinogenesis, metastasis and epidemiology.
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