抗血管生成酪氨酸激酶抑制剂的心血管毒性:一项回顾性药物警戒研究。
Cardiovascular Toxicities of Antiangiogenic Tyrosine Kinase Inhibitors: A Retrospective, Pharmacovigilance Study.
机构信息
Leviev Heart Center, Sheba Medical Center, Ramat Gan, Israel.
School of Medicine, Sackler Faculty of Medicine, Tel-Aviv University, Tel-Aviv, Israel.
出版信息
Target Oncol. 2021 Jul;16(4):471-483. doi: 10.1007/s11523-021-00817-2. Epub 2021 May 10.
BACKGROUND
Vascular endothelial growth factor receptor (VEGFR) tyrosine kinase inhibitors (TKIs) are an essential therapeutic option in the management of various solid tumors, particularly renal cell carcinoma (RCC). However, post-marketing data regarding their potential cardiovascular toxicities are scant.
OBJECTIVE
To identify and characterize cardiovascular adverse events (CVAEs) of VEGFR-TKIs indicated for RCC.
PATIENTS AND METHODS
Disproportionality analysis of the US Food and Drug Administration adverse event reporting system (July 2014-December 2019) using the reporting odds ratio (ROR) and the lower bound of the Information component (IC) 95% credibility interval (IC > 0 is significant).
RESULTS
We identified 51,836 adverse event reports of sunitinib, pazopanib, axitinib, cabozantinib, and lenvatinib in the full database [36% women; median age 65 years (range 57-73)]. CVAEs accounted for 11,784 (23%) of the reports, with hypertension [n = 5548 (11%), ROR = 6.55 (95% CI 6.37-6.74), IC = 2.48] and hemorrhages [n = 3710 (7.2%), ROR = 1.28 (1.24-1.32), IC = 0.28] being the most frequent types. Additional CVAEs were over-reported with VEGFR-TKIs treatment, including aortic dissection [n = 61 (0.1%), ROR = 3.50 (2.71-4.51)], pericardial diseases [n = 173 (0.3%), ROR = 1.98 (1.70-2.30)], cardiomyopathy [n = 61 (0.1%), ROR = 1.89 (1.47-2.43)], heart failure [n = 868 (1.7%), ROR = 1.35 (1.26-1.44)], and venous thromboembolism [n = 604 (1.2%), ROR = 1.33 (1.23-1.45), all IC > 0]. The major pericardial disorder was non-malignant pericardial effusion [n = 134 (77%)]. Aortic dissections were also over-reported in patients without concomitant elevated blood pressure [ROR = 2.68 (1.97-3.63), IC = 0.91]. Finally, CVAEs were reported more often following lenvatinib and sunitinib treatment compared to other VEGFR-TKIs.
CONCLUSIONS
In post-marketing surveillance data, VEGFR-TKIs are associated with increased reporting of various CVAEs, including pericardial diseases, particularly non-malignant pericardial effusion, and aortic dissections. Moreover, VEGFR-TKIs differ in their CVAE reporting patterns. Clinicians should be conscious of these findings in the care of VEGFR-TKIs recipients.
背景
血管内皮生长因子受体(VEGFR)酪氨酸激酶抑制剂(TKI)是治疗各种实体瘤(尤其是肾细胞癌[RCC])的重要治疗选择。然而,关于其潜在心血管毒性的上市后数据很少。
目的
确定并描述用于治疗 RCC 的 VEGFR-TKI 的心血管不良事件(CVAEs)。
患者和方法
使用报告比值比(ROR)和信息分量(IC)下限 95%置信区间(IC > 0 为显著)对美国食品和药物管理局不良事件报告系统(2014 年 7 月至 2019 年 12 月)的上市后数据进行不匹配分析。
结果
我们在完整数据库中确定了 51836 例舒尼替尼、帕唑帕尼、阿西替尼、卡博替尼和仑伐替尼的不良事件报告[36%为女性;中位年龄 65 岁(范围 57-73)]。CVAEs 占报告的 11784 例(23%),其中高血压[n = 5548(11%),ROR = 6.55(95%CI 6.37-6.74),IC = 2.48]和出血[n = 3710(7.2%),ROR = 1.28(1.24-1.32),IC = 0.28]是最常见的类型。VEGFR-TKI 治疗后还过度报告了其他 CVAEs,包括主动脉夹层[n = 61(0.1%),ROR = 3.50(2.71-4.51)]、心包疾病[n = 173(0.3%),ROR = 1.98(1.70-2.30)]、心肌病[n = 61(0.1%),ROR = 1.89(1.47-2.43)]、心力衰竭[n = 868(1.7%),ROR = 1.35(1.26-1.44)]和静脉血栓栓塞[n = 604(1.2%),ROR = 1.33(1.23-1.45)],所有 IC > 0]。主要心包疾病为非恶性心包积液[n = 134(77%)]。在没有同时伴有高血压的患者中,主动脉夹层的报告也过多[ROR = 2.68(1.97-3.63),IC = 0.91]。最后,与其他 VEGFR-TKIs 相比,仑伐替尼和舒尼替尼治疗后 CVAEs 的报告更为常见。
结论
在上市后监测数据中,VEGFR-TKI 与各种 CVAEs 的报告增加有关,包括心包疾病,特别是非恶性心包积液和主动脉夹层。此外,VEGFR-TKI 在其 CVAE 报告模式上存在差异。临床医生在接受 VEGFR-TKI 治疗的患者护理中应注意这些发现。
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