多激酶抑制剂帕唑帕尼或lenvatinib治疗血栓栓塞危险因素的探索性回顾性研究

K. Nio, K. Tsuchihashi, K. Taguchi, Tomoyasu Yoshihiro, K. Yamaguchi, Mamoru Ito, Shohei Moriyama, Mitsuhiro Fukata, T. Fujiwara, Nokitaka Setsu, M. Endo, Y. Matsumoto, Y. Nakashima, T. Wakasaki, R. Yasumatsu, H. Ariyama, H. Kusaba, J. Kishimoto, K. Akashi, E. Baba
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引用次数: 0

摘要

酪氨酸激酶抑制剂(TKI)通过抑制血管生成信号来对抗各种类型的癌症。在常规临床实践中,对TKI引起的血栓栓塞的发生率、特征和危险因素了解甚少。我们回顾性分析了29例接受lenvatinib (n=10)和pazopanib (n=19)治疗的甲状腺癌或软组织肉瘤(STS)患者的数据。8例(动脉n=4;6例(20%)患者发生静脉血栓栓塞事件。血栓栓塞发生的平均时间为TKI开始后149天(范围42-847天)。所有血栓栓塞患者的原发疾病均有进展。血栓栓塞改善患者和未改善患者的总生存时间分别为572[95%可信区间(CI), 225 - 918]和176 (95% CI, 84-394)天,差异无统计学意义(P=0.33)。有和没有改善的血栓栓塞患者在发病后存活122天(95% CI, 71-173)和27天(95% CI, 21-42) (P=0.049),差异有统计学意义。单因素分析和多因素分析的多因素选择选择血栓栓塞史作为新血栓栓塞的最强大的危险因素。综上所述,临床实践中血栓栓塞的发生频率高于以往的临床试验。此外,血栓栓塞史是TKI治疗患者发生新血栓栓塞的危险因素。血栓栓塞尤其随着原发疾病的进展而发展。我们的发现需要大规模研究的验证。
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Exploratory retrospective study of risk factors for thromboembolism treated with multi-kinase inhibitor pazopanib or lenvatinib
Tyrosine kinase inhibitors (TKI) work against various types of cancer by inhibiting angiogenic signaling. Little is understood about the incidence, characteristics, and risk factors associated with thromboembolism induced by TKI in routine clinical practice. We retrospectively analyzed data derived from 29 patients with thyroid cancer or soft tissue sarcoma (STS) treated with lenvatinib (n=10) and pazopanib (n=19). Eight (arterial n=4; venous n=4) thromboembolic events developed in 6 (20%) patients. Thromboembolisms occurred during a mean of 149 (range, 42–847) days from starting TKI. The primary disease progressed in all patients with thromboembolism. The overall survival durations of patients with and without improved thromboembolism were 572 [95% confidence interval (CI), 225– 918] and 176 (95% CI, 84–394) days, respectively, which did not significantly differ (P=0.33). Patients with and without improved thromboembolism survived after onset for 122 (95% CI, 71–173) versus 27 (95% CI, 21–42) days (P=0.049), which significantly differed. Univariate analysis and variate selection for multivariate analysis selected a history of thromboembolism as the most powerful risk factor for new thromboembolism. In summary, the frequency of thromboembolism in clinical practice was higher than that in previous clinical trials. Furthermore, a history of thromboembolism was a risk factor for the development of new thromboembolism in patients treated with TKI. Thromboembolism developed particularly as the primary disease progressed. Our findings require validation in a large-scale study.
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