手足皮肤反应随索拉非尼累积剂量以及联合抗血管内皮生长因子治疗而增加。
Hand-foot skin reaction increases with cumulative sorafenib dose and with combination anti-vascular endothelial growth factor therapy.
作者信息
Azad Nilofer S, Aragon-Ching Jeanny B, Dahut William L, Gutierrez Martin, Figg William D, Jain Lokesh, Steinberg Seth M, Turner Maria L, Kohn Elise C, Kong Heidi H
机构信息
Medical Oncology Branch, Biostatistics and Data Management Section, Center for Cancer Research, NIH, Bethesda, Maryland 20892, USA.
出版信息
Clin Cancer Res. 2009 Feb 15;15(4):1411-6. doi: 10.1158/1078-0432.CCR-08-1141.
PURPOSE
Sorafenib, a vascular endothelial growth factor (VEGF) receptor-2 and RAF kinase inhibitor, commonly causes skin toxicity. We retrospectively analyzed dermatologic toxicity in patients receiving combined antiangiogenic therapy involving sorafenib and bevacizumab.
EXPERIMENTAL DESIGN
Castration-resistant prostate cancer and metastatic non-small cell lung cancer patients were accrued to phase II studies, receiving sorafenib 400 mg twice daily. A phase I study explored sorafenib 200 to 400 mg twice daily with bevacizumab 5 to 10 mg/kg every 2 weeks in patients with advanced solid tumors. The probability of development of maximum grade of dermatologic toxicity as a function of the cumulative dose of sorafenib was determined. Additional analyses compared extent of toxicity, pharmacokinetics, and patient risk factors.
RESULTS
Ninety-six patients were enrolled: 54 received sorafenib and 42 received bevacizumab/sorafenib. Hand-foot skin reaction (HFSR) was observed in 50 of 96 (52%) patients. Grade 2 to 3 HFSR developed in 16 of 54 (30%) sorafenib patients and 24 of 42 (57%) bevacizumab/sorafenib patients (P=0.012) and was associated with cumulative sorafenib exposure (P=0.0008). Twenty-four of 42 phase I patients randomized to start with bevacizumab had increased risk of grade 2 to 3 HFSR than those starting with sorafenib (P=0.013) after adjusting for association between HFSR risk and hypertension (P=0.01), which was the only toxicity associated with HFSR. There was no association between HFSR and baseline history of neuropathy, prior taxane/platinum treatment, or systemic sorafenib levels.
CONCLUSIONS
Sorafenib-related HFSR is associated with increasing cumulative sorafenib dose. HFSR is increased in patients treated with bevacizumab/sorafenib combination anti-VEGF therapy, and this finding is not explained by pharmacokinetic interaction between the two agents. Our results suggest that the pathophysiology of HFSR may be related to VEGF inhibition.
目的
索拉非尼是一种血管内皮生长因子(VEGF)受体-2和RAF激酶抑制剂,常引起皮肤毒性。我们回顾性分析了接受索拉非尼和贝伐单抗联合抗血管生成治疗的患者的皮肤毒性。
实验设计
去势抵抗性前列腺癌和转移性非小细胞肺癌患者入组II期研究,接受索拉非尼每日两次,每次400mg。一项I期研究探索了晚期实体瘤患者每日两次服用索拉非尼200至400mg,每2周服用贝伐单抗5至10mg/kg的情况。确定了作为索拉非尼累积剂量函数的最大程度皮肤毒性发生的概率。额外的分析比较了毒性程度、药代动力学和患者风险因素。
结果
96名患者入组:54名接受索拉非尼治疗,42名接受贝伐单抗/索拉非尼治疗。96名患者中有50名(52%)观察到手足皮肤反应(HFSR)。54名索拉非尼治疗患者中有16名(30%)出现2至3级HFSR,42名贝伐单抗/索拉非尼治疗患者中有24名(57%)出现2至3级HFSR(P=0.012),且与索拉非尼累积暴露相关(P=0.0008)。在调整了HFSR风险与高血压之间的关联(P=0.01)后,42名随机开始使用贝伐单抗的I期患者中,2至3级HFSR的风险高于开始使用索拉非尼的患者(P=0.013),高血压是与HFSR相关的唯一毒性。HFSR与神经病变的基线病史、先前的紫杉烷/铂类治疗或全身索拉非尼水平之间无关联。
结论
索拉非尼相关的HFSR与索拉非尼累积剂量增加有关。接受贝伐单抗/索拉非尼联合抗VEGF治疗的患者中HFSR增加,这一发现无法用两种药物之间的药代动力学相互作用来解释。我们的结果表明,HFSR的病理生理学可能与VEGF抑制有关。
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