Canter Robert J, Borys Dariusz, Olusanya Abimbola, Li Chin-Shang, Lee Li-Yuan, Boutin Robert D, Christensen Scott D, Tamurian Robert M, Monjazeb Arta M
Division of Surgical Oncology, UC Davis Comprehensive Cancer Center, University of California Davis Medical Center, Sacramento, CA, USA,
Ann Surg Oncol. 2014 May;21(5):1616-23. doi: 10.1245/s10434-014-3543-7. Epub 2014 Feb 20.
Despite effective local therapy with surgery and radiotherapy (RT), ~50 % of patients with high-grade soft tissue sarcoma (STS) will relapse and die of disease. Since experimental data suggest a significant synergistic effect when antiangiogenic targeted therapies such as sorafenib are combined with RT, we chose to evaluate preoperative combined modality sorafenib and conformal RT in a phase I/II trial among patients with extremity STS amenable to treatment with curative intent.
For the phase I trial, eight patients with intermediate- or high-grade STS >5 cm in maximal dimension or low-grade STS >8 cm in maximal dimension received concomitant sorafenib (dose escalation cohort 1:200 twice daily, cohort 2:200/400 daily) and preoperative RT (50 Gy in 25 fractions). Sorafenib was continued during the entire period of RT as tolerated. Surgical resection was completed 4-6 weeks following completion of neoadjuvant sorafenib/RT. Three sorafenib dose levels were planned. Primary endpoints of the phase I trial were maximal tolerated dose and dose-limiting toxicity (DLT).
Eight patients were enrolled in the phase I (five females, median age 44 years, two high-grade pleomorphic, two myxoid/round cell liposarcoma, four other). Median tumor size was 16 cm (range 8-29), and all tumors were located in the lower extremity. Two of five patients treated at dose level 2 developed DLT consisting of grade 3 rash not tolerating drug reintroduction. Other grade 3 side effects included anemia, perirectal abscess, and supraventricular tachycardia. Radiation toxicity (grade 1 or 2 dermatitis; N = 8) and post-surgical complications (three grade 3 wound complications) were comparable to historical controls and other series of preoperative RT monotherapy. Complete pathologic reponse (≥95 % tumor necrosis) was observed in three patients (38 %).
Neoadjuvant sorafenib in combination with RT is tolerable and appears to demonstrate activity in locally advanced extremity STS. Further study to determine efficacy at dose level 1 is warranted. (ClinicalTrials.gov identifier NCT00805727).
尽管采用手术和放疗(RT)进行局部治疗有效,但约50%的高级别软组织肉瘤(STS)患者会复发并死于该疾病。由于实验数据表明,索拉非尼等抗血管生成靶向疗法与放疗联合使用时具有显著的协同效应,我们选择在一项I/II期试验中评估术前联合使用索拉非尼和适形放疗,该试验针对有治愈意向且适合治疗的肢体STS患者。
在I期试验中,8例最大直径>5 cm的中高级别STS患者或最大直径>8 cm的低级别STS患者接受索拉非尼(剂量递增队列1:每日2次,每次200 mg;队列2:每日200/400 mg)与术前放疗(25次分割,共50 Gy)联合治疗。在耐受的情况下,放疗期间持续使用索拉非尼。新辅助索拉非尼/放疗完成后4 - 6周进行手术切除。计划了三个索拉非尼剂量水平。I期试验的主要终点是最大耐受剂量和剂量限制毒性(DLT)。
8例患者入组I期试验(5例女性,中位年龄44岁,2例高级别多形性,2例黏液样/圆形细胞脂肪肉瘤,4例其他类型)。肿瘤中位大小为16 cm(范围8 - 29 cm),所有肿瘤均位于下肢。在剂量水平2治疗的5例患者中有2例出现DLT,表现为3级皮疹,无法耐受重新引入药物。其他3级副作用包括贫血、直肠周围脓肿和室上性心动过速。放疗毒性(1或2级皮炎;N = 8)和术后并发症(3例3级伤口并发症)与历史对照及其他术前单纯放疗系列相当。3例患者(38%)观察到完全病理缓解(≥95%肿瘤坏死)。
新辅助索拉非尼联合放疗是可耐受的,并且在局部晚期肢体STS中似乎显示出活性。有必要进一步研究确定剂量水平1时的疗效。(ClinicalTrials.gov标识符NCT00805727)