Jakob Jens, Simeonova Anna, Kasper Bernd, Ronellenfitsch Ulrich, Rauch Geraldine, Wenz Frederik, Hohenberger Peter
Division of Surgical, Oncology and Thoracic Surgery, Department of Surgery, University Medical Center and Medical Faculty Mannheim, University of Heidelberg, Th.-Kutzer-Ufer 1-3, Mannheim, 68137, Germany.
Department of Radiation Oncology, University Medical Center Mannheim, University of Heidelberg, Th.-Kutzer-ufer 1-3, Mannheim, 68137, Germany.
Radiat Oncol. 2016 Jun 3;11:77. doi: 10.1186/s13014-016-0654-2.
Experimental data demonstrated that concurrent anti-angiogenic treatment with sunitinib may improve the efficacy of radiation therapy (RT). Here we report the results of a phase I trial performed within the German Interdisciplinary Sarcoma Group (GISG-03) of combined sunitinib and RT for neoadjuvant treatment of locally advanced soft tissue sarcoma (STS).
The primary endpoint of the study was to explore the recommended dose of sunitinib combined with RT for subsequent trials. Treatment response, postoperative complications after tumor resection and toxicity according to CTCAE 4.0 were secondary endpoints. The study used a 3 + 3 design. Patients received either 25 mg (dose level 1) or 37.5 mg (dose level 2) sunitinib two weeks prior to and throughout RT (28 × 1.8 Gy). Surgery was scheduled 5-8 weeks after completion of neoadjuvant treatment.
NCT01498835.
Six patients were enrolled in dose level 1 and three patients in dose level 2. Median tumor size was 11 cm. Tumors were located in the retroperitoneum (4/9), lower leg (3/9) or trunk (2/9). At dose level 1, 1/6 patients developed dose limiting lymphopenia. At dose level 2, no patient developed dose limiting toxicity. Most frequent toxicities were hematological (8/9) and oral (5/9). Dose adjustments of sunitinib were necessary in 5/9 patients. All patients received full dose RT and underwent tumor resection (8/9 R0 and 1/9 R1). Local toxicity of RT did not exceed Grade 2. 2/9 patients had postoperative complications requiring re-intervention. Treatment response according to RECIST was as follows: partial response 1/9, stable disease 7/9, and progressive disease 1/9. Pathological examination revealed ≥ 95 % tumor necrosis in 3/9 resected specimens.
Combined sunitinib and RT was tolerable as neoadjuvant treatment for locally advanced STS patients regardless of tumor localization. The recommended sunitinib dose for subsequent trials is 37.5 mg.
实验数据表明,舒尼替尼联合抗血管生成治疗可能会提高放射治疗(RT)的疗效。在此,我们报告德国跨学科肉瘤组(GISG-03)开展的一项I期试验结果,该试验采用舒尼替尼联合放疗对局部晚期软组织肉瘤(STS)进行新辅助治疗。
本研究的主要终点是探索舒尼替尼联合放疗用于后续试验的推荐剂量。根据CTCAE 4.0评估治疗反应、肿瘤切除术后的并发症及毒性作为次要终点。本研究采用3+3设计。患者在放疗前两周及整个放疗期间(28×1.8 Gy)接受25 mg(剂量水平1)或37.5 mg(剂量水平2)的舒尼替尼治疗。新辅助治疗结束后5-8周安排手术。
NCT01498835。
6例患者入组剂量水平1,3例患者入组剂量水平2。肿瘤中位大小为11 cm。肿瘤位于腹膜后(4/9)、小腿(3/9)或躯干(2/9)。在剂量水平1,1/6的患者出现剂量限制性淋巴细胞减少。在剂量水平2,无患者出现剂量限制性毒性。最常见的毒性反应为血液学毒性(8/9)和口腔毒性(5/9)。9例患者中有5例需要调整舒尼替尼剂量。所有患者均接受了全剂量放疗并接受了肿瘤切除术(8/9为R0切除,1/9为R1切除)。放疗的局部毒性未超过2级。9例患者中有2例术后出现并发症需要再次干预。根据RECIST标准评估的治疗反应如下:部分缓解1/9,病情稳定7/9,疾病进展1/9。病理检查显示,9例切除标本中有3例肿瘤坏死≥95%。
舒尼替尼联合放疗作为局部晚期STS患者的新辅助治疗是可耐受的,与肿瘤部位无关。后续试验推荐的舒尼替尼剂量为37.5 mg。