Background: Treatment with fluoropyrimidines and concomitant long-course external radiotherapy (RTE) is the standard of care in locally advanced rectal cancer (LARC) preoperative chemoradiation. A randomized phase II study (RaP/STAR-03) was conducted that aimed to evaluate the activity and safety of the monoclonal antibody anti-epidermal growth factor receptor panitumumab as a single agent in combination with radiotherapy in low-risk LARC preoperative treatment.
Materials and methods: Patients had adenocarcinoma of the mid-low rectum, cT3N- or cT2-T3N+, KRAS wild-type status, and negative circumferential radial margin. Panitumumab was administered concomitant to RTE. Rectal surgery was performed 6-8 weeks after the end of preoperative treatment. The adjuvant chemotherapy regimen was FOLFOX. The primary endpoint was the pathologic complete response (pCR) rate. The sample size was calculated using Simon's two-stage design. A pCR of 16% was considered to qualify the experimental treatment for further testing.
Results: Ninety-eight patients were enrolled in 13 Italian centers from October 2012 to October 2015. Three panitumumab infusions were administered in 92 (93.4%) patients. The RTE compliance was median dose 50.4 Gy; ≥28 fractions in 82 (83.7%) patients. Surgical treatment was performed in 92 (93.9%) patients, and no severe intraoperative complications were observed. A pCR was observed in 10 (10.9%) patients (95% confidence interval, 4.72%-17.07%). Pathological downstaging occurred in 45 (45.9%) patients. Grade 3 toxicities were observed in 22 (22.3%) patients, and the common adverse events were skin rash in 16 (16.3%) patients. No grade 4 toxicities were reported.
Conclusion: The pCR rate (our primary endpoint), at only 10.9%, did not reach the specified level considered suitable for further testing. However, the analysis showed a good toxicity profile and compliance to concomitant administration of panitumumab and RTE in preoperative treatment of LARC. The pCR evaluation in all wild-type RAS is ongoing.
Implications for practice: The aim of the RaP/STAR-03 study was to evaluate the activity and safety of monoclonal antibody anti-epidermal growth factor receptor (EGFR) panitumumab as a single agent without chemotherapy in low-risk, locally advanced rectal cancer (LARC) preoperative treatment. Nevertheless, the use of panitumumab in combination with radiotherapy in preoperative treatment in patients with KRAS wild type and low-risk LARC did not reach the pathologic complete response primary endpoint. This study showed a good toxicity profile and compliance to combination treatment. Further analysis of NRAS and BRAF on tissue and circulating levels of the EGFR ligands and vascular factors (soluble vascular endothelial growth factor, E-selectin) may provide insight on the potential molecular pathways involved in the anti-EGFR response.
摘要
背景.氟尿嘧啶同步长期外部放疗(RTE)治疗是局部晚期直肠癌(LARC)术前放化疗的标准。我们开展了一项随机II期研究(RaP/STAR‐03),旨在评估单克隆抗体抗表皮生长因子受体帕尼单抗作为单药联合放疗用于低风险LARC术前治疗的活性和安全性。
材料和方法.患者患有中低段直肠腺癌,cT3N−或cT2–T3N+,KRAS野生型状态,环周切缘为阴性。RTE同步帕尼单抗给药。在术前治疗结束后6–8周时进行直肠手术。辅助化疗方案为FOLFOX。主要终点是病理完全缓解(pCR)率。使用Simon两阶段设计计算样本量。16%的pCR可使实验治疗符合进一步检测的标准。
结果.在2012年10月至2015年10月期间,13个意大利中心入组了98例患者。在92例(93.4%)患者中进行了三次帕尼单抗输注。RTE依从性:中位剂量50.4 Gy,82例(83.7%)患者≥28次分割。在92例(93.9%)患者中进行了手术治疗,未观察到严重术中并发症。在10例(10.9%)患者中观察到pCR(95%置信区间,4.72%–17.07%)。45例(45.9%)患者发生病理学降期。在22例(22.3%)患者中观察到3级毒性,常见不良事件为皮疹,见于16(16.3%)例患者。未报告4级毒性。
结论.pCR率(我们的主要终点)仅为10.9%,未达到被视为适合进一步检测的规定水平。不过,该分析显示在LARC术前治疗中同步RTE和帕尼单抗治疗具有良好的毒性特征和依从性。正在针对所有野生型RAS进行pCR评价。
对临床实践的提示:RaP/STAR‐03研究的目的是评价单克隆抗体抗表皮生长因子受体(EGFR)帕尼单抗作为单药(不联合化疗)在低风险、局部晚期直肠癌(LARC)术前治疗中的活性和安全性。不过,在存在KRAS野生型、低风险LARC患者的术前治疗中帕尼单抗与放疗联用并未达到病理学完全缓解的主要终点。本研究显示联合治疗具有良好的毒性特征和依从性。对组织以及EGFR配体和血管因子(可溶性血管内皮生长因子,E‐选择素)循环水平进行的进一步NRAS和BRAF分析可能会提供有关涉及抗EGFR应答的潜在分子途径的见解。
Keywords: KRAS; Panitumumab; Radiotherapy; Rectal cancer.
© AlphaMed Press 2018.