术前卡培他滨/奥沙利铂和西妥昔单抗联合放化疗治疗直肠癌:前瞻性 1/2 期研究的长期结果。
Preoperative chemoradiation therapy with capecitabine/oxaliplatin and cetuximab in rectal cancer: long-term results of a prospective phase 1/2 study.
机构信息
Department of Radiation Therapy and Oncology, University of Frankfurt, Germany.
出版信息
Int J Radiat Oncol Biol Phys. 2013 Dec 1;87(5):992-9. doi: 10.1016/j.ijrobp.2013.09.011. Epub 2013 Oct 24.
PURPOSE
We have previously shown that the addition of cetuximab to chemoradiation therapy failed to improve complete response rates (pCR) in rectal cancer. Here we report the long-term results of the cetuximab added to preoperative radiation therapy with capecitabine and oxaliplatin (CET-CAPOX-RT) phase 1/2 study that evaluated preoperative chemoradiation with cetuximab, capecitabine, and oxaliplatin in patients with rectal cancer.
METHODS AND MATERIALS
The median follow-up was 63 months (range, 5-73 months). Sixty patients were enrolled; 3 patients were excluded due to protocol violation, and 4 died before surgery. Total mesorectal excision was performed in 53 patients, in 85% (n=45) with curative intention (M0-status). Secondary end points including overall survival (OS) disease-free survival (DFS) and cancer-specific survival (CSS) were calculated. The prognostic value of KRAS mutation status was also assessed.
RESULTS
Histopathological examination confirmed ypUICC stages 0 (n=4; pCR), I (n=17), II (n=10), III (n=14), and IV (n=8). For patients who underwent surgery (n=53), OS at 1, 3, and 5 years was 88.7%, 83%, and 75.5%, respectively, whereas CSS rates were 94.1%, 88.1%, and 78.1%, respectively. In the 45 patients who were treated with curative intent (M0), the OS rates at 1, 3, and 5 years were 91.1%, 88.9%, and 86.7%, respectively; whereas CSS rates were 97.6%, 95.2%, and 90.3%, respectively; and DFS rates were 90.7%, 88.3%, and 88.3%, respectively. We did not find any locoregional failure in patients with M0-status (n=45). Chronic toxicity was rare. KRAS mutations, as detected in 33.3%, showed no correlation with the clinicopathological parameters nor significance for either OS (P=.112), CSS (P=.264), or DFS (P=.565).
CONCLUSIONS
Taken together, chemoradiation therapy combined with cetuximab is safe, feasible, and offers excellent survival rates. KRAS mutation status was not a predictive factor. Importantly, lack of improvement in pCR rate did not translate to poor survival in our clinical trial.
目的
我们之前的研究表明,在直肠癌中,西妥昔单抗联合放化疗未能提高完全缓解率(pCR)。在此,我们报告了西妥昔单抗联合卡培他滨和奥沙利铂术前放疗(CET-CAPOX-RT)的 1/2 期研究的长期结果,该研究评估了西妥昔单抗、卡培他滨和奥沙利铂联合术前放化疗治疗直肠癌患者。
方法和材料
中位随访时间为 63 个月(范围,5-73 个月)。共纳入 60 例患者,3 例因违反方案被排除,4 例在术前死亡。53 例患者行全直肠系膜切除术,其中 85%(n=45)为根治性(M0 状态)。计算总生存(OS)、无病生存(DFS)和癌症特异性生存(CSS)等次要终点。还评估了 KRAS 突变状态的预后价值。
结果
组织病理学检查证实 ypUICC 分期为 0 期(n=4;pCR)、Ⅰ期(n=17)、Ⅱ期(n=10)、Ⅲ期(n=14)和Ⅳ期(n=8)。对于接受手术的患者(n=53),1、3 和 5 年的 OS 分别为 88.7%、83%和 75.5%,CSS 率分别为 94.1%、88.1%和 78.1%。在 45 例根治性治疗(M0)的患者中,1、3 和 5 年的 OS 率分别为 91.1%、88.9%和 86.7%;CSS 率分别为 97.6%、95.2%和 90.3%;DFS 率分别为 90.7%、88.3%和 88.3%。我们在 M0 状态(n=45)的患者中未发现局部区域复发。慢性毒性罕见。KRAS 突变在 33.3%的患者中被检测到,但与临床病理参数无关,对 OS(P=.112)、CSS(P=.264)或 DFS(P=.565)均无意义。
结论
联合放化疗的西妥昔单抗治疗安全可行,生存率高。KRAS 突变状态不是预测因素。重要的是,我们的临床试验中 pCR 率的提高并未转化为生存不良。
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