一项针对 III 期黑色素瘤伴 BRAF、NRAS 和 KIT 突变患者的辅助性抗 PD-1 免疫治疗的真实世界研究。
A real-world study of adjuvant anti-PD -1 immunotherapy on stage III melanoma with BRAF, NRAS, and KIT mutations.
机构信息
Department of Musculoskeletal Surgery, Fudan University Shanghai Cancer Center; Department of Oncology, Shanghai Medical College, Fudan University, Shanghai, China.
Department of gastrointestinal medical oncology, Fudan University Shanghai Cancer Center; Department of Oncology, Shanghai Medical College, Fudan University, Shanghai, China.
出版信息
Cancer Med. 2023 Aug;12(15):15945-15954. doi: 10.1002/cam4.6234. Epub 2023 Jul 5.
BACKGROUND
Melanoma frequently harbors BRAF, NRAS, or KIT mutations which influence both tumor development and treatment strategies. For example, it is still controversial whether adjuvant anti-PD-1 monotherapy or BRAF/MEK inhibitors may better improve the survival for resected BRAF-mutant melanoma. Furthermore, outcomes for melanoma with NRAS and KIT mutation receiving adjuvant immunotherapy remain unclear.
METHODS
One hundred seventy-four stage III melanoma patients who underwent radical surgery in Fudan University Shanghai Cancer Center (FUSCC) during January 2017 to December 2021 were included in this real-world study. Patients were followed up until death or May 30th, 2022. Pearson's chi-squared test or Fisher's exact test was performed for univariable analysis of the different category groups. Log-rank analysis was used to identify the prognostic factors for disease-free survival (DFS).
RESULTS
There were 41 (23.6%) patients with BRAF mutation, 31 (17.8%) with NRAS mutation, 17 (9.8%) with KIT mutation, and 85 (48.9%) wild-type patients without either genomic alteration of those three genes. Most ( n = 118, 67.8%) of them were acral melanoma, while 45 (25.9%) were cutaneous subtype, and 11 were (6.3%) primary unknown. Among them, 115 (66.1%) patients received pembrolizumab or toripalimab monotherapy as adjuvant therapy; 22 (12.6%) patients received high-dose interferon (IFN), and 37 (21.3%) patients were just for observation. There was no statistical difference in clinicopathologic factors between anti-PD-1 group and IFN/OBS group. Of all the enrolled patients, anti-PD-1 group had a better DFS than IFN/OBS group ( p = 0.039). In anti-PD-1 group, patients with BRAF or NRAS mutations had poorer DFS than wild-type group. No survival difference was found among patients harboring different gene mutations in IFN/OBS group. In wild-type patients, anti-PD-1 group had a better DFS than IFN/OBS group ( p = 0.003), while no survival benefits were found for patients with BRAF, NRAS, or KIT mutations.
CONCLUSION
Although anti-PD-1 adjuvant therapy provides a better DFS in the general population and in wild-type patients, patients with BRAF, KIT or, especially, NRAS mutation may not benefit further from immunotherapy than conventional IFN treatment or observation.
背景
黑色素瘤常携带 BRAF、NRAS 或 KIT 突变,这些突变既影响肿瘤的发生发展,也影响治疗策略。例如,对于接受手术切除的 BRAF 突变型黑色素瘤患者,辅助抗 PD-1 单药治疗或 BRAF/MEK 抑制剂治疗是否能更好地改善患者的生存仍然存在争议。此外,NRAS 和 KIT 突变的黑色素瘤患者接受辅助免疫治疗的结局仍不清楚。
方法
本研究为真实世界研究,共纳入 2017 年 1 月至 2021 年 12 月期间在复旦大学附属肿瘤医院接受根治性手术的 174 例 III 期黑色素瘤患者。患者随访至死亡或 2022 年 5 月 30 日。采用 Pearson 卡方检验或 Fisher 确切概率法进行单因素分析。采用对数秩检验分析无病生存(DFS)的预后因素。
结果
41 例(23.6%)患者存在 BRAF 突变,31 例(17.8%)存在 NRAS 突变,17 例(9.8%)存在 KIT 突变,85 例(48.9%)为野生型患者,未发现这三种基因的任何一种基因改变。大多数患者(n=118,67.8%)为肢端黑色素瘤,45 例(25.9%)为皮肤亚型,11 例(6.3%)为原发灶不明。其中,115 例(66.1%)患者接受了 pembrolizumab 或 toripalimab 单药作为辅助治疗;22 例(12.6%)患者接受了高剂量干扰素(IFN)治疗,37 例(21.3%)患者仅接受观察。抗 PD-1 组与 IFN/OBS 组在临床病理特征方面无统计学差异。所有入组患者中,抗 PD-1 组的 DFS 优于 IFN/OBS 组(p=0.039)。在抗 PD-1 组中,BRAF 或 NRAS 突变患者的 DFS 较野生型组差。IFN/OBS 组中不同基因突变患者的生存无差异。在野生型患者中,抗 PD-1 组的 DFS 优于 IFN/OBS 组(p=0.003),而 BRAF、NRAS 或 KIT 突变患者未从免疫治疗中获益。
结论
尽管抗 PD-1 辅助治疗在总体人群和野生型患者中提供了更好的 DFS,但 BRAF、KIT 或特别是 NRAS 突变患者可能不会从免疫治疗中获益,反而可能不如常规 IFN 治疗或观察。
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