Third Faculty of Medicine, Charles University and University Hospital Kralovske Vinohrady, Prague, Czech Republic.
First Faculty of Medicine, Charles University and General University Hospital in Prague, Prague, Czech Republic.
J Immunother Cancer. 2022 Jan;10(1). doi: 10.1136/jitc-2021-003190.
Most patients with epithelial ovarian cancer (EOC) relapse despite primary debulking surgery and chemotherapy (CT). Autologous dendritic cell immunotherapy (DCVAC) can present tumor antigens to elicit a durable immune response. We hypothesized that adding parallel or sequential DCVAC to CT stimulates antitumor immunity and improves clinical outcomes in patients with EOC. Based on the interim results of sequential DCVAC/OvCa administration and to accommodate the increased interest in maintenance treatment in EOC, the trial was amended by adding Part 2.
Patients with International Federation of Gynecology and Obstetrics stage III EOC (serous, endometrioid, or mucinous), who underwent cytoreductive surgery up to 3 weeks prior to randomization and were scheduled for first-line platinum-based CT were eligible. Patients, stratified by tumor residuum (0 or <1 cm), were randomized (1:1:1) to DCVAC/OvCa parallel to CT (Group A), DCVAC/OvCa sequential to CT (Group B), or CT alone (Group C) in Part 1, and to Groups B and C in Part 2. Autologous dendritic cells for DCVAC were differentiated from patients' CD14 monocytes, pulsed with two allogenic OvCa cell lines (SK-OV-3, OV-90), and matured in the presence of polyinosinic:polycytidylic acid. We report the safety outcomes (safety analysis set, Parts 1 and 2 combined) along with the primary (progression-free survival (PFS)) and secondary (overall survival (OS)) efficacy endpoints. Efficacy endpoints were assessed in the modified intention-to-treat (mITT) analysis set in Part 1.
Between November 2013 and March 2016, 99 patients were randomized. The mITT (Part 1) comprised 31, 29, and 30 patients in Groups A, B, and C, respectively. Baseline characteristics and DCVAC/OvCa exposure were comparable across the treatment arms. DCVAC/OvCa showed a good safety profile with treatment-emergent adverse events related to DCVAC/OvCa in 2 of 34 patients (5.9%) in Group A and 2 of 53 patients (3.8%) in Group B. Median PFS was 20.3, not reached, and 21.4 months in Groups A, B, and C, respectively. The HR (95% CI) for Group A versus Group C was 0.98 (0.48 to 2.00; p=0.9483) and the HR for Group B versus Group C was 0.39 (0.16 to 0.96; p=0.0336). This was accompanied by a non-significant trend of improved OS in Groups A and B. Median OS was not reached in any group after a median follow-up of 66 months (34% of events).
DCVAC/OvCa and leukapheresis was not associated with significant safety concerns in this trial. DCVAC/OvCa sequential to CT was associated with a statistically significant improvement in PFS in patients undergoing first-line treatment of EOC.
NCT02107937, EudraCT2010-021462-30.
尽管进行了原发性减瘤手术和化疗(CT),大多数上皮性卵巢癌(EOC)患者仍会复发。自体树突状细胞免疫疗法(DCVAC)可以呈现肿瘤抗原,引发持久的免疫反应。我们假设,在 CT 中添加平行或序贯的 DCVAC 可以刺激抗肿瘤免疫并改善 EOC 患者的临床结局。基于序贯 DCVAC/OvCa 给药的中期结果,并为适应 EOC 中维持治疗的兴趣增加,试验通过添加第 2 部分进行了修订。
符合国际妇产科联合会(FIGO)III 期 EOC(浆液性、子宫内膜样或黏液性)标准、在随机分组前 3 周内接受细胞减灭术且计划接受一线铂类 CT 的患者有资格参加。根据肿瘤残留(0 或 <1cm)对患者进行分层,将患者随机分为 1:1:1 比例的三组,即 DCVAC/OvCa 与 CT 平行组(A 组)、DCVAC/OvCa 序贯 CT 组(B 组)和 CT 单一组(C 组),第 2 部分中,B 组和 C 组分别进行 DCVAC/OvCa 治疗。用于 DCVAC 的自体树突状细胞从患者的 CD14 单核细胞中分化而来,用两种异体 OvCa 细胞系(SK-OV-3、OV-90)进行脉冲处理,并在聚肌苷酸:聚胞苷酸存在的情况下成熟。我们报告了安全性结果(第 1 部分和第 2 部分的安全性分析集)以及主要(无进展生存期(PFS))和次要(总生存期(OS))疗效终点。第 1 部分的修改意向治疗(mITT)分析集中评估了疗效终点。
2013 年 11 月至 2016 年 3 月期间,共 99 名患者被随机分组。mITT(第 1 部分)中,A、B 和 C 组分别有 31、29 和 30 名患者。各组的基线特征和 DCVAC/OvCa 暴露情况相似。DCVAC/OvCa 表现出良好的安全性特征,A 组中有 2 名(5.9%)患者和 B 组中有 2 名(3.8%)患者出现与 DCVAC/OvCa 相关的治疗后不良事件。A、B 和 C 组的中位 PFS 分别为 20.3、未达到和 21.4 个月。A 组与 C 组的 HR(95%CI)为 0.98(0.48 至 2.00;p=0.9483),B 组与 C 组的 HR 为 0.39(0.16 至 0.96;p=0.0336)。这伴随着 A 组和 B 组 OS 改善的非显著趋势。中位随访 66 个月后,任何一组的中位 OS 均未达到(34%的事件)。
在这项试验中,DCVAC/OvCa 和白细胞分离术与明显的安全性问题无关。在接受 EOC 一线治疗的患者中,DCVAC/OvCa 序贯 CT 与 PFS 的统计学显著改善相关。
NCT02107937,EudraCT2010-021462-30。
