Center for Personalized Diagnostics, School of Life Sciences, Biodesign Institute, Arizona State University, PO Box 876401, Tempe, AZ, 85287-6401, USA.
Department of Medical Oncology, Mayo Clinic, Scottsdale, AZ, USA.
Breast Cancer Res Treat. 2022 Jul;194(1):65-78. doi: 10.1007/s10549-022-06562-y. Epub 2022 Apr 28.
The antigenic targets of immunity and the role of vaccination in breast cancer are unknown. We performed a phase I study of an autologous GM-CSF-secreting breast cancer vaccine in patients with metastatic and stage II-III breast cancer.
Tumor cells from patients with metastatic (n = 15) and stage II-III (n = 7) disease were transduced with a replication-defective adenoviral vector encoding GM-CSF, and then irradiated. Twelve and seven patients with metastatic and stage II-III disease, respectively, received weekly vaccination for three weeks, followed by every other week until disease progression or vaccine supply was exhausted (metastatic) or until six total vaccine doses were administered (stage II-III).
Among those patients with metastatic disease who received vaccinations, eight had progressive disease at two months, three had stable disease for 4-13 months, and one has had no evidence of disease for 13 years. Of the patients with stage II-III disease, five died of metastatic disease between 1.16 and 8.49 years after the start of vaccinations (median 6.24 years) and two are alive as of September 2021. Toxicities included injection site reactions, fatigue, fever, upper respiratory symptoms, joint pain, nausea, and edema. Four of five evaluable patients with metastatic disease developed a skin reaction with immune cell infiltration after the fifth injection of unmodified, irradiated tumor cells.
We conclude that tumor cells can be harvested from patients with metastatic or stage II-III breast cancer to prepare autologous GM-CSF-secreting vaccines that induce coordinated immune responses with limited toxicity. TRIAL REGISTRATION AND DATE OF REGISTRATION: clinicaltrials.gov, NCT00317603 (April 25, 2006) and NCT00880464 (April 13, 2009).
免疫的抗原靶标以及疫苗在乳腺癌中的作用尚不清楚。我们对转移性和 II-III 期乳腺癌患者进行了自体 GM-CSF 分泌型乳腺癌疫苗的 I 期研究。
从转移性(n=15)和 II-III 期(n=7)疾病患者的肿瘤细胞中转导复制缺陷型腺病毒载体编码的 GM-CSF,然后进行照射。分别有 12 名和 7 名转移性和 II-III 期疾病患者接受每周一次的疫苗接种,持续 3 周,然后每两周一次,直到疾病进展或疫苗供应耗尽(转移性)或直到给予 6 次总疫苗剂量(II-III 期)。
在接受疫苗接种的转移性疾病患者中,8 例在两个月时出现进展性疾病,3 例在 4-13 个月时出现稳定疾病,1 例在 13 年内未出现疾病证据。在 II-III 期疾病患者中,5 例在接种疫苗开始后 1.16 至 8.49 年(中位 6.24 年)死于转移性疾病,2 例截至 2021 年 9 月仍存活。毒性包括注射部位反应、疲劳、发热、上呼吸道症状、关节痛、恶心和水肿。在接受五次未修饰、照射的肿瘤细胞注射后,有 5 名可评估的转移性疾病患者中有 4 名出现皮肤反应,伴有免疫细胞浸润。
我们得出的结论是,可以从转移性或 II-III 期乳腺癌患者中采集肿瘤细胞,以制备自体 GM-CSF 分泌型疫苗,该疫苗可引起具有有限毒性的协调免疫反应。
clinicaltrials.gov,NCT00317603(2006 年 4 月 25 日)和 NCT00880464(2009 年 4 月 13 日)。
