Parney Ian F, Chang Lung-Ji, Farr-Jones Maxine A, Hao Chunhai, Smylie Michael, Petruk Kenneth C
Department of Clinical Neurosciences, Southern Alberta Cancer Research Institute, University of Calgary, Calgary, Alberta, Canada.
J Neurooncol. 2006 May;78(1):71-80. doi: 10.1007/s11060-005-9058-0. Epub 2006 Apr 21.
Malignant glioblastomas and melanomas continue to have a dismal prognosis despite advances in conventional therapy. This has led to investigations of novel treatment strategies including immunogene therapy. We report a pilot clinical trial of combined B7-2 and GM-CSF immunogene therapy for gliomas and melanomas and discuss technical hurdles encountered.
Patients with recurrent malignant gliomas or medically refractory melanomas were vaccinated with irradiated autologous tumor cells transduced with B7-2 and GM-CSF genes using a retroviral vector. Patients were monitored for toxicity, inflammatory/immune reactions, and clinical status.
Vaccine preparation was attempted from 116 malignant glioma and 32 melanoma specimens. Adequate vaccines could only be prepared for five glioblastoma and three melanoma patients. Six patients (three recurrent glioblastomas and three melanomas) were actually vaccinated. Minor toxicities included flu-like symptoms (3/6), injection site erythema (4/6), and asymptomatic elevations in liver enzymes (3/6). Most patients showed evidence of an inflammatory response but specific anti-tumor immunity was not demonstrated. All six patients have died, although three patients with minimal residual disease at treatment had prolonged recurrence-free intervals after vaccination.
Combined B7-2 and GM-CSF immunogene therapy for glioblastomas and melanomas using autologous tumor cells has many technical pitfalls hindering large scale application and evaluation. As a result, this pilot study was too limited to draw meaningful conclusions regarding safety or anti-tumor immunity. While immunotherapy has been promising in pre-clinical studies, alternate strategies will be required to bring these benefits to patients.
尽管传统治疗方法取得了进展,但恶性胶质母细胞瘤和黑色素瘤的预后仍然很差。这促使人们对包括免疫基因治疗在内的新型治疗策略进行研究。我们报告了一项针对胶质瘤和黑色素瘤的联合B7-2和GM-CSF免疫基因治疗的试点临床试验,并讨论了遇到的技术障碍。
复发性恶性胶质瘤或药物难治性黑色素瘤患者接受了用逆转录病毒载体转导B7-2和GM-CSF基因的经辐照自体肿瘤细胞疫苗接种。对患者进行毒性、炎症/免疫反应和临床状态监测。
尝试从116例恶性胶质瘤和32例黑色素瘤标本制备疫苗。仅能为5例胶质母细胞瘤患者和3例黑色素瘤患者制备足够的疫苗。实际接种疫苗的有6例患者(3例复发性胶质母细胞瘤和3例黑色素瘤)。轻微毒性包括流感样症状(3/6)、注射部位红斑(4/6)和无症状的肝酶升高(3/6)。大多数患者显示出炎症反应的证据,但未证明有特异性抗肿瘤免疫。所有6例患者均已死亡,尽管3例治疗时残留疾病最少的患者在接种疫苗后无复发生存期延长。
使用自体肿瘤细胞对胶质母细胞瘤和黑色素瘤进行联合B7-2和GM-CSF免疫基因治疗存在许多技术缺陷,阻碍了大规模应用和评估。因此,这项试点研究过于有限,无法就安全性或抗肿瘤免疫得出有意义的结论。虽然免疫疗法在临床前研究中前景广阔,但需要采用替代策略才能将这些益处带给患者。
