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激素抵抗性前列腺癌异体细胞疫苗接种后疾病进展延迟及其与免疫变量的相关性

Delayed disease progression after allogeneic cell vaccination in hormone-resistant prostate cancer and correlation with immunologic variables.

作者信息

Michael Agnieska, Ball Graham, Quatan Nadine, Wushishi Fatima, Russell Nick, Whelan Joe, Chakraborty Prabir, Leader David, Whelan Michael, Pandha Hardev

机构信息

Department of Oncology, St. George's Hospital Medical School, London, United Kingdom.

出版信息

Clin Cancer Res. 2005 Jun 15;11(12):4469-78. doi: 10.1158/1078-0432.CCR-04-2337.

Abstract

PURPOSE

There are a significant number of patients with asymptomatic hormone-resistant prostate cancer who have increasing prostate-specific antigen (PSA) levels but little or no evaluable disease. The immunogenicity and minimal toxicity associated with cell-based vaccine therapy makes this approach attractive for these patients.

EXPERIMENTAL DESIGN

We have evaluated a vaccine comprising monthly intradermal injection of three irradiated allogeneic prostate cell lines (8 x 10(6) cells each) over 1 year. The first two doses were supplemented with bacille Calmette-Guérin as vaccine adjuvant. Twenty-eight hormone-resistant prostate cancer patients were enrolled. Patients were assessed clinically and PSA levels were measured monthly. Radiologic scans (X-ray, computed tomography, and bone scan) were taken at baseline and at intervals throughout the treatment period. Comprehensive monthly immunologic monitoring was undertaken including proliferation studies, activation markers, cytokine protein expression, and gene copy number. This longitudinal data was analyzed through predictive modeling using artificial neural network feed-forward/back-propagation algorithms with multilayer perceptron architecture.

RESULTS

Eleven of the 26 patients showed statistically significant, prolonged decreases in their PSA velocity (PSAV). None experienced any significant toxicity. Median time to disease progression was 58 weeks, compared with recent studies of other agents and historical control values of around 28 weeks. PSAV-responding patients showed a titratable T(H)1 cytokine release profile in response to restimulation with a vaccine lysate, while nonresponders showed a mixed T(H)1 and T(H)2 response. Furthermore, immunologic profile correlated with PSAV response by artificial neural network analysis. We found predictive power not only in expression of cytokines after maximal stimulation with phorbol 12-myristate 13-acetate, but also the method of analysis (qPCR measurement of IFN-gamma > qPCR measurement tumor necrosis factor-alpha > protein expression of IFN-gamma > protein expression of interleukin 2).

CONCLUSIONS

Whole cell allogeneic vaccination in hormone-resistant prostate cancer is nontoxic and improves the natural history of the disease. Longitudinal changes in immunologic function in vaccinated patients may be better interpreted through predictive modeling using tools such as the artificial neural network rather than periodic "snapshot" readouts.

摘要

目的

有相当数量无症状激素抵抗性前列腺癌患者,其前列腺特异性抗原(PSA)水平不断升高,但几乎没有可评估的疾病。基于细胞的疫苗疗法具有免疫原性且毒性极小,这使得该方法对这些患者具有吸引力。

实验设计

我们评估了一种疫苗,该疫苗包括在1年内每月皮内注射三种经辐照的同种异体前列腺细胞系(每种8×10⁶个细胞)。前两剂补充了卡介苗作为疫苗佐剂。招募了28名激素抵抗性前列腺癌患者。对患者进行临床评估,并每月测量PSA水平。在基线和整个治疗期间定期进行放射学扫描(X线、计算机断层扫描和骨扫描)。每月进行全面的免疫监测,包括增殖研究、激活标志物、细胞因子蛋白表达和基因拷贝数。使用具有多层感知器架构的人工神经网络前馈/反向传播算法,通过预测建模对这些纵向数据进行分析。

结果

26名患者中有11名患者的PSA速度(PSAV)出现统计学上显著的、持续的下降。没有人经历任何显著的毒性。疾病进展的中位时间为58周,而最近对其他药物的研究以及历史对照值约为28周。对PSAV有反应的患者在用疫苗裂解物重新刺激后显示出可滴定的Th1细胞因子释放谱,而无反应者显示出混合的Th1和Th2反应。此外,通过人工神经网络分析,免疫谱与PSAV反应相关。我们不仅在佛波酯12 -肉豆蔻酸酯13 -乙酸酯最大刺激后细胞因子的表达中发现了预测能力,而且在分析方法中也发现了预测能力(IFN -γ的qPCR测量>肿瘤坏死因子 -α的qPCR测量>IFN -γ的蛋白表达>白细胞介素2的蛋白表达)。

结论

激素抵抗性前列腺癌的全细胞同种异体疫苗接种无毒,并改善了疾病的自然病程。通过使用人工神经网络等工具进行预测建模,而不是定期的“快照”读数,可能更好地解释接种疫苗患者免疫功能的纵向变化。

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