Knutson K L, Disis M L
Tumor Vaccine Group, Division of Oncology, University of Washington, Seattle 98195-6527, USA.
Clin Exp Immunol. 2004 Feb;135(2):322-9. doi: 10.1111/j.1365-2249.2004.02360.x.
CD4+ T cells are essential for the immune response against cancer. Vaccination against cancer will likely only be effective at preventing growth of micrometastatic disease while adoptive T cell therapy will be better suited for eradication of bulky pre-existing disease (Knutson et al. Expert Opin Biol Ther 2002; 2:55-66). Problems with the use of adoptive T cell therapy include lack of CD4+ T cell help, low frequency of antigen-specific T cells, and lack of effective ex vivo expansion techniques. In this study, we focused on improving ex vivo expansion of CD4+ T helper cells. The effects of IL-12, along with IL-2, on the ex vivo generation of HER-2/neu antigen-specific T cells were examined. Patients were immunized with a peptide-based vaccine that contained a helper epitope, p776-790, derived from the intracellular domain of HER-2/neu. While T cell immunity to p776-790, assessed by proliferation assays, could be readily measured in short-term cultures, cell line generation by multiple in vitro stimulation with peptide and IL-2 as the only added cytokine resulted in loss of antigen-specific proliferation. The inclusion of IL-12, along with IL-2, restored antigen-specific proliferation in a dose-dependent fashion. The resulting p776-790-specific T cells responded readily to antigen by proliferating and producing type I cytokines (IFN-gamma and TNF-alpha). The increased proliferative response of the cultures was due in part to an increase in the number of HER-2/neu-specific T cells. These results suggest that IL-12 is an important cytokine for ex vivo recovery and maintenance of antigen-specific CD4+ T lymphocytes that would otherwise be lost by using IL-2 alone in combination with antigen. Furthermore, these results have important implications for ex vivo expansion of CD4+ T cell for use in anti-tumour adoptive immunotherapy.
CD4 + T细胞对于抗癌免疫反应至关重要。癌症疫苗接种可能仅在预防微转移疾病生长方面有效,而过继性T细胞疗法更适合根除已存在的大块疾病(Knutson等人,《专家意见:生物治疗》2002年;2:55 - 66)。过继性T细胞疗法使用中存在的问题包括缺乏CD4 + T细胞辅助、抗原特异性T细胞频率低以及缺乏有效的体外扩增技术。在本研究中,我们专注于改善CD4 + T辅助细胞的体外扩增。研究了白细胞介素-12(IL - 12)与白细胞介素-2(IL - 2)对HER - 2 / neu抗原特异性T细胞体外生成的影响。患者用一种基于肽的疫苗进行免疫,该疫苗包含一个源自HER - 2 / neu细胞内结构域的辅助表位p776 - 790。虽然通过增殖试验评估的对p776 - 790的T细胞免疫在短期培养中很容易测量,但以肽和IL - 2作为唯一添加细胞因子进行多次体外刺激产生细胞系会导致抗原特异性增殖丧失。IL - 12与IL - 2一起加入后,以剂量依赖方式恢复了抗原特异性增殖。产生的p776 - 790特异性T细胞通过增殖和产生I型细胞因子(干扰素-γ和肿瘤坏死因子-α)对抗原做出迅速反应。培养物增殖反应的增加部分归因于HER - 2 / neu特异性T细胞数量的增加。这些结果表明,IL - 12是体外恢复和维持抗原特异性CD4 + T淋巴细胞的重要细胞因子,否则仅使用IL - 2与抗原组合会导致这些细胞丢失。此外,这些结果对于用于抗肿瘤过继性免疫治疗的CD4 + T细胞的体外扩增具有重要意义。
