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将MHC II类/CD80+肿瘤细胞与白细胞介素-12相结合的疫苗免疫疗法可减少已形成的转移性疾病,并刺激免疫效应细胞和干扰素γ诱导的单核因子。

Immunotherapy with vaccines combining MHC class II/CD80+ tumor cells with interleukin-12 reduces established metastatic disease and stimulates immune effectors and monokine induced by interferon gamma.

作者信息

Pulaski B A, Clements V K, Pipeling M R, Ostrand-Rosenberg S

机构信息

Department of Biological Sciences, University of Maryland, Baltimore 21250, USA.

出版信息

Cancer Immunol Immunother. 2000 Apr;49(1):34-45. doi: 10.1007/s002620050024.

Abstract

Because they are difficult to treat, animal models of widespread, established metastatic cancer are rarely used to test novel immunotherapies. Two such mouse models are used in this report to demonstrate the therapeutic efficacy and to probe the mechanisms of a novel combination immunotherapy consisting of the cytokine interleukin-12 (IL-12) combined with a previously described vaccine based on MHC class II, CD80-expressing cells. BALB/c mice with 3-week established primary 4T1 mammary carcinomas up to 6 mm in diameter and with extensive, spontaneous lung metastases show a significant reduction in lung metastases following a 3-week course of immunotherapy consisting of weekly injections of the cell-based vaccine plus injections of IL-12 three times per week. C57BL/6 mice with 7-day established intravenous B16 melF10 lung metastases show a similar response following immunotherapy with IL-12 plus a vaccine based on B16 MHC class II, CD80-expressing cells. In both systems the combination therapy of cells plus IL-12 is more effective than IL-12 or the cellular vaccine alone, although, in the 4T1 system, optimal activity does not require MHC class II and CD80 expression in the vaccine cells. The cell-based vaccines were originally designed to activate tumor-specific CD4+ T lymphocytes specifically and thereby provide helper activity to tumor-cytotoxic CD8+ T cells, and IL-12 was added to the therapy to facilitate T helper type 1 lymphocyte (Th1) differentiation. In vivo depletion experiments for CD4+ and CD8+ T cells and natural killer (NK) cells and tumor challenge experiments in beige/nude/XID immunodeficient mice demonstrate that the therapeutic effect is not exclusively dependent on a single cell population, suggesting that T and NK cells are acting together to optimize the response. IL-12 may also be enhancing the immunotherapy via induction of the chemokine Mig (monokine induced by interferon gamma), because reverse PCR experiments demonstrate that Mig is present in the lungs of mice receiving therapy and is most likely synthesized by the tumor cells. These results demonstrate that the combination therapy of systemic IL-12 and a cell-based vaccine is an effective agent for the treatment of advanced, disseminated metastatic cancers in experimental mouse models and that multiple effector cell populations and anti-angiostatic factors are likely to mediate the effect.

摘要

由于难以治疗,广泛存在且已形成转移的癌症动物模型很少用于测试新型免疫疗法。本报告中使用了两种这样的小鼠模型来证明治疗效果,并探究一种新型联合免疫疗法的机制,该疗法由细胞因子白细胞介素-12(IL-12)与先前描述的基于表达MHC II类、CD80的细胞的疫苗组成。患有已形成3周、直径达6毫米的原发性4T1乳腺癌且伴有广泛自发性肺转移的BALB/c小鼠,在接受为期3周的免疫疗法后,肺转移显著减少,该免疫疗法包括每周注射基于细胞的疫苗以及每周注射三次IL-12。患有已形成7天的静脉内B16 melF10肺转移的C57BL/6小鼠,在接受IL-12与基于B16 MHC II类、CD80表达细胞的疫苗的免疫疗法后,显示出类似的反应。在这两个系统中,细胞加IL-12的联合疗法比单独使用IL-12或细胞疫苗更有效,尽管在4T1系统中,最佳活性并不要求疫苗细胞表达MHC II类和CD80。基于细胞的疫苗最初设计用于特异性激活肿瘤特异性CD4+ T淋巴细胞,从而为肿瘤细胞毒性CD8+ T细胞提供辅助活性,并且在治疗中添加IL-12以促进1型辅助性T淋巴细胞(Th1)分化。对CD4+和CD8+ T细胞以及自然杀伤(NK)细胞进行的体内清除实验,以及在米色/裸鼠/XID免疫缺陷小鼠中进行的肿瘤攻击实验表明,治疗效果并非完全依赖于单一细胞群体,这表明T细胞和NK细胞共同作用以优化反应。IL-12也可能通过诱导趋化因子Mig(γ干扰素诱导的单核因子)来增强免疫疗法,因为逆转录PCR实验表明Mig存在于接受治疗的小鼠肺中,并且很可能由肿瘤细胞合成。这些结果表明,全身性IL-12与基于细胞的疫苗的联合疗法是实验小鼠模型中治疗晚期、播散性转移性癌症的有效药物,并且多种效应细胞群体和抗血管生成因子可能介导了这种效应。

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