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首页> 外文期刊>Cancer gene therapy >Synergistic antitumor effect by coexpression of chemokine CCL21|[sol]|SLC and costimulatory molecule LIGHT
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Synergistic antitumor effect by coexpression of chemokine CCL21|[sol]|SLC and costimulatory molecule LIGHT

机译:共表达趋化因子CCL21 | [sol] | SLC和共刺激分子LIGHT的协同抗肿瘤作用

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To establish a more efficient treatment for immunotherapy against solid tumors, we have evaluated the antitumor effect by coexpression of a chemokine CCL21/secondary lymphoid tissue chemokine and a costimulatory molecule LIGHT in colon carcinoma C26. C26 cells expressing either CCL21 or LIGHT exhibited a significantly reduced tumor growth in vivo, and mice inoculated with these cells showed a prolonged survival, but eventually all these mice died. In contrast, C26 cells expressing both CCL21 and LIGHT exhibited a minimal tumor growth in vivo, and all these mice survived healthily with a tumor remission and consequently acquired a strong protective immunity. A markedly increased infiltration of mature dendritic cells (DCs), and CD8+ T cells was observed in the tumor mass, and their spleen cells showed a greatly enhanced cytotoxic T lymphocyte (CTL) activity against C26 tumor and interferon (IFN)- production. Neutralization of IFN- or depletion of CD8+ or CD4+ T cells significantly reduced the antitumor activity. These results suggest that the combined treatment with CCL21 and LIGHT is able to induce a synergistic antitumor effect to eradicate tumor completely by greatly enhancing tumor-infiltration of lymphocytes including mature DCs and CD8+ T cells, resulting in markedly augmented CTL activity and IFN- production.
机译:为了建立针对实体瘤的免疫疗法的更有效治疗方法,我们已经通过在结肠癌C26中共表达趋化因子CCL21 /次级淋巴组织趋化因子和共刺激分子LIGHT评估了抗肿瘤作用。表达CCL21或LIGHT的C26细胞在体内的肿瘤生长显着减少,接种这些细胞的小鼠存活时间延长,但最终所有这些小鼠死亡。相反,表达CCL21和LIGHT的C26细胞在体内表现出最小的肿瘤生长,并且所有这些小鼠都健康地存活并具有肿瘤缓解,因此获得了强的保护性免疫。在肿瘤块中观察到成熟树突细胞(DC)和CD8 + T细胞的浸润明显增加,并且它们的脾细胞显示出对C26肿瘤和干扰素(IFN)产生的细胞毒性T淋巴细胞(CTL)活性大大增强。 IFN-的中和或CD8 +或CD4 + T细胞的耗竭显着降低了抗肿瘤活性。这些结果表明,CCL21和LIGHT的联合治疗能够通过极大地增强包括成熟DC和CD8 + T细胞在内的淋巴细胞的肿瘤浸润来诱导协同抗肿瘤作用,从而彻底根除肿瘤,从而显着提高CTL活性和IFN产生。

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