Kirk C J, Hartigan-O'Connor D, Mulé J J
Department of Surgery, University of Michigan Medical Center, Ann Arbor, Michigan 48109-0666, USA.
Cancer Res. 2001 Dec 15;61(24):8794-802.
Direct administration of dendritic cells (DCs) genetically modified to express secondary lymphoid tissue chemokine (SLC) into growing B16 melanoma could result in a substantial, sustained influx of T cells within the mass with only a transient increase in T-cell numbers in the draining lymph node (DLN). DCs were retained at the tumor site with only a very small percentage trafficking to the DLN. The T cells infiltrating the tumor mass expressed the activation marker CD25 within 24 h and developed IFN-gamma-secreting function within 7 days as tumor growth was inhibited. Similar results were obtained in lymphotoxin alpha-/- mice, which lacked peripheral lymph nodes. Our data demonstrate that effective T-cell priming can occur extranodally and result in measurable antitumor effects in vivo.
将经过基因改造以表达二级淋巴组织趋化因子(SLC)的树突状细胞(DC)直接注入生长中的B16黑色素瘤内,可导致肿瘤块内T细胞大量持续涌入,而引流淋巴结(DLN)中的T细胞数量仅短暂增加。DC保留在肿瘤部位,仅有极小比例迁移至DLN。浸润肿瘤块的T细胞在24小时内表达激活标志物CD25,并在7天内产生分泌γ干扰素的功能,同时肿瘤生长受到抑制。在缺乏外周淋巴结的淋巴毒素α基因敲除小鼠中也获得了类似结果。我们的数据表明,有效的T细胞启动可在淋巴结外发生,并在体内产生可测量的抗肿瘤作用。
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