Shimizu Y, Iwatsuki S, Herberman R B, Whiteside T L
Pittsburgh Cancer Institute, University of Pittsburgh School of Medicine, PA 15213.
Cancer Immunol Immunother. 1991;32(5):280-8. doi: 10.1007/BF01789045.
Tumor-infiltrating lymphocytes (TIL) were isolated from 22 human primary and metastatic liver tumors, and expanded in vitro in the presence of either interleukin-2 (IL-2, 100 U/ml) plus tumor necrosis factor alpha (TNF alpha, 1000 U/ml), IL-2 (1000 U/ml) plus IL-4 (1000 U/ml) or IL-2 (1000 U/ml) alone. TIL proliferated in culture in 20/22 cases. Among different cytoline combination, TNF alpha and IL-2 were most effective in promoting the outgrowth of CD3+CD8+T lymphocytes (mean +/- SEM: 90% +/- 5) in the cultures of TIL from primary liver tumors. Cytotoxicity against autologous tumor cells was demonstrated in all early cultures of TIL from primary liver cancers in the presence of IL-2 plus TNF alpha. In contrast, cultures of TIL derived from colon cancer metastatic to liver had significantly lower levels of autotumor cytotoxicity and proportions of CD3+CD8+ cells (40% +/- 13) than those of TIL from primary liver tumors. The addition on day 0 of interferons (alpha or gamma) to TIL cultured in the presence of TNF alpha and IL-2, significantly augmented cytotoxicity against autologous tumor. In contrast, incubation of TIL in the presence of IL-4 and IL-2 did not result in increased autotumor responses in the cultures of TIL from primary liver tumors. The expansion (-fold) of TIL (day 30) cultured in the presence of IL-2 alone compared to that in the presence of TNF alpha and IL-2 was significantly greater for hepatocellular carcinoma (median, 280 vs 260) than for autologous peripheral blood lymphocytes (36 vs 27), cholangiocarcinoma (42 vs 51) or TIL from metastatic colon cancer (39 vs 30). Outgrowth of TIL in IL-2 plus TNF alpha offers an opportunity for in vitro enrichment in cells with autotumor cytotoxicity in primary liver tumors. However, this cytokine combination was unable to promote and sustain growth of autotumor effectors from TIL in metastatic liver cancer.
从22例人类原发性和转移性肝肿瘤中分离出肿瘤浸润淋巴细胞(TIL),并在白细胞介素-2(IL-2,100 U/ml)加肿瘤坏死因子α(TNFα,1000 U/ml)、IL-2(1000 U/ml)加IL-4(1000 U/ml)或单独使用IL-2(1000 U/ml)的情况下进行体外扩增。22例中有20例TIL在培养中增殖。在不同的细胞因子组合中,TNFα和IL-2在促进原发性肝肿瘤TIL培养物中CD3+CD8+T淋巴细胞生长(平均±标准误:90%±5)方面最有效。在IL-2加TNFα存在的情况下,原发性肝癌TIL的所有早期培养物中均显示出对自体肿瘤细胞的细胞毒性。相比之下,源自转移至肝脏的结肠癌的TIL培养物中,自体肿瘤细胞毒性水平和CD3+CD8+细胞比例(40%±13)明显低于原发性肝肿瘤的TIL。在TNFα和IL-2存在的情况下培养的TIL中,在第0天添加干扰素(α或γ)可显著增强对自体肿瘤的细胞毒性。相比之下,在IL-4和IL-2存在的情况下培养原发性肝肿瘤TIL,其培养物中的自体肿瘤反应并未增加。与TNFα和IL-2存在的情况相比,单独使用IL-2培养的肝细胞癌TIL(第30天)的扩增倍数(中位数,280对260)显著高于自体外周血淋巴细胞(36对27)、胆管癌(42对51)或转移性结肠癌的TIL(39对30)。IL-2加TNFα培养TIL为原发性肝肿瘤中具有自体肿瘤细胞毒性的细胞提供了体外富集的机会。然而,这种细胞因子组合无法促进和维持转移性肝癌TIL中自体肿瘤效应细胞的生长。
