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活肿瘤细胞的免疫原性。异种肿瘤细胞与卡介苗-肿瘤细胞混合物的比较。

Immunogenicity of viable tumor cells. A comparison of xenogenized tumor cells and BCG-tumor cell mixtures.

作者信息

Suzuki Y, Suzuki K, Hosokawa M, Kobayashi H

出版信息

Cancer Immunol Immunother. 1986;22(3):204-10. doi: 10.1007/BF00200034.

Abstract

The immunogenicity of KMT-17 fibrosarcoma cells which had been xenogenized by infection with FV was compared to that of KMT-17 cells which had been admixed with BCG. We report here that 10(5) and 10(6) KMT-17 cells also grew progressively to kill rats, but when 10(5) KMT-17 cells were administered with BCG the tumor cells did not grow in the majority of rats. The strength of immunogenicity (ETD50), as measured by the number of immunizing cells required for a suppression of growth of 10(7) KMT-17 cells in 50% of the rats, was 2.1 X 10(3) for FV-KMT-17 and 36.3 X 10(3) for BCG + KMT-17. The tumor cell dose (LTD50) which was required to kill 50% of the rats immunized with 10(5) FV-KMT-17 was more than 10,000 times higher than that found in normal rats, whereas the number of tumor cells required to kill 50% of the rats immunized with the same number of BCG + KMT-17 was only 3,680 times higher than the amount found in normal rats. Thus the immunogenicity of FV-KMT-17 is much stronger than that of BCG + KMT-17. The difference in immunogenicity between the two vaccines was also observed in the tumor-neutralizing activities of spleen cells obtained from rats which had been immunized with both vaccines, as measured by a Winn assay. Moreover, the antitumor activity of spleen cells from rats immunized with FV-KMT-17 was concentrated in the carrageenan-resistant and plastic nonadherent cells, while that of spleen cells from rats immunized with BCG + KMT-17 was observed in carrageenan-sensitive and plastic adherent cells as well as in nonadherent cells. The involvement of different effector cells indicates that different mechanisms operate in the antitumor resistance in rats immunized with either FV-KMT-17 or BCG + KMT-17.

摘要

将感染FV后异种移植的KMT - 17纤维肉瘤细胞的免疫原性与混合卡介苗的KMT - 17细胞的免疫原性进行了比较。我们在此报告,10⁵和10⁶个KMT - 17细胞也会逐渐生长并杀死大鼠,但当10⁵个KMT - 17细胞与卡介苗一起给药时,大多数大鼠体内的肿瘤细胞并未生长。通过抑制50%的大鼠体内10⁷个KMT - 17细胞生长所需的免疫细胞数量来衡量的免疫原性强度(ETD50),FV - KMT - 17为2.1×10³,卡介苗 + KMT - 17为36.3×10³。用10⁵个FV - KMT - 17免疫大鼠,杀死50%的大鼠所需的肿瘤细胞剂量(LTD50)比正常大鼠高10000多倍,而用相同数量的卡介苗 + KMT - 17免疫大鼠,杀死50%的大鼠所需的肿瘤细胞数量仅比正常大鼠中发现的数量高3680倍。因此,FV - KMT - 17的免疫原性比卡介苗 + KMT - 17强得多。通过Winn试验测量,在用两种疫苗免疫的大鼠获得的脾细胞的肿瘤中和活性中也观察到了两种疫苗免疫原性的差异。此外,用FV - KMT - 17免疫的大鼠的脾细胞的抗肿瘤活性集中在抗角叉菜胶和塑料非贴壁细胞中,而用卡介苗 + KMT - 17免疫的大鼠的脾细胞的抗肿瘤活性在角叉菜胶敏感和塑料贴壁细胞以及非贴壁细胞中均有观察到。不同效应细胞的参与表明,在用FV - KMT - 17或卡介苗 + KMT - 17免疫的大鼠的抗肿瘤抗性中,存在不同的作用机制。

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