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单核细胞介导的药物依赖性细胞毒性:对不同的WEHI 164靶细胞系的影响

Monocyte-mediated drug-dependent cellular cytotoxicity: effects on different WEHI 164 target cell lines.

作者信息

Austgulen R, Kildahl-Andersen O, Espevik T

出版信息

Cancer Immunol Immunother. 1986;22(3):176-80. doi: 10.1007/BF00200029.

Abstract

The contribution of monocyte cytotoxic protein factor (CF) to monocyte-mediated drug-dependent cellular cytotoxicity (DDCC) has been investigated. Cell lines which have been derived from murine WEHI 164 cells (termed WEHI 164 parental) by selecting for high (WEHI 164 clone 3) and low (R-WEHI 164) sensitivity to CF-mediated cytotoxicity were used as target cells in DDCC. By comparing the CF doses which produced 50% dead cells (LD 50) we found that WEHI 164 clone 3 was approximately 30 times more sensitive than WEHI 164 parental which in turn was 70 times more sensitive than R-WEHI 164. Actinomycin D (Act D) treatment of WEHI 164 parental and R-WEHI 164 greatly increase susceptibility to CF-mediated cytotoxicity. The susceptibility of WEHI 164 clone 3 was apparently somewhat increased at low dilutions of CF, whereas no significant increase was observed at high dilutions. The susceptibility to DDCC of the three target cell lines (WEHI 164 parental, WEHI 164 clone 3, and R-WEHI 164) correlated with the sensitivity pattern obtained in CF-mediated cytotoxicity of Act D-treated target cells. Monocyte- and CF-mediated cytotoxicity against Act D-treated WEHI 164 clone 3 and R-WEHI 164 was inhibited by neutralizing CF antiserum. These data indicate that CF is an effector molecule in monocyte-mediated DDCC.

摘要

已经研究了单核细胞细胞毒性蛋白因子(CF)对单核细胞介导的药物依赖性细胞毒性(DDCC)的作用。通过选择对CF介导的细胞毒性具有高敏感性(WEHI 164克隆3)和低敏感性(R-WEHI 164),从鼠源WEHI 164细胞(称为WEHI 164亲本细胞)衍生而来的细胞系被用作DDCC中的靶细胞。通过比较产生50%死亡细胞的CF剂量(LD50),我们发现WEHI 164克隆3的敏感性比WEHI 164亲本细胞高约30倍,而WEHI 164亲本细胞又比R-WEHI 164高70倍。用放线菌素D(Act D)处理WEHI 164亲本细胞和R-WEHI 164可大大增加对CF介导的细胞毒性的敏感性。在低稀释度的CF下,WEHI 164克隆3的敏感性明显有所增加,而在高稀释度下未观察到显著增加。三种靶细胞系(WEHI 164亲本细胞、WEHI 164克隆3和R-WEHI 164)对DDCC的敏感性与Act D处理的靶细胞在CF介导的细胞毒性中获得的敏感性模式相关。针对Act D处理的WEHI 164克隆3和R-WEHI 164的单核细胞和CF介导的细胞毒性被中和性CF抗血清所抑制。这些数据表明CF是单核细胞介导的DDCC中的效应分子。

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