Kanar M C, Winkelstein A, Platt D
J Natl Cancer Inst. 1983 Feb;70(2):267-73.
The tumorigenicity and host protective mechanisms induced by simian virus 40 (SV40)-transformed 3T3 cells (SV403T3) were evaluated in syngeneic BALB/c mice. Tumors were regularly produced by sc inoculation of SV403T3 cells; the incidence, latent period, and survival were proportional to the size of the initial inoculum. With the use of an in vitro 18-hour 51Cr cytotoxicity assay, spleen cells from normal mice showed a dose-related killing activity against the SV403T3 cells. At an effector cell-to-target cell ratio of 200:1, the average lysis was 56 +/- 6%. This reaction appeared specific for the virally transformed targets; the mean lysis of parent 3T3 cells was 23 +/- 5%. Effectors were resistant to anti-theta serum and not removed by adherence to plastic or nylon wool. Tissue distribution studies indicated that these effectors were present in high concentrations in spleen, bone marrow, lymph nodes, and peritoneal cavity. Low levels of activity were associated with cells from the thymus. In the present studies specific T-cell cytotoxicity against the SV403T3 cells could not be demonstrated. Animals challenged with nonviable SV403T3 cells prior to tumor cell inoculation did not show increased in vivo resistance. In parallel, the in vitro cytotoxicity of animals inoculated with SV403T3 tumor cells showed no heightened cell killing compared to the cytotoxicity of normal controls.
在同基因BALB/c小鼠中评估了猿猴病毒40(SV40)转化的3T3细胞(SV403T3)诱导的致瘤性和宿主保护机制。通过皮下接种SV403T3细胞可定期产生肿瘤;发病率、潜伏期和存活率与初始接种物的大小成正比。使用体外18小时的51Cr细胞毒性试验,正常小鼠的脾细胞对SV403T3细胞表现出剂量相关的杀伤活性。在效应细胞与靶细胞比例为200:1时,平均裂解率为56±6%。这种反应似乎对病毒转化的靶细胞具有特异性;亲代3T3细胞的平均裂解率为23±5%。效应细胞对抗θ血清有抗性,且不会因附着于塑料或尼龙毛而被去除。组织分布研究表明,这些效应细胞在脾脏、骨髓、淋巴结和腹腔中高浓度存在。低水平的活性与来自胸腺的细胞有关。在本研究中,未证明对SV403T3细胞有特异性T细胞细胞毒性。在接种肿瘤细胞之前用无活力的SV403T3细胞攻击的动物在体内没有表现出抗性增加。同时,与正常对照的细胞毒性相比,接种SV403T3肿瘤细胞的动物的体外细胞毒性没有显示出增强的细胞杀伤作用。
