首页> 外文OA文献 >Syngeneic immune response to rat tracheal epithelial cells transformed in vitro by N-methyl-N-nitro-N-nitrosoguanidine.
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Syngeneic immune response to rat tracheal epithelial cells transformed in vitro by N-methyl-N-nitro-N-nitrosoguanidine.

机译:N-甲基-N-硝基-N-亚硝基胍对体外转化的大鼠气管上皮细胞的同源免疫应答。

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摘要

Two cell lines (2-10-1 and 8-10-2) derived by exposure to primary tracheal explants to MNNG in vitro were not tumorigenic in syngeneic F-344 rats or athymic BALB/c (nu/nu) mice at early passage, but became tumorigenic at late passage. These cell lines are therefore suited to study the expression of neoantigens during neoplastic development. Transplantation resistance to late-passage, tumorigenic cells was indicated in syngeneic rats using an immunization protocol of repeated cell inoculation and tumour ablation. Spleen cells from such animals were reactive in 20h microcytotoxicity assays against neoplastic cell lines, but unreactive to normal tracheal epithelial cells. Similarly, immune spleen cells co-cultivated in vitro for 6 days with irradiated neoplastic cell lines before assay for microcytotoxicity were strongly reactive, whereas co-cultivation with normal epithelial cells did not stimulate reactivity. Antibody to these neoplastic cell lines was demonstrated in sera of tumour-resistant rats by an indirect radiolabelled-antibody binding test and by indirect immunofluorescence. There was no significant binding to normal tracheal epithelial cell outgrowths.
机译:在早期传代的同系F-344大鼠或无胸腺BALB / c(nu / nu)小鼠中,通过暴露于体外气管外植体暴露于MNNG衍生的两种细胞系(2-10-1和8-10-2)并非致瘤性的,但在晚期传承时具有致瘤性。因此,这些细胞系适合研究肿瘤发展过程中新抗原的表达。使用重复细胞接种和肿瘤消融的免疫方案,在同系大鼠中表明了对晚期传代的致瘤细胞的移植抗性。来自此类动物的脾细胞在20小时的针对肿瘤细胞系的微细胞毒性试验中具有反应性,但与正常气管上皮细胞无反应。类似地,在测定微细胞毒性之前,体外与辐射的肿瘤细胞系共培养6天的免疫脾细胞具有强反应性,而与正常上皮细胞共培养则不会刺激反应性。通过间接放射性标记的抗体结合试验和间接免疫荧光在肿瘤抗性大鼠的血清中证实了这些肿瘤细胞系的抗体。与正常的气管上皮细胞生长没有明显的结合。

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