Nair A P, Diamantis I D, Conscience J F, Kindler V, Hofer P, Moroni C
Friedrich Miescher-Institut, Basel, Switzerland.
Mol Cell Biol. 1989 Mar;9(3):1183-90. doi: 10.1128/mcb.9.3.1183-1190.1989.
Autocrine interleukin 3 (IL-3)-secreting tumors were generated from an IL-3-dependent mouse mast cell line (PB-3c) after introduction of the v-H-ras oncogene. Tumor progression was characterized by four distinct phenotypes. The first corresponded to immortalized mast cells unresponsive to the oncogenic effect of v-H-ras. The second was expressed in a clonable subpopulation of PB-3c cells and was marked by the competence to form v-H-ras-dependent tumors (immortalized transformation competence). The third was a direct effect of v-H-ras expression on all PB-3c cells and was characterized in vitro by a reduced IL-3 requirement. Upon injection of v-H-ras-expressing, transformation-competent cells into mice, the final, fully malignant phenotype developed with a long latency period and was marked in vitro by independence of exogenous IL-3 and by autocrine IL-3 stimulation. Northern (RNA) blot analysis and an RNase A-T1 protection assay showed that IL-3 production was strictly associated with the tumor phenotype. Two of six tumors showed an alteration at the 5' region of the IL-3 gene. We conclude that v-H-ras required complementation by IL-3 gene rearrangement or an alternate event to generate autocrine mastocytomas.
在导入v-H-ras癌基因后,从依赖白细胞介素3(IL-3)的小鼠肥大细胞系(PB-3c)中产生了自分泌IL-3的肿瘤。肿瘤进展具有四种不同的表型特征。第一种表型对应于对v-H-ras致癌作用无反应的永生化肥大细胞。第二种表型在PB-3c细胞的一个可克隆亚群中表达,其特征是具有形成依赖v-H-ras的肿瘤的能力(永生化转化能力)。第三种表型是v-H-ras表达对所有PB-3c细胞的直接作用,其体外特征是对IL-3的需求减少。将表达v-H-ras且具有转化能力的细胞注射到小鼠体内后,最终的完全恶性表型在较长潜伏期后出现,其体外特征是不依赖外源性IL-3且有自分泌IL-3刺激。Northern(RNA)印迹分析和核糖核酸酶A-T1保护试验表明,IL-3的产生与肿瘤表型密切相关。六个肿瘤中有两个在IL-3基因的5'区域出现改变。我们得出结论,v-H-ras需要通过IL-3基因重排或其他事件进行互补才能产生自分泌肥大细胞瘤。
