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Neoplastic transformation by the human gene N-myc.

机译:人类基因N-myc进行肿瘤转化。

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Amplification and abundant expression of a gene known as N-myc are found frequently in advanced stages of human neuroblastoma and may play a role in the genesis of several malignant human tumors. Previous studies have shown that N-myc can cooperate with a mutant allele of the proto-oncogene c-Ha-ras to transform embryonic rat cells in culture. Here we show that N-myc can also act alone to elicit neoplastic growth of an established line of rat fibroblasts (Rat-1). We used recombinant DNA vectors to express either N-myc or its kindred gene c-myc in transfected cells. Both genes caused morphological transformation, anchorage-independent growth, and tumorigenicity. We noticed two variables that appeared to influence the ability to isolate cells transformed by N-myc and c-myc: the abundance in which the genes were expressed and biological selection to eliminate untransformed cells from the cultures. Our findings sustain the belief that N-myc is an authentic proto-oncogene, lend further credibility to the role of N-myc in the genesis of human tumors, and establish a convenient assay that can be used to explore further the properties of both N-myc and c-myc.
机译:在人类神经母细胞瘤的晚期经常发现一种名为N-myc的基因的扩增和丰富表达,并且可能在几种恶性人类肿瘤的发生中起作用。先前的研究表明,N-myc可以与原癌基因c-Ha-ras的突变等位基因协同作用,以转化培养中的胚胎大鼠细胞。在这里,我们显示N-myc也可以单独发挥作用,诱导已建立的大鼠成纤维细胞系(Rat-1)的肿瘤生长。我们使用重组DNA载体在转染的细胞中表达N-myc或其同类基因c-myc。这两个基因均引起形态转化,不依赖锚定的生长和致瘤性。我们注意到似乎影响分离由N-myc和c-myc转化的细胞的能力的两个变量:基因表达的丰度和从培养物中消除未转化细胞的生物学选择。我们的发现坚持认为N-myc是真实的原癌基因,进一步证明了N-myc在人类肿瘤发生中的作用,并建立了可用于进一步探索这两种N的特性的简便测定方法。 -myc和c-myc。

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