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首页> 外文期刊>Cancer biology & therapy >C-Raf-1 protein kinase is not essential for Ras transformation of mouse embryo fibroblasts.
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C-Raf-1 protein kinase is not essential for Ras transformation of mouse embryo fibroblasts.

机译:C-Raf-1蛋白激酶对于小鼠胚胎成纤维细胞的Ras转化不是必需的。

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摘要

Transfection of primary cells with mutated oncogenic ras plus a cooperating oncogene such as myc results in the acquisition of the transformed cell phenotype. The pathways downstream of Ras that are required for transformation are an active topic of research. The Raf-MEKK-MAP kinase pathway is triggered by activation of Ras and thought to be important in Ras transformation of rodent fibroblasts. To further explore the involvement of this pathway, fibroblasts from homozygous knock out c-Raf-1 mouse embryos (20 KO) and wild-type c-Raf-1 mouse embryos (16 WT) were transfected with H-ras and myc(v). The resulting cell line derived from the knock out cells grew slower both in tissue culture and had a longer latency period as tumors than the transformed cell line from the wild-type cells. Both cell lines were however able to form tumors in nude mice. These results suggest that c-Raf-1 is not required for Ras transformation in this system.
机译:用突变的致癌性ras加上协同致癌基因(如myc)转染原代细胞会导致获得转化的细胞表型。转化所需的Ras下游途径是研究的活跃话题。 Raf-MEKK-MAP激酶途径由Ras激活而触发,被认为在啮齿动物成纤维细胞的Ras转化中很重要。为了进一步探索该途径的参与,将纯合敲除c-Raf-1小鼠胚胎(20 KO)和野生型c-Raf-1小鼠胚胎(16 WT)的成纤维细胞用H-ras和myc(v )。与从野生型细胞转化的细胞系相比,源自敲除细胞的所得细胞系在组织培养中生长都较慢,并且作为肿瘤的潜伏期更长。然而,两种细胞系都能够在裸鼠中形成肿瘤。这些结果表明,在该系统中,Ras转化不需要c-Raf-1。

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