Sotillo R, Dubus P, Martín J, de la Cueva E, Ortega S, Malumbres M, Barbacid M
Molecular Oncology Program, Centro Nacional de Investigaciones Oncológicas, Melchor Fernández Almagro 3 E-28029 Madrid, Spain.
EMBO J. 2001 Dec 3;20(23):6637-47. doi: 10.1093/emboj/20.23.6637.
We have introduced a point mutation in the first coding exon of the locus encoding the cyclin-dependent kinase 4 (Cdk4) by homologous recombination in embryonic stem cells. This mutation (replacement of Arg24 by Cys) was first found in patients with hereditary melanoma and renders Cdk4 insensitive to INK4 inhibitors. Here, we report that primary embryonic fibroblasts expressing the mutant Cdk4R24C kinase are immortal and susceptible to transformation by Ras oncogenes. Moreover, homozygous Cdk4(R24C/R24C) mutant mice develop multiple tumors with almost complete penetrance. The most common neoplasia (endocrine tumors and hemangiosarcomas) are similar to those found in pRb(+/-) and p53(-/-) mice. This Cdk4 mutation cooperates with p53 and p27(Kip1) deficiencies in decreasing tumor latency and favoring development of specific tumor types. These results provide experimental evidence for a central role of Cdk4 regulation in cancer and provide a valuable model for testing the potential anti-tumor effect of Cdk4 inhibitors in vivo.
我们通过胚胎干细胞中的同源重组,在编码细胞周期蛋白依赖性激酶4(Cdk4)的基因座的第一个编码外显子中引入了一个点突变。这种突变(将Arg24替换为Cys)最初在遗传性黑色素瘤患者中发现,使Cdk4对INK4抑制剂不敏感。在此,我们报告表达突变型Cdk4R24C激酶的原代胚胎成纤维细胞是永生的,并且易被Ras癌基因转化。此外,纯合的Cdk4(R24C/R24C)突变小鼠几乎完全显性地发生多种肿瘤。最常见的肿瘤(内分泌肿瘤和血管肉瘤)与在pRb(+/-)和p53(-/-)小鼠中发现的肿瘤相似。这种Cdk4突变与p53和p27(Kip1)缺陷协同作用,可缩短肿瘤潜伏期并促进特定肿瘤类型的发生。这些结果为Cdk4调控在癌症中的核心作用提供了实验证据,并为在体内测试Cdk4抑制剂的潜在抗肿瘤作用提供了有价值的模型。