首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Activating Met mutations produce unique tumor profiles in mice with selective duplication of the mutant allele
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Activating Met mutations produce unique tumor profiles in mice with selective duplication of the mutant allele

机译:活化的Met突变在小鼠中产生独特的肿瘤特征,选择性复制突变等位基因

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摘要

Tyrosine kinase-activating mutations in Met have been observed in hereditary papillary renal carcinomas as well as in other cancers. These mutations have been examined in several in vitro systems, where they cause constitutive Met activation, focus formation, and cell motility, and are tumorigenic in xenografts. To study the influence of these mutations on tumorigenesis in vivo, we generated mice with targeted mutations in the murine met locus. The following five mouse lines with mutant Met were created: WT, D1226N, Y1228C, M1248T, and M1248T/ L1193V. We observed that mice harboring D1226N, Y1228C, and M1248T/ L1193V mutations developed a high frequency of sarcomas and some lymphomas, whereas the M1248T mice developed carcinomas and lymphomas. Of considerable interest, we observed trisomy of chromosome 6 and duplication of the mutant met allele in a majority of the tumors, similar to what has been reported in patients with hereditary renal papillary carcinomas. These results demonstrate that activating Met mutations and met amplification play key roles in promoting tumorigenesis in vivo. Moreover, our findings show that different mutations in the Met kinase domain can influence the types of cancers that develop.
机译:在遗传性乳头状肾癌以及其他癌症中,已观察到Met中酪氨酸激酶激活突变。这些突变已在几种体外系统中进行了检查,它们引起组成型Met活化,焦点形成和细胞运动,并且在异种移植物中具有致瘤性。为了研究这些突变对体内肿瘤发生的影响,我们在鼠类基因座中产生了具有目标突变的小鼠。创建了具有突变Met的以下五种小鼠系:WT,D1226N,Y1228C,M1248T和M1248T / L1193V。我们观察到,携带D1226N,Y1228C和M1248T / L1193V突变的小鼠发生肉瘤和某些淋巴瘤的频率很高,而M1248T小鼠则发生癌和淋巴瘤。相当感兴趣的是,我们在大多数肿瘤中观察到了6号染色体的三体性和突变的met等位基因重复,这与遗传性肾乳头状癌患者的报道相似。这些结果表明,激活Met突变并实现扩增在体内促进肿瘤发生中起关键作用。此外,我们的发现表明,Met激酶结构域中的不同突变可影响正在发展的癌症类型。

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