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A model for RAS mutation patterns in cancers: finding the sweet spot

机译:癌症中RAS突变模式的模型:寻找甜蜜点

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摘要

The three RAS genes-HRAS, NRAS and KRAS-are collectively mutated in one-third of human cancers, where they act as prototypic oncogenes. Interestingly, there are rather distinct patterns to RAS mutations; the isoform mutated as well as the position and type of substitution vary between different cancers. As RAS genes are among the earliest, if not the first, genes mutated in a variety of cancers, understanding how these mutation patterns arise could inform on not only how cancer begins but also the factors influencing this event, which has implications for cancer prevention. To this end, we suggest that there is a narrow window or 'sweet spot' by which oncogenic RAS signalling can promote tumour initiation in normal cells. As a consequence, RAS mutation patterns in each normal cell are a product of the specific RAS isoform mutated, as well as the position of the mutation and type of substitution to achieve an ideal level of signalling.
机译:三个Ras基因 - HRAS,NRAS和KRAS-在三分之一的人类癌症中共同突变,在那里它们用作原型癌基因。 有趣的是,对Ras突变有相当鲜明的模式; 同种型突变以及替代的位置和类型在不同的癌症之间变化。 随着RAS基因最早的,如果不是第一个,则在各种癌症中突变的第一个基因,了解这些突变模式如何出现如何通知癌症的开始,也是影响这一事件的因素,这对癌症预防有影响。 为此,我们建议存在狭窄的窗户或“甜点”,致癌RAS信号可以促进正常细胞中的肿瘤起始。 结果,每个正常细胞中的RAS突变模式是特定RAS同种型突变的产物,以及突变的位置和替换类型以实现理想的信号程。

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  • 来源
    《Nature reviews Cancer》 |2018年第12期|共11页
  • 作者单位

    Duke Univ Med Ctr Dept Pharmacol &

    Canc Biol Durham NC 27708 USA;

    Univ Calif San Francisco Helen Diller Family Comprehens Canc Ctr San Francisco CA 94143 USA;

    Duke Univ Med Ctr Dept Pharmacol &

    Canc Biol Durham NC 27708 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

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