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首页> 外文期刊>Frontiers in Genetics >The Functional Effects of Key Driver KRAS Mutations on Gene Expression in Lung Cancer
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The Functional Effects of Key Driver KRAS Mutations on Gene Expression in Lung Cancer

机译:关键驾驶员KRA突变对肺癌基因表达的功能效应

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摘要

Lung cancer is a common malignant cancer. Kirsten rat sarcoma oncogene (KRAS) mutations have been considered as a key driver for lung cancers. KRAS p.G12C mutations were most predominant in NSCLC which was comprised about 11–16% of lung adenocarcinomas (p.G12C accounts for 45–50% of mutant KRAS). But it is still not clear how the KRAS mutation triggers lung cancers. To study the molecular mechanisms of KRAS mutation in lung cancer. We analyzed the gene expression profiles of 156 KRAS mutation samples and other negative samples with two stage feature selection approach: (1) minimal Redundancy Maximal Relevance (mRMR) and (2) Incremental Feature Selection (IFS). At last, 41 predictive genes for KRAS mutation were identified and a KRAS mutation predictor was constructed. Its leave one out cross validation MCC was 0.879. Our results were helpful for understanding the roles of KRAS mutation in lung cancer.
机译:肺癌是一种常见的恶性癌症。 Kirsten Rat Sarcoma癌基因(KRAS)突变被认为是肺癌的关键驱动因素。 KRAS P.G12C突变在NMSCLC中最多的突变,其包含约11-16%的肺腺癌(P.G12C占45-50%的突变KRA)。但仍然不清楚KRAS突变如何触发肺癌。研究肺癌克拉斯突变的分子机制。我们分析了156克拉斯突变样本的基因表达谱和具有两个阶段特征选择方法的其他阴性样本:(1)最小冗余最大相关性(MRMR)和(2)增量特征选择(IFS)。最后,鉴定了KRAS突变的41个预测基因,构建了KRAS突变预测器。它留下了一个交叉验证MCC为0.879。我们的结果有助于了解KRAS突变在肺癌中的作用。

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