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首页> 外文期刊>Biochemical and Biophysical Research Communications >Correlation of PIK3Ca mutations with gene expression and drug sensitivity in NCI-60 cell lines.
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Correlation of PIK3Ca mutations with gene expression and drug sensitivity in NCI-60 cell lines.

机译:NCI-60细胞株中PIK3Ca突变与基因表达和药物敏感性的相关性。

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摘要

The gene that encodes the alpha-isoform of phosphatidylinositol 3-kinase (PIK3Ca) is frequently mutated in human cancers. We profiled the mutation status of the PIK3Ca gene in the National Cancer Institute (NCI)-60 panel of human cancer cell lines maintained by the Developmental Therapeutics Program of the NCI. Mutation hotspots on the gene were PCR amplified and sequenced, and the trace data were analyzed with software designed to detect mutations. Seven of the cell lines tested have PIK3Ca mutations: two lines derived from breast cancer, two from colon cancer, two from ovarian cancer, and one from lung cancer. BRAF and EGFR genes were normal in the PIK3Ca mutant lines. Two of the cell lines with mutant PIK3Ca also have a mutant version of the KRAS gene. The mutation status was correlated with array-based gene expression that is publicly available for the NCI-60 cell lines. We found increased expression levels for estrogen receptor (ER) and ERBB2 in PIK3Ca mutant lines. The PIK3Ca mutation status was also correlated with compound screening data for the cell lines. PIK3Ca-mutant cell lines were relatively more sensitive than PIK3Ca-normal cell lines to the ER inhibitor tamoxifen and the AKT inhibitor triciribine, among other compounds. The results provide insights into the role of mutant PIK3Ca in oncogenic signaling and allow preliminary identification of novel targets for therapeutic intervention in cancers harboring PIK3Ca mutations.
机译:编码磷脂酰肌醇3-激酶(PIK3Ca)的α-同工型的基因在人类癌症中经常发生突变。我们在由NCI的发展治疗计划维护的人类癌细胞系的国家癌症研究所(NCI)-60小组中分析了PIK3Ca基因的突变状态。对基因上的突变热点进行PCR扩增和测序,并使用旨在检测突变的软件对痕量数据进行分析。测试的七个细胞系具有PIK3Ca突变:两个源自乳腺癌的细胞系,两个来自结肠癌的细胞系,两个来自卵巢癌的细胞系,一个来自肺癌的细胞系。在PIK3Ca突变株中,BRAF和EGFR基因正常。具有突变PIK3Ca的两个细胞系也具有KRAS基因的突变形式。突变状态与NCI-60细胞系可公开获得的基于阵列的基因表达相关。我们发现PIK3Ca突变株中的雌激素受体(ER)和ERBB2的表达水平增加。 PIK3Ca突变状态还与细胞系的化合物筛选数据相关。 PIK3Ca突变细胞系对ER抑制剂他莫昔芬和AKT抑制剂曲西立滨等化合物的敏感性比PIK3Ca正常细胞系高。结果提供了洞察突变体PIK3Ca在致癌信号中的作用,并允许初步鉴定用于治疗具有PIK3Ca突变的癌症的新靶标。

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