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Global molecular dysfunctions in gastric cancer revealed by an integrated analysis of the phosphoproteome and transcriptome

机译:磷酸化蛋白质组和转录组的综合分析揭示了胃癌的全球分子功能异常

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We integrated LC-MS/MS-based and protein antibody array-based proteomics with genomics approaches to investigate the phosphoproteome and transcriptome of gastric cancer cell lines and endoscopic gastric biopsies from normal subjects and patients with benign gastritis or gastric cancer. More than 3,000 non-redundant phosphorylation sites in over 1,200 proteins were identified in gastric cancer cells. We correlated phosphoproteome data with transcriptome data sets and reported the expression of 41 protein kinases, 5 phosphatases and 65 phosphorylated mitochondrial proteins in gastric cancer cells. Transcriptional expression levels of 190 phosphorylated proteins were >2-fold higher in gastric cancer cells compared to normal stomach tissue. Pathway analysis demonstrated over-presentation of DNA damage response pathway and underscored critical roles of phosphorylated p53 in gastric cancer. This is the first study to comprehensively report the gastric cancer phosphoproteome. Integrative analysis of the phosphoproteome and transcriptome provided an expansive view of molecular signaling pathways in gastric cancer.
机译:我们将基于LC-MS / MS和蛋白质抗体阵列的蛋白质组学与基因组学方法相结合,以研究正常受试者和良性胃炎或胃癌患者的胃癌细胞系和内窥镜胃活检组织的磷酸化蛋白质组和转录组。在胃癌细胞中鉴定出1,200多种蛋白质中的3,000多个非冗余磷酸化位点。我们将磷酸化蛋白质组数据与转录组数据集相关联,并报道了胃癌细胞中41种蛋白激酶,5种磷酸酶和65种磷酸化的线粒体蛋白的表达。与正常胃组织相比,胃癌细胞中190种磷酸化蛋白的转录表达水平高2倍以上。途径分析表明,DNA损伤反应途径过多,并强调了磷酸化p53在胃癌中的关键作用。这是首次全面报道胃癌磷酸化蛋白质组的研究。磷酸化蛋白质组和转录组的综合分析提供了胃癌分子信号通路的广阔视野。

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