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Targeted Exome Sequencing of the Cancer Genome in Patients with Very High-risk Bladder Cancer

机译:极高风险膀胱癌患者癌症基因组的靶向外显子组测序

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We completed targeted exome sequencing of the tumors of 50 patients with pTis-pT4b bladder cancer. Mutations were categorized by type, stratified against previously identified cancer loci in the Catalogue of Somatic Mutations in Cancer and The Cancer Genome Atlas databases, and evaluated in pathway analysis and comutation plots. We analyzed mutation associations with receipt of neoadjuvant chemotherapy, nodal involvement, metastatic disease development, and survival. Compared with The Cancer Genome Atlas, we found higher mutation rates in genes encoding products involved in epigenetic regulation and cell cycle regulation. Of the pathways examined, PI3K/mTOR and Cell Cycle/DNA Repair exhibited the greatest frequencies of mutation. RB1 and TP53, as well as NF1 and PIK3CA were frequently comutated. We identified no association between mutations in specific genes and key clinical outcomes of interest when corrected for multiple testing. Discovery phase analysis of the somatic mutations in 50 high-risk bladder cancer patients revealed novel mutations and mutational patterns, which may be useful for developing targeted therapy regimens or new biomarkers for patients at very high risk of disease metastasis and death.
机译:我们完成了50例pTis-pT4b膀胱癌患者肿瘤的靶向外显子组测序。根据类型对突变进行分类,并根据《癌症中的体细胞突变目录》和《癌症基因组图谱》数据库中先前确定的癌症位点进行分层,并在途径分析和减法图中进行评估。我们分析了新辅助化疗,淋巴结受累,转移性疾病发展和生存与接收突变。与《癌症基因组图谱》相比,我们发现编码表观遗传调控和细胞周期调控产物的基因突变率更高。在检查的途径中,PI3K / mTOR和细胞周期/ DNA修复表现出最大的突变频率。经常使用RB1和TP53以及NF1和PIK3CA。当进行多次测试校正后,我们发现特定基因的突变与关注的关键临床结果之间没有关联。在50位高危膀胱癌患者中进行的体细胞突变的发现阶段分析揭示了新的突变和突变模式,这对于开发靶向治疗方案或新的生物标志物可能非常有用,可用于极高的疾病转移和死亡风险患者。

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