首页> 外文期刊>Lung cancer: Journal of the International Association for the Study of Lung Cancer >ASCL1-coexpression profiling but not single gene expression profiling defines lung adenocarcinomas of neuroendocrine nature with poor prognosis
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ASCL1-coexpression profiling but not single gene expression profiling defines lung adenocarcinomas of neuroendocrine nature with poor prognosis

机译:ASCL1共表达谱而非单基因表达谱定义了神经内分泌性质的肺腺癌,预后较差

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Background: Lung adenocarcinoma is heterogeneous regarding histology, etiology and prognosis. Although there have been several attempts to find a subgroup with poor prognosis, it is unclear whether or not adenocarcinoma with neuroendocrine (NE) nature has unfavorable prognosis. Materials and methods: To elucidate whether a subtype of adenocarcinoma with NE nature has poor prognosis, we performed gene expression profiling by cDNA microarray for 262 Japanese lung cancer and 30 normal lung samples, including 171 adenocarcinomas, 56 squamous cell carcinomas and 35 NE tumors. A co-expression gene set with ASCL1, an NE master gene, was utilized to classify tumors by non-negative matrix factorization, followed by validation using an ASCL1 knock-down gene set in DMS79 cells as well as an independent cohort (n= 139) derived from public microarray databases as a test set. Results: The co-expression gene set classified the adenocarcinomas into alveolar cell (AL), squamoid, and NE subtypes. The NE subtype, which clustered together almost all the NE tumors, had significantly poorer prognosis than the AL subtype that clustered with normal lung samples (p= 0.0075). The knock-down gene set also classified the 171 adenocarcinomas into three subtypes and this NE subtype also had the poorest prognosis. The co-expression gene set classified the independent database-derived American cohort into two subtypes, with the NE subtype having poorer prognosis. None of the single NE gene expression was found to be linked to survival difference. Conclusion: Co-expression gene set with ASCL1, rather than single NE gene expression, successfully identifies an NE subtype of lung adenocarcinoma with poor prognosis.
机译:背景:肺腺癌在组织学,病因学和预后方面是异质的。尽管已经进行了多次尝试来寻找预后不良的亚组,但尚不清楚具有神经内分泌(NE)性质的腺癌是否预后不良。材料和方法:为了阐明具有NE性质的腺癌亚型是否预后不良,我们通过cDNA微阵列技术对262例日本肺癌和30例正常肺样本进行了基因表达谱分析,其中包括171例腺癌,56例鳞状细胞癌和35例NE肿瘤。利用与NE主基因ASCL1共同表达的基因,通过非负矩阵分解对肿瘤进行分类,然后使用DMS79细胞中的ASCL1敲低基因组以及独立队列进行验证(n = 139) )来自公共微阵列数据库作为测试集。结果:共表达基因集将腺癌分为肺泡细胞(AL),鳞状细胞和NE亚型。几乎所有NE肿瘤都聚集在一起的NE亚型的预后要比与正常肺样本聚集的AL亚型的预后差得多(p = 0.0075)。敲除基因组还将171例腺癌分为3个亚型,该NE亚型的预后也最差。共表达基因集将来自独立数据库的美国人群分为两个亚型,NE亚型的预后较差。没有发现单个NE基因表达与生存差异有关。结论:与ASCL1共表达的基因组,而不是单一的NE基因表达组,成功鉴定出了预后不良的NE亚型肺腺癌。

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