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Discovery and analysis of pancreatic adenocarcinoma genes using cDNA microarrays.

机译:使用cDNA微阵列发现和分析胰腺腺癌基因。

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AIM: To study the pathogenetic processes and the role of gene expression by microarray analyses in expediting our understanding of the molecular pathophysiology of pancreatic adenocarcinoma, and to identify the novel cancer-associated genes. METHODS: Nine histologically defined pancreatic head adenocarcinoma specimens associated with clinical data were studied. Total RNA and mRNA were isolated and labeled by reverse transcription reaction with Cy5 and Cy3 for cDNA probe. The cDNA microarrays that represent a set of 4 096 human genes were hybridized with labeled cDNA probe and screened for molecular profiling analyses. RESULTS: Using this methodology, 184 genes were screened out for differences in gene expression level after nine couples of hybridizations. Of the 184 genes, 87 were upregulated and 97 downregulated, including 11 novel human genes. In pancreatic adenocarcinoma tissue, several invasion and metastasis related genes showed their high expression levels, suggesting that poor prognosis of pancreatic adenocarcinoma might have a solid molecular biological basis. CONCLUSION: The application of cDNA microarray technique for analysis of gene expression patterns is a powerful strategy to identify novel cancer-associated genes, and to rapidly explore their role in clinical pancreatic adenocarcinoma. Microarray profiles provide us new insights into the carcinogenesis and invasive process of pancreatic adenocarcinoma. Our results suggest that a highly organized and structured process of tumor invasion exists in the pancreas.
机译:目的:通过微阵列分析研究胰腺癌的致病过程和基因表达的作用,以加深对胰腺腺癌分子病理生理的认识,并鉴定与癌症有关的新基因。方法:对9例组织学定义的胰头腺癌标本与临床资料进行了研究。分离总RNA和mRNA并通过与Cy5和Cy3的逆转录反应标记cDNA探针。代表一组4 096个人类基因的cDNA微阵列与标记的cDNA探针杂交,并进行分子分析分析。结果:使用这种方法,经过九对杂交后,筛选出184个基因的基因表达水平差异。在184个基因中,有87个被上调,而97个被下调,其中包括11个新的人类基因。在胰腺腺癌组织中,一些与侵袭和转移相关的基因均显示其高表达水平,提示胰腺腺癌的不良预后可能具有坚实的分子生物学基础。结论:cDNA微阵列技术在分析基因表达模式中的应用是鉴定新的癌症相关基因并迅速探索其在临床胰腺癌中的作用的有力策略。微阵列概况为我们提供了胰腺癌的发生和浸润过程的新见解。我们的结果表明胰腺中存在高度组织化和结构化的肿瘤侵袭过程。

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