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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >MicroRNA expression profiling in human Barrett's carcinogenesis.
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MicroRNA expression profiling in human Barrett's carcinogenesis.

机译:MicroRNA表达谱在人类巴雷特癌变中的作用。

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Barrett's esophagus (BE) is characterized by the native stratified squamous epithelium (N) lining the esophagus being replaced by a columnar epithelium with intestinal differentiation (Barrett's mucosa; BM). BM is considered as the main risk factor for esophageal adenocarcinoma (Barrett's adenocarcinoma; BAc). MicroRNAs (miRNAs) are a class of small noncoding RNAs that control gene expression by targeting messenger RNAs and they are reportedly dysregulated in BM. To test the hypothesis that a specific miRNA expression signature characterizes BM development and progression, we performed miRNA microarray analysis comparing native esophageal mucosa with all the phenotypic lesions seen in the Barrett's carcinogenic process. Specimens were collected from 14 BE patients who had undergone esophagectomy, including: 14 with N, 14 with BM, 7 with low-grade intraepithelial neoplasia, 5 with high-grade intra-epithelial neoplasia and 11 with BAc. Microarray findings were further validated by quantitive real-time polymerase chain reaction and in situ hybridization analyses using a different series of consecutive cases (162 biopsy samples and 5 esophagectomies) of histologically proven, long-segment BE. We identified a miRNA signature of Barrett's carcinogenesis consisting of an increased expression of 6 miRNAs and a reduced expression of 7 miRNAs. To further support these results, we investigated target gene expression using the Oncomine database and/or immunohistochemical analysis. We found that target gene expression correlated significantly with miRNA dysregulation. Specific miRNAs are directly involved in BE progression to cancer. miRNA profiling significantly expands current knowledge on the molecular history of Barrett's carcinogenesis, also identifying molecular markers of cancer progression.
机译:Barrett食道(BE)的特征是食管内衬的天然分层鳞状上皮(N)被具有肠分化的柱状上皮(Barrett粘膜; BM)代替。 BM被认为是食管腺癌(Barrett腺癌; BAc)的主要危险因素。 MicroRNA(miRNA)是一类小的非编码RNA,通过靶向信使RNA来控制基因表达,据报道它们在BM中失调。为了检验特定miRNA表达特征表征BM发育和进展的假说,我们进行了miRNA微阵列分析,将天然食道粘膜与在Barrett致癌过程中看到的所有表型病变进行了比较。从14例行食管切除术的BE患者中收集标本,包括:14例N,14例BM,7例低度上皮内瘤变,5例高度上皮内瘤变和11例BAc。通过定量实时聚合酶链反应和原位杂交分析,使用一系列经组织学证实的长段BE的连续病例(162例活检样本和5例食管切除术),进一步验证了微阵列的发现。我们确定了Barrett癌变的miRNA标志,包括6个miRNA的表达增加和7个miRNA的表达减少。为了进一步支持这些结果,我们使用Oncomine数据库和/或免疫组化分析研究了靶基因的表达。我们发现靶基因表达与miRNA失调显着相关。特定的miRNA直接参与BE向癌症的发展。 miRNA分析显着扩展了有关Barrett致癌分子史的最新知识,还鉴定了癌症进展的分子标记。

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