首页> 外文期刊>The Journal of Urology >CpG island hypermethylation frequently silences FILIP1L isoform 2 expression in prostate cancer
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CpG island hypermethylation frequently silences FILIP1L isoform 2 expression in prostate cancer

机译:CpG岛高甲基化经常沉默前列腺癌中的FILIP1L亚型2表达

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Purpose: Senescence related regulatory pathways serve as barriers to cancer immortalization and progression but they are currently not well defined. FILIP1L is a growth inhibitory gene with multiple isoforms whose expression is increased in senescent prostate and prostate cancer cells, and decreased in many cancers. We investigated whether DNA methylation regulates FILIP1L in senescence and in prostate cancer development. Materials and Methods: FILIP1L mRNA expression was assessed in prostate cancer and associated normal prostate tissues using quantitative polymerase chain reaction. A tissue microarray was constructed using 95 prostate cancer specimens and 45 benign prostate specimens. Vectra? imaging was used to quantitate nuclear and cytoplasmic FILIP1L protein expression. Bisulfite sequencing and Pyrosequencing? were used to assess methylation. Prostate cancer cell lines were treated with 2??-deoxy-5-azacytidine and mRNA expression was assessed. Results: FILIP1L isoform 2 mRNA was increased in replicatively senescent human prostate epithelial cells and decreased in prostate cancer specimens. We verified a reduction in nuclear FILIP1L protein in prostate cancer using tissue microarrays (p = 0.006). A CpG island 5?? of the isoform 2 translational start site was identified that showed hypermethylation in prostate cancer cell lines and tumors compared to normal prostate cells and tissues. Pyrosequencing confirmed FILIP1L hypermethylation in all 14 tumors compared to paired normal tissues (p <0.0001). Isoform 2 expression was induced in prostate cancer cell lines using 2??-deoxy-5-azacytidine. Conclusions: FILIP1L isoform 2 is one of the most commonly hypermethylated genes in prostate cancer. It may serve as an important marker of prostate cancer. Isoform 2 expression is associated with senescence and its down-regulation may represent an early important biological event in prostate cancer development. ? 2013 American Urological Association Education and Research, Inc.
机译:目的:衰老相关的调节途径成为癌症永生化和进展的障碍,但目前尚不明确。 FILIP1L是具有多种同工型的生长抑制基因,其表达在衰老的前列腺和前列腺癌细胞中增加,而在许多癌症中减少。我们调查了DNA甲基化是否在衰老和前列腺癌的发展中调节FILIP1L。材料和方法:使用定量聚合酶链反应评估FILIP1L mRNA在前列腺癌和相关正常前列腺组织中的表达。使用95个前列腺癌标本和45个良性前列腺标本构建了组织微阵列。 Vectra?成像用于定量核和细胞质FILIP1L蛋白表达。亚硫酸氢盐测序和焦磷酸测序?被用来评估甲基化。用2′-脱氧-5-氮胞苷处理前列腺癌细胞系并评估mRNA表达。结果:FILIP1L亚型2 mRNA在复制性衰老的人前列腺上皮细胞中增加,而在前列腺癌标本中减少。我们使用组织芯片验证了前列腺癌中核FILIP1L蛋白的减少(p = 0.006)。 CpG岛5?与正常前列腺细胞和组织相比,鉴定出同工型2翻译起始位点的80%显示出在前列腺癌细胞系和肿瘤中的高甲基化。与配对的正常组织相比,焦磷酸测序证实了所有14种肿瘤中的FILIP1L甲基化程度较高(p <0.0001)。使用2β-脱氧-5-氮杂胞苷在前列腺癌细胞系中诱导同工型2表达。结论:FILIP1L同工型2是前列腺癌中最常见的高甲基化基因之一。它可能是前列腺癌的重要标志。 Isoform 2表达与衰老相关,其下调可能代表前列腺癌发展中的早期重要生物学事件。 ? 2013美国泌尿科协会教育与研究公司

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