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Screening for differentially methylated genes among human colorectal cancer tissues and normal mucosa by microarray chip

机译:利用微阵列芯片筛选大肠癌组织和正常黏膜中差异甲基化基因

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摘要

High density DNA methylation microarrays were used to study the differences of gene methylation level in six pairs of colorectal cancer (CRC) and adjacent normal mucosa. We analyzed the profile of methylated genes by NimbleGen Microarray and the biologic functions by NIH-NAVID. In addition, preliminary validation studies were done in six pairs of samples by MSP (methylation-specific PCR). A total of 4,644 genes had a difference in methylation levels. Among them 2,296 were hypermethylated (log2ratio > 1), 2,348 genes were hypomethylated (log2ratio < −1), in which 293 hypermethylated and 313 hypomethylated genes were unmapped according to the NIH-NAVID. All these genes were randomly distributed on all the chromosomes. However, chromosome 1 contained the most of the hypermethylated genes (232 genes), followed by chromosome 19 (149 genes), chromosome 11 (144 genes), chromosome 2 (141 genes), chromosomes 3 (127 genes). Through the analysis of the statistics, There were 2 hypermethylated/3 hypomethylated genes involved in six pairs of samples simultaneously, followed by 10/14 in five samples, 34/37 in four samples, 101/113 in three samples, 341/377 in two samples, 1,808/1,804 in one sample. According to gene ontology analysis, some physiological processes play important roles in the cell division and the development of tumor, such as apoptosis, DNA repair, immune, cell cycle, cell cycle checkpoint, cell adhesion and invasion etc. Through Preliminary validation, there were two genes (St3gal6, Opcml) in thirty top-ranking genes shown hypermethylated in six pairs of CRC and adjacent normal mucosa. Conclusions High density DNA methylation microarrays is an effective method for screening aberrantly methylated genes in CRC. The methylated genes should be further studied for diagnostic or prognostic markers for CRC.
机译:高密度DNA甲基化微阵列用于研究六对结直肠癌(CRC)和邻近正常黏膜中基因甲基化水平的差异。我们通过NimbleGen Microarray分析了甲基化基因的概况,并通过NIH-NAVID分析了其生物学功能。此外,通过MSP(甲基化特异性PCR)对六对样品进行了初步验证研究。共有4,644个基因的甲基化水平有所不同。其中2,296个被高甲基化(log2ratio> 1),2,348个基因被低甲基化(log2ratio <-1),其中293个高甲基化的基因和313个低甲基化的基因没有根据NIH-NAVID进行映射。所有这些基因都随机分布在所有染色体上。然而,染色体1包含大多数的高甲基化基因(232个基因),其次是染色体19(149个基因),染色体11(144个基因),染色体2(141个基因),染色体3(127个基因)。通过统计分析,六对样本中同时涉及2个高甲基化/ 3个亚甲基化基因,其次是五个样本中的10/14,四个样本中的34/37,三个样本中的101/113,341/377。两个样本,一个样本中为1,808 / 1,804。根据基因本体分析,一些生理过程在细胞分裂和肿瘤的发展中起着重要作用,例如凋亡,DNA修复,免疫,细胞周期,细胞周期检查点,细胞粘附和侵袭等。在三十对排名靠前的基因中,有两个基因(St3gal6,Opcml)在六对CRC和邻近正常黏膜中显示出高度甲基化。结论高密度DNA甲基化微阵列是一种筛选CRC中异常甲基化基因的有效方法。甲基化的基因应进一步研究以作为CRC的诊断或预后指标。

著录项

  • 来源
    《Molecular Biology Reports》 |2013年第5期|3457-3464|共8页
  • 作者单位

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat-sen University">(2);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat-sen University">(2);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Sun Yat-sen University">(3);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

    Department of Colorectal Surgery The Sixth Affiliated Hospital Sun Yat-sen University">(1);

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Methylation; Colorectal cancer; Microarray; Epigenetics;

    机译:甲基化大肠癌;微阵列;表观遗传学;

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