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Methylation variable position profiles of hMLH1 promoter CpG islands in human sporadic colorectal carcinoma

机译:人类散发性结直肠癌中hMLH1启动子CpG岛的甲基化可变位置谱

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摘要

Aberrant hypermethylation of CpG islands (CGIs) in hMLH1 promoter regions has been well known to play an important role in the tumorigenesis of human sporadic colorectal carcinoma (SCRC). In this study, bisulfite sequencing was performed to analyze the methylation variable positions (MVPs) profiles of hMLH1 promoter CGIs in 30 clinical SCRC patients, and further analysis was carried out to evaluate the associations between the CGI methylation and the clinicopathological features in SCRC. Among the 2 CGIs in the hMLH1 promoter, that is, CGI-I and CGI-II, 20% (6/30) and 13% (4/30) of the patients had methylated CGI-I and CGI-II, respectively. Suppressed expression of hMLH1was significantly correlated with methylation of CGI-I but not CGI-II. Further analysis of the MVP profiles of CGI-I showed that most of the MVPs were hypermethylated and others were poorly methylated or unmethylated. The profiles could be classified into at least 4 groups based on the methylation status of 3 MVPs at positions 21 to 23 in CGI-I. All 6 patients with methylated CGI-I belonged to group I. This result suggests that the above 3 MVPs in CGI-I should be a targeted region to further analyze the epigenetic features of hMLH1 in human SCRC. Our results further suggest that MVP profiling is useful for identifying the aberrantly methylated CGIs associated with suppressed gene expression.
机译:众所周知,hMLH1启动子区域的CpG岛(CGI)异常甲基化在人类散发性结直肠癌(SCRC)的肿瘤发生中起重要作用。在这项研究中,进行亚硫酸氢盐测序以分析30例临床SCRC患者中hMLH1启动子CGI的甲基化可变位置(MVPs)谱,并进行进一步分析以评估CGI甲基化与SCRC临床病理特征之间的关联。在hMLH1启动子的2个CGI中,即CGI-I和CGI-II,分别有20%(6/30)和13%(4/30)的患者甲基化了CGI-I和CGI-II。 hMLH1的抑制表达与CGI-I的甲基化显着相关,而与CGI-II无关。对CGI-1的MVP谱图的进一步分析表明,大多数MVP都被甲基化,而其他MVP则被甲基化或未甲基化。基于CGI-1中21至23位的3个MVP的甲基化状态,可将概况分为至少4个组。所有6例甲基化CGI-1患者均属于I组。这一结果表明,CGI-1中的上述3个MVP应该成为进一步分析hMLH1在人SCRC中的表观遗传学特征的目标区域。我们的结果进一步表明,MVP分析可用于鉴定与抑制的基因表达相关的异常甲基化的CGI。

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