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PTEN gene is infrequently hypermethylated in human esophageal squamous cell carcinoma

机译:PTEN基因在人食管鳞状细胞癌中很少发生甲基化

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摘要

Whether promoter hypermethylation of phosphatase and tensin homologue deleted from chromosome 10 (PTEN) is associated with loss of PTEN expression was not yet elucidated in esophageal squamous cell carcinoma (ESCC). The methylation status of PTEN gene was evaluated in 74 ESCC specimens and four esophageal cancer cell lines. Its association with clinicopathological factors or the prognosis was investigated by statistical analysis. We further measured messenger RNA (mRNA) and protein level of PTEN by quantitative RT-PCR and immunohistochemistry and studied the role of PTEN hypermethylation in loss of PTEN expression in clinical samples. Next, demethylation of PTEN gene with 5-azaC in EC9706 was performed to confirm the clinical findings. PTEN methylation was only found in 14 (18.9 %) of 74 ESCC tumor samples and one (EC9706) of four esophageal cancer cell lines. PTEN methylation was not statistically associated with clinicopathological factors and the prognosis (p > 0.05). In addition, 41 patients (55.4 %) and 38 patients (51.4 %) showed reduced mRNA level of PTEN and negative expression of PTEN protein in ESCC tumors, respectively. Detailed analysis indicated that PTEN methylation was a possible mechanism of loss of PTEN expression in ESCC, and further 5-azaC demethylation revealed inversed methylation status and increased mRNA or protein level of PTEN in EC9706. However, the role of PTEN methylation in loss of PTEN expression was still limited due to low frequency of methylation in ESCC. PTEN hypermethylation is a rare event and did not play an important role in the prognosis and loss of PTEN expression in ESCC.
机译:在食管鳞状细胞癌(ESCC)中尚未阐明从10号染色体(PTEN)缺失的磷酸酶和张力蛋白同源物的启动子高甲基化与PTEN表达的丧失是否相关。在74个食管鳞癌标本和4个食道癌细胞系中评估了PTEN基因的甲基化状态。通过统计分析研究其与临床病理因素或预后的关系。我们通过定量RT-PCR和免疫组织化学进一步测量了信使RNA(mRNA)和PTEN蛋白水平,并研究了PTEN高甲基化在临床样品中PTEN表达缺失中的作用。接下来,在EC9706中用5-azaC对PTEN基因进行脱甲基,以确认临床发现。 PTEN甲基化仅在74个ESCC肿瘤样本中的14个(18.9%)和四个食管癌细胞系中的一个(EC9706)中发现。 PTEN甲基化与临床病理因素和预后无统计学相关性(p> 0.05)。另外,在ESCC肿瘤中,分别有41例患者(55.4%)和38例患者(51.4%)表现出PTEN mRNA水平降低和PTEN蛋白阴性表达。详细的分析表明,PTEN甲基化是ESCC中PTEN表达缺失的可能机制,进一步的5-azaC去甲基化揭示了EC9706中甲基化状态反转和PTEN的mRNA或蛋白质水平升高。然而,由于ESCC中甲基化的频率低,PTEN甲基化在PTEN表达丧失中的作用仍然受到限制。 PTEN高甲基化是罕见的事件,并且在ESCC中PTEN表达的预后和丧失中不发挥重要作用。

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