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首页> 外文期刊>Journal of Gynecologic Oncology >Role of 5'-CpG island hypermethylation of the FHIT gene in cervical carcinoma
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Role of 5'-CpG island hypermethylation of the FHIT gene in cervical carcinoma

机译:FHIT基因的5'-CpG岛甲基化在宫颈癌中的作用

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Objective The abnormal expression of fragile histidine triad ( FHIT ) gene has been frequently reported in a variety of epithelial malignancies including cervical carcinoma. Furthermore, in a recent study it was proposed that transcriptional inactivation of FHIT , as a consequence of aberrant 5'-CpG island methylation, plays an important role in the carcinogenesis of human cervical carcinoma. The authors sought to determine whether abnormal FHIT transcription occurs in human cervical carcinoma, and if so, whether this abnormal expression is associated with aberrant 5'-CpG island methylation. In addition, the clinical significance of FHIT inactivation was investigated in Korean women with cervical cancer. Methods To examine for abnormal transcripts of the FHIT gene, quantitative RT-PCR, genomic DNA-PCR and nonisotopic RT-PCR-SSCP analysis were performed using the standard method. The methylation status was determined by methylation specific PCR and bisulfite DNA sequencing. Results The FHIT gene was down-regulated in 15 of 58 (25.9%) cervical carcinomas. FHIT promoter hypermethylation was detected in 15 of 15 (100%) abnormally expression in cervical carcinomas. Bisulfite DNA sequencing confirmed these findings and a significant correlation was found between CpG site hypermethylation and low FHIT expression. However, no significant correlation was found between reduced FHIT expression and clinicopathological characteristics. Conclusion In this study, FHIT inactivation in cervical cancer was found to be strongly correlated with 5'-CpG island hypermethylation rather than a genetic alteration. Furthermore, no significant relation was found between a lack of FHIT expression and the prognostic factors of cervical cancer in our Korean cohort.
机译:目的脆性组氨酸三联体(FHIT)基因的异常表达在包括宫颈癌在内的多种上皮恶性肿瘤中屡见报道。此外,在最近的研究中提出,由于5'-CpG岛甲基化异常,FHIT的转录失活在人宫颈癌的癌变中起重要作用。作者试图确定人宫颈癌中是否发生了异常的FHIT转录,如果存在,则该异常表达是否与异常的5'-CpG岛甲基化有关。此外,对韩国宫颈癌女性进行FHIT失活的临床意义进行了研究。方法为了检查FHIT基因的异常转录本,使用标准方法进行了定量RT-PCR,基因组DNA-PCR和非同位素RT-PCR-SSCP分析。甲基化状态通过甲基化特异性PCR和亚硫酸氢盐DNA测序确定。结果58例宫颈癌中有15例(25.9%)的FHIT基因被下调。在宫颈癌的15个异常表达中,有15个(100%)异常检测到FHIT启动子甲基化过高。亚硫酸氢盐DNA测序证实了这些发现,并且发现CpG位点甲基化过度与FHIT低表达之间存在显着相关性。但是,在降低的FHIT表达与临床病理特征之间未发现显着相关性。结论在这项研究中,发现宫颈癌的FHIT失活与5'-CpG岛超甲基化高度相关,而不与基因改变密切相关。此外,在我们的韩国队列中,FHIT表达的缺乏与宫颈癌的预后因素之间没有发现显着关系。

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