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Detection of hTERC and c-MYC genes in cervical epithelial exfoliated cells for cervical cancer screening

机译:检测宫颈上皮脱落细胞中hTERC和c-MYC基因以筛查宫颈癌

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Cervical cancer is the principal cause of mortality due to cancer in women worldwide. New predictive markers may increase survival rates by improving the treatment of patients at a high risk for cancer. This study was carried out to investigate the amplification of human telomerase RNA component (hTERC) or/and c-MYC in cervical epithelial exfoliated cells for cervical carcinoma screening. We collected 171?specimens. including speciments from normal cervix, benign lesions, cervical intraepithelial neoplasia (CIN)1, CIN2 and CIN3, or carcinoma in?situ, as well as invasive cervical squamous cell carcinoma. Fluorescence in?situ hybridization (FISH) was performed to detect alterations in hTERC and c-MYC expression. We analyzed the area under the receiver operating characteristic (ROC) curve (AUC), as well as the sensitivity and specificity of single screening and conjoined screening. There was a trend toward an increasing amplification of 2?genes with the increasing severity of cervical lesions. ROC curve analysis demonstrated that the AUC values of the hTERC gene for the screening of different cervical lesions were >0.8. Compared with the hTERC gene, the AUC of the c-MYC gene for the screening of ≥CIN3 was >0.8 and the AUC for the screening of other cervical lesions was >0.7. For the screening of cervical lesions above the grade of benign lesions, cytological diagnosis was superior to the gene detection with significant differences. For the screening of cervical lesions >CIN1, there were no statistically significant differences (P>0.05) between the hTERC gene and cytological diagnosis, whereas the screening results of c-MYC detection and cytological diagnosis differed significantly (PCIN2 or >CIN3, the detection of hTERC and c-MYC genes and cytological diagnosis had similar screening results with no statistically significant differences (P>0.05). In conclusion, using FISH to detect the amplification of hTERC or/and c-MYC on cervical epithelial exfoliated cells may be a useful and specific screening method for precancerous lesions.
机译:宫颈癌是全世界女性因癌症而致死的主要原因。新的预测标志物可能会通过改善对癌症高风险患者的治疗来提高生存率。这项研究是为了研究宫颈癌上皮脱落细胞中人端粒酶RNA成分(hTERC)或c-MYC的扩增而进行的。我们收集了171个样本。包括来自正常宫颈,良性病变,宫颈上皮内瘤变(CIN)1,CIN2和CIN3或原位癌以及浸润性宫颈鳞状细胞癌的标本。进行荧光原位杂交(FISH)以检测hTERC和c-MYC表达的变化。我们分析了接受者工作特征(ROC)曲线(AUC)下的面积,以及单次筛选和联合筛选的敏感性和特异性。随着宫颈病变严重程度的增加,2α基因的扩增也有增加的趋势。 ROC曲线分析表明,用于筛选不同宫颈病变的hTERC基因的AUC值> 0.8。与hTERC基因相比,用于筛选≥CIN3的c-MYC基因的AUC> 0.8,而用于筛选其他宫颈病变的AUC> 0.7。对于筛查良性病变以上的宫颈病变,细胞学诊断优于基因检测,且有显着差异。对于宫颈病变> CIN1的筛查,hTERC基因与细胞学诊断之间无统计学差异(P> 0.05),而c-MYC检测和细胞学诊断的筛查结果有显着差异(PCIN2或> CIN3, hTERC和c-MYC基因的检测及细胞学诊断结果相似,无统计学差异(P> 0.05),因此,用FISH检测宫颈上皮脱落细胞中hTERC或c-MYC的扩增可能癌前病变的有用且特异性的筛查方法。

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