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Detection of SNCA and FBN1 methylation in the stool as a biomarker for colorectal cancer

机译:检测粪便中的SNCA和FBN1甲基化作为结直肠癌的生物标志物

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Aim. We examined the methylation status of SNCA and FBN1 genes in patients' paired tissue and stool samples for detection of colorectal cancer (CRC). Patients and Methods. 89 DNA tissue samples (normal/cancer) and corresponding stool samples were analyzed in our study. In addition, 30 stool samples were collected as healthy controls. Results. The methylation level of those samples was measured by methylation-specific polymerase chain reaction (MSP). The result shows that compared with the paired controls, both SNCA and FBN1 were significantly hypermethylated in CRC patients in tissue samples (P<0.001). In the stool samples, hypermethylated SNCA and FBN1 were detected to be significantly higher than that in normal stool samples (P<0.001). The combined sensitivity of at least one positive among the two markers in stool samples was 84.3%, with a specificity of 93.3%. In addition, our experiment suggested that the positive rates of SNCA and FBN1 in Dukes A stage were significantly higher than that of FOBT (P=0.039; P=0.006, resp.). Conclusion. We concluded that methylation testing of SNCA and FBN1 genes in stool sample may offer a good alternative in a simple, promising, and noninvasive detection of colorectal cancer. ? 2015 Wen-han Li et al.
机译:目的。我们检查了患者配对组织和粪便样品中SNCA和FBN1基因的甲基化状态,用于检测结直肠癌(CRC)。患者和方法。在我们的研究中分析了89个DNA组织样品(正常/癌症)和相应的粪便样品。此外,收集30种粪便样品作为健康对照。结果。这些样品的甲基化水平通过甲基化特异性聚合酶链式反应(MSP)测量。结果表明,与配对对照相比,SNCA和FBN1在组织样品中的CRC患者中显着高甲基化(P <0.001)。在粪便样品中,检测到高甲基化的SNCA和FBN1明显高于正常粪便样品(P <0.001)。粪便样品中两种标记中至少一个正阳性的组合敏感性为84.3%,特异性为93.3%。此外,我们的实验表明,Dukes中SnCA和FBN1的阳性率显着高于FOBT(P = 0.039; P = 0.006,REAC)。结论。我们得出结论,粪便样品中SNCA和FBN1基因的甲基化检测可以在简单,有前途和非侵入性的结肠直肠癌中提供良好的替代方案。还2015 Wen-Han Li等人。

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