domingo, 10 de diciembre de 2017

The feasibility of detecting endometrial and ovarian cancer using DNA methylation biomarkers in cervical scrapings. - PubMed - NCBI

The feasibility of detecting endometrial and ovarian cancer using DNA methylation biomarkers in cervical scrapings. - PubMed - NCBI



 2018 Jan;29(1):e17. doi: 10.3802/jgo.2018.29.e17.

The feasibility of detecting endometrial and ovarian cancer using DNA methylation biomarkers in cervical scrapings.

Abstract

OBJECTIVE:

We hypothesized that DNA methylation of development-related genes may occur in endometrial cancer (EC)/ovarian cancer (OC) and may be detected in cervical scrapings.

METHODS:

We tested methylation status by quantitative methylation-specific polymerase chain reaction for 14 genes in DNA pools of endometrial and OC tissues. Tissues of EC/normal endometrium, OC/normal ovary, were verified in training set using cervical scrapings of 10 EC/10 OC patients and 10 controls, and further validated in the testing set using independent cervical scrapings in 30 EC/30 OC patients and 30 controls. We generated cutoff values of methylation index (M-index) from cervical scrapings to distinguish between cancer patients and control. Sensitivity/specificity of DNA methylation biomarkers in detecting EC and OC was calculated.

RESULTS:

Of 14 genes, 4 (PTGDR, HS3ST2, POU4F3, MAGI2) showed hypermethylation in EC and OC tissues, and were verified in training set. POU4F3 and MAGI2 exhibited hypermethylation in training set were validated in independent cases. The mean M-index of POU4F3 is 78.28 in EC and 20.36 in OC, which are higher than that in controls (6.59; p<0.001 and p=0.100, respectively), and that of MAGI2 is 246.0 in EC and 12.2 in OC, which is significantly higher that than in controls (2.85; p<0.001 and p=0.480, respectively). Sensitivity and specificity of POU4F3/MAGI2 were 83%-90% and 69%-75% for detection of EC, and 61% and 62%-69% for the detection of OC.

CONCLUSION:

The findings demonstrate the potential of EC/OC detection through testing for DNA methylation in cervical scrapings.

KEYWORDS:

DNA Methylation; Endometrial Neoplasms; Ovarian Neoplasms

PMID:
 
29185275
 
PMCID:
 
PMC5709527
 [Available on 2018-01-01]
 
DOI:
 
10.3802/jgo.2018.29.e17
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