Genome-wide DNA Methylation Profiling Reveals Methylation Markers Associated with 3q Gain for Detection of Cervical Precancer and Cancer

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2017 Jan 26

PMID 28119363

Citations 43

Authors

Wina Verlaat

Peter J F Snijders

Putri W Novianti

Saskia M Wilting

Lise M A De Strooper

Geert Trooskens

Johan Vandersmissen

Wim Van Criekinge

G Bea A Wisman

Chris J L M Meijer

Danielle A M Heideman

Renske D M Steenbergen

Affiliations

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Abstract

Epigenetic host cell changes involved in cervical cancer development following a persistent high-risk human papillomavirus (hrHPV) infection, provide promising markers for the management of hrHPV-positive women. In particular, markers based on DNA methylation of tumor suppressor gene promoters are valuable. These markers ideally identify hrHPV-positive women with precancer (CIN2/3) in need of treatment. Here, we set out to identify biologically relevant methylation markers by genome-wide methylation analysis of both hrHPV-transformed cell lines and cervical tissue specimens. Genome-wide discovery by next-generation sequencing (NGS) of methyl-binding domain-enriched DNA (MBD-Seq) yielded 20 candidate methylation target genes. Further verification and validation by multiplex-targeted bisulfite NGS and (quantitative) methylation-specific PCR (MSP) resulted in 3 genes (, and ) that showed a significant increase in methylation with severity of disease in both tissue specimens and cervical scrapes ( < 0.005). The area under the ROC curve for CIN3 or worse varied between 0.86 and 0.89. Within the group of CIN2/3, methylation levels of all 3 genes increased with duration of lesion existence ( < 0.0005), characterized by duration of preceding hrHPV infection, and were significantly higher in the presence of a 3q gain ( < 0.05) in the corresponding tissue biopsy. By unbiased genome-wide DNA methylation profiling and comprehensive stepwise verification and validation studies using and patient-derived samples, we identified 3 promising methylation markers (, and associated with a 3q gain for the detection of cervical (pre)cancer. .

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