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CADM1 and MAL methylation status in cervical scrapes is representative of the most severe underlying lesion in women with multiple cervical biopsies
Authors:Romy van Baars  Jacolien van der Marel  Agata Rodriquez‐Manfredi  Bram ter Harmsel  Henk AM van den Munckhof  Jaume Ordi  Marta del Pino  Miekel M van de Sandt  N Wentzensen  Wim GV Quint
Institution:1. DDL Diagnostic Laboratory, Rijswijk, The Netherlands;2. Department of Obstetrics and Gynaecology, Hospital Clínic, Barcelona, Spain;3. Roosevelt Kliniek, Leiden, The Netherlands;4. Department of Pathology, CRESIB (Centre De Recerca En Salut Internacional De Barcelona)—Hospital Clinic, Faculty of Medicine‐University of Barcelona, Barcelona, Spain;5. Division of Cancer Epidemiology and Genetics, National Cancer Institute, Bethesda, MD
Abstract:Recent studies have shown that CADM1/MAL methylation levels in cervical scrapes increase with severity and duration of the underlying cervical intraepithelial neoplasia (CIN) lesion. Multiple lesions of different histological grades and duration are frequently present on the cervix. To gain more insight into the possible epigenetic heterogeneity and its consequences for the methylation status in cervical scrapes, we performed an exploratory study of CADM1/MAL methylation in different grades of CIN lesions present in women with multiple cervical biopsies. CADM1‐M18 and MAL‐M1 methylation was assessed using a standardised, multiplex, quantitative methylation specific PCR on 178 biopsies with various grades of CIN in 65 women, and in their corresponding cervical scrapes. CADM1/MAL methylation positivity increased with disease severity, from 5.5% in normal biopsies to 63.3% and 100% in biopsies with CIN3 and cervical cancer, respectively. In the majority (8/9) of women where besides a CIN2/3 lesion a biopsy from normal cervical tissue was present, the CIN2/3 biopsy was CADM1/MAL methylation positive and the normal biopsy was CADM1/MAL methylation negative. A good concordance (78%) was found between CADM1/MAL methylation results on the scrapes and the biopsy with the worst diagnosis, particularly between samples of women with CIN3 and cervical cancer (92% and 100% concordance, respectively). Thus, in women with multiple cervical biopsies, CADM1/MAL methylation increases with severity of the lesion and is lesion‐specific. CADM1/MAL methylation status in cervical scrapes appears to be representative of the worst underlying lesion, particularly for CIN3 and cervical cancer.
Keywords:DNA methylation  tumour suppressor genes  human papillomavirus  cervical intraepithelial neoplasia  cervical cancer
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