Low methylation marker levels among human papillomavirus‐vaccinated women with cervical high‐grade squamous intraepithelial lesions

Author:

Louvanto Karolina12ORCID,Verhoef Lisanne34ORCID,Pimenoff Ville5ORCID,Eriksson Tiina1,Leppälä Siiri1,Lagheden Camilla5,Gray Penelope5ORCID,Scibior‐Bentkowska Dorota6,Sumiec Elizabeth6,Nieminen Pekka7,Dillner Joakim5ORCID,Berkhof Johannes8,Meijer Chris J. L. M.34,Lehtinen Matti15ORCID,Nedjai Belinda6,Heideman Daniëlle A. M.34

Affiliation:

1. Faculty of Medicine and Health Technology Tampere University Tampere Finland

2. Department of Obstetrics and Gynecology Tampere University Hospital Tampere Finland

3. Pathology Amsterdam UMC, Vrije Universiteit Amsterdam Amsterdam The Netherlands

4. Imaging and Biomarkers Cancer Center Amsterdam Amsterdam The Netherlands

5. Unit of Cervical Cancer Elimination, Department of Clinical Science, Intervention and Technology CLINTEC, Karolinska Institute Stockholm Sweden

6. Centre for Cancer Screening, Prevention and Early Detection (SPED), Wolfson Institute of Population Health Queen Mary University of London London UK

7. Department of Obstetrics and Gynecology Helsinki University Hospital Helsinki Finland

8. Epidemiology and Data Science Amsterdam UMC, Vrije Universiteit Amsterdam Amsterdam The Netherlands

Abstract

AbstractCervical cancer screening programs, including triage tests, need redesigning as human papillomavirus (HPV)‐vaccinated women are entering the programs. Methylation markers offer a potential solution to reduce false‐positive rates by identifying clinically relevant cervical lesions with progressive potential. In a nested case–control study, 9242 women who received the three‐dose HPV16/18‐vaccine at ages 12–15 or 18 in a community‐randomized trial were included. Subsequently, they were re‐randomized for either frequent or infrequent cervical cancer screening trials. Over a 15‐year post‐vaccination follow‐up until 2022, 17 high‐grade squamous intraepithelial lesion (HSIL) and 15 low‐grade (LSIL) cases were identified at the 25‐year screening round, alongside 371 age and community‐matched HPV16/18‐vaccinated controls. Methylation analyses were performed on cervical samples collected at age 25, preceding histologically confirmed LSIL or HSIL diagnoses. DNA methylation of viral (HPV16/18/31/33) and host‐cell genes (EPB41L3, FAM19A4, and miR124‐2) was measured, along with HPV‐genotyping. No HPV16/18 HSIL cases were observed. The predominant HPV‐genotypes were HPV52 (29.4%), HPV59/HPV51/HPV58 (each 23.5%), and HPV33 (17.7%). Methylation levels were generally low, with no significant differences in mean methylation levels of viral or host‐cell genes between the LSIL/HSIL and controls. However, a significant difference in methylation levels was found between HSIL cases and controls when considering a combination of viral genes and EPB41L3 (p value = .0001). HPV‐vaccinated women with HSIL had HPV infections with uncommon HPV types that very rarely cause cancer and displayed low methylation levels. Further investigation is warranted to understand the likely regressive nature of HSIL among HPV‐vaccinated women and its implications for management.

Publisher

Wiley

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