Molecular Heterogeneity in Human Papillomavirus-dependent and -independent Vulvar Carcinogenesis

Overview

Journal Cancer Med

Specialty Oncology

Date 2018 Jul 22

PMID 30030907

Citations 12

Authors

Dorian R A Swarts

Quirinus J M Voorham

Annina P van Splunter

Saskia M Wilting

Daoud Sie

Divera Pronk

Marc van Beurden

Danielle A M Heideman

Peter J F Snijders

Chris J L M Meijer

Renske D M Steenbergen

Maaike C G Bleeker

Affiliations

Soon will be listed here.

Abstract

Vulvar squamous cell carcinoma (VSCC) and precancerous vulvar intraepithelial neoplasia (VIN) can develop through human papillomavirus (HPV)-dependent and -independent pathways, indicating a heterogeneous disease. Only a minority of VIN progress, but current clinicopathological classifications are insufficient to predict the cancer risk. Here we analyzed copy number alterations (CNA) to assess the molecular heterogeneity of vulvar lesions in relation to HPV and cancer risk. HPV-status and CNA by means of whole-genome next-generation shallow-sequencing were assessed in VSCC and VIN. The latter included VIN of women with associated VSCC (VIN ) and women who did not develop VSCC during follow-up (VIN ). HPV-testing resulted in 41 HPV-positive (16 VIN , 14 VIN , and 11 VSCC) and 24 HPV-negative (11 VIN and 13 VSCC) lesions. HPV-positive and -negative VSCC showed a partially overlapping pattern of recurrent CNA, including frequent gains of 3q and 8q. In contrast, amplification of 11q13/cyclinD1 was exclusively found in HPV-negative lesions. HPV-negative VIN had less CNA than HPV-negative VSCC (P = .009), but shared chromosome 8 alterations. HPV-positive VIN had less CNA than VIN (P = .022). Interestingly, 1pq gain was detected in 81% of HPV-positive VIN and only in 21% of VIN (P = .001). In conclusion, HPV-dependent and -independent vulvar carcinogenesis is characterized by distinct CNA patterns at the VIN stage, while more comparable patterns are present at the cancer stage. Cancer risk in VIN seems to be reflected by the extent of CNA, in particular chromosome 1 gain in HPV-positive cases.

Citing Articles

Incidence and Risk Factors for Recurrence and Progression of HPV-Independent Vulvar Intraepithelial Neoplasia.

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Differentiated vulvar intraepithelial neoplasia long-term follow up and prognostic factors: An analysis of a large historical cohort.

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Biomarker Expression in Multifocal Vulvar High-Grade Squamous Intraepithelial Lesions.

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Exploring Differentially Methylated Genes in Vulvar Squamous Cell Carcinoma.

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