Proliferative verrucous and homogeneous Leukoplakias exhibit differential methylation patterns

Author:

Herreros‐Pomares Alejandro12ORCID,Hervás David3ORCID,Bagán Leticia4ORCID,Proaño Alex4,Bagan José2456ORCID

Affiliation:

1. Department of Biotechnology Universitat Politècnica de València Valencia Spain

2. Centro de Investigación Biomédica en Red Cáncer CIBERONC Madrid Spain

3. Departament of Applied Statistics and Operational Research, and Quality Universitat Politècnica de València Valencia Spain

4. Medicina Oral Unit, Stomatology Department Valencia University Valencia Spain

5. Department of Stomatology and Maxillofacial Surgery Hospital General Universitario de Valencia Valencia Spain

6. Precancer and Oral Cancer Research Group of Valencia University Valencia Spain

Abstract

AbstractObjectiveProliferative verrucous leukoplakia (PVL) is considered a clinically distinct entity from other oral leucoplakias (OLs) due to its clinical presentation and evolution. However, molecular differences between them remain unclear. We aimed to determine whether there are methylation differences between PVL and other forms of OLs.Materials and MethodsOral biopsies from 12 patients with PVL, eight patients with homogeneous leucoplakia (HL), and 10 healthy individuals were obtained for a genome‐wide DNA methylation analysis via the Infinium EPIC Platform.ResultsA total of 1815 differentially methylated CpGs were found between PVL and HL, with a prominent state of hypermethylation in HL patients. CpGs covered 813 genes with distinct roles, including cell adhesion, extracellular matrix organization, and cell and synaptic signaling. 43% of these genes had been previously described in cancer and associated with prognosis. We developed a multinomial logistic regression model able to differentiate HL, PVL, and control samples. The model had a cross‐validated estimate of 73% and included differentially methylated cancer‐related genes between the pathological conditions and the healthy donors, including ADNP, BRCA2, CDK13, GNB1, NIN, NUMB, PIK3C2B, PTK2, SHISA4, THSD7B, WWP1, and ZNF292. It also included CpGs covering differentially methylated genes in HL (MEN1 and TNRC6B) and PVL (ACOXL, ADH1B, CAMTA1, CBFA2T3, CPXM2, LRFN2, SORCS2, and SPN).ConclusionsPVL and HL present differential methylation patterns that could be linked to their differential clinical behavior. Our findings show the potential of methylation markers and suggest novel diagnostic biomarkers.

Funder

Instituto de Salud Carlos III

Publisher

Wiley

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