Use of Allelic Loss to Predict Malignant Risk for Low-grade Oral Epithelial Dysplasia

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2000 Feb 26

PMID 10690511

Citations 107

Authors

M P Rosin

X Cheng

C Poh

W L Lam

Y Huang

J Lovas

K Berean

J B Epstein

R Priddy

N D Le

L Zhang

Affiliations

Soon will be listed here.

Abstract

One of the best approaches to identifying genetic changes critical to oral cancer progression is to compare progressing and nonprogressing oral premalignant lesions. However, such samples are rare, and they require long-term follow-up. The current study used the large archive network and clinical database in British Columbia to study loss of heterozygosity (LOH) in cases of early oral premalignancies, comparing those with a history of progression to carcinoma in situ or invasive cancer and those without a history of progression (referred to as nonprogressing cases). Each of 116 cases was analyzed for LOH at 19 microsatellite loci on seven chromosome arms (3p, 4q, 8p, 9p, 11q, 13q, and 17p). The progressing and nonprogressing cases showed dramatically different LOH patterns of multiple allelic losses. An essential step for progression seems to involve LOH at 3p and/or 9p because virtually all progressing cases showed such loss. However, LOH at 3p and/or 9p also occurred in nonprogressing cases. Individuals with LOH at 3p and/or 9p but at no other arms exhibit only a slight increase of 3.8-fold in relative risk for developing cancer. In contrast, individuals with additional losses (on 4q, 8p, 11q, or 17p), which appeared uncommon in nonprogressing cases, showed 33-fold increases in relative cancer risk. In conclusion, analysis of LOH at 3p and 9p could serve as an initial screening for cancer risk of early premalignancies. Follow-up investigation for additional losses would be essential for predicting cancer progression.

Citing Articles

Clinical Management Update of Oral Leukoplakia: A Review From the American Head and Neck Society Cancer Prevention Service.

Gates J, Abouyared M, Shnayder Y, Farwell D, Day A, Alawi F Head Neck. 2024; 47(2):733-741.

PMID: 39584361 PMC: 11717973. DOI: 10.1002/hed.28013.

Clinicopathological risk factors of oral second primary tumours.

Karan J, Rosin M, Zhang L, Laronde D Oral Oncol Rep. 2024; 11.

PMID: 39484056 PMC: 11526299. DOI: 10.1016/j.oor.2024.100638.

Reconstructing oral cavity tumor evolution through brush biopsy.

John E, Lesluyes T, Baker T, Tarabichi M, Gillenwater A, Wang J Sci Rep. 2024; 14(1):22591.

PMID: 39343812 PMC: 11439926. DOI: 10.1038/s41598-024-72946-3.

Exploring the microbiome of oral epithelial dysplasia as a predictor of malignant progression.

Wright R, Pewarchuk M, Marshall E, Murrary B, Rosin M, Laronde D BMC Oral Health. 2023; 23(1):206.

PMID: 37024828 PMC: 10080811. DOI: 10.1186/s12903-023-02911-5.

Spatial PD-L1, immune-cell microenvironment, and genomic copy-number alteration patterns and drivers of invasive-disease transition in prospective oral precancer cohort.

William Jr W, Zhang J, Zhao X, Parra E, Uraoka N, Lin H Cancer. 2023; 129(5):714-727.

PMID: 36597662 PMC: 10508302. DOI: 10.1002/cncr.34607.