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Promoter DNA Methylation Patterns in Oral, Laryngeal and Oropharyngeal Anatomical Regions Are Associated with Tumor Differentiation, Nodal Involvement and Survival.

Oncology Letters(2024)

Univ Puerto Rico | Johns Hopkins Univ | Puerto Rico Dept Hlth | IRCCS Inst Romagnolo Studio Tumori Dino Amadori | Univ Pittsburgh | LifeGene Biomarks | 4University of Puerto Rico Medical Sciences Campus

Cited 0|Views17
Abstract
Differentially methylated regions (DMRs) can be used as head and neck squamous cell carcinoma (HNSCC) diagnostic, prognostic and therapeutic targets in precision medicine workflows. DNA from 21 HNSCC and 10 healthy oral tissue samples was hybridized to a genome-wide tiling array to identify DMRs in a discovery cohort. Downstream analyses identified differences in promoter DNA methylation patterns in oral, laryngeal and oropharyngeal anatomical regions associated with tumor differentiation, nodal involvement and survival. Genome-wide DMR analysis showed 2,565 DMRs common to the three subsites. A total of 738 DMRs were unique to laryngeal cancer (n=7), 889 DMRs were unique to oral cavity cancer (n=10) and 363 DMRs were unique to pharyngeal cancer (n=6). Based on the genome-wide analysis and a Gene Ontology analysis, 10 candidate genes were selected to test for prognostic value and association with clinicopathological features. TIMP3 was associated with tumor differentiation in oral cavity cancer (P=0.039), DAPK1 was associated with nodal involvement in pharyngeal cancer (P=0.017) and PAX1 was associated with tumor differentiation in laryngeal cancer (P=0.040). A total of five candidate genes were selected, DAPK1, CDH1, PAX1, CALCA and TIMP3, for a prevalence study in a larger validation cohort: Oral cavity cancer samples (n=42), pharyngeal cancer tissues (n=25) and laryngeal cancer samples (n=52). PAX1 hypermethylation differed across HNSCC anatomic subsites (P=0.029), and was predominantly detected in laryngeal cancer. Kaplan-Meier survival analysis (P=0.043) and Cox regression analysis of overall survival (P=0.001) showed that DAPK1 methylation is associated with better prognosis in HNSCC. The findings of the present study showed that the HNSCC subsites oral cavity, pharynx and larynx display substantial differences in aberrant DNA methylation patterns, which may serve as prognostic biomarkers and therapeutic targets.
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differentially methylated regions,precision medicine,head and neck squamous cell carcinoma survival,prognostic biomarkers,epigenome-wide analysis
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要点】:该论文研究了口腔、喉部及口咽部位头颈鳞状细胞癌(HNSCC)的启动子DNA甲基化模式,发现这些模式与肿瘤分化、淋巴结受累和生存率相关,可作为诊断、预后和治疗的精准医学标记。

方法】:使用全基因组tiling阵列对21例HNSCC和10例健康口腔组织样本的DNA进行杂交,以识别差异甲基化区域(DMRs),并通过下游分析关联临床病理特征。

实验】:在发现队列中识别了与三种亚位点共有的2,565个DMRs,以及分别特有于喉癌、口腔癌和咽癌的738、889和363个DMRs。通过基因本体分析选择了10个候选基因,并在更大验证队列中研究了其中5个基因(DAPK1、CDH1、PAX1、CALCA和TIMP3)的表达情况。研究显示PAX1在HNSCC亚位点间存在差异甲基化,而DAPK1甲基化与更好的预后相关。实验使用的数据集为21例HNSCC和10例健康口腔组织样本,以及后续验证队列中的42例口腔癌、25例咽癌和52例喉癌样本。