Genome sequencing reveals molecular subgroups in oral epithelial dysplasia.

IF 2.5 4区 医学 Q2 Dentistry
Agustín Márquez, Isidora Mujica, Natalia Jordan, Pablo Baez, Sandra Tarquinio, Jean Nunes, Daniela Adorno, Benjamín Martínez, Sebastian Morales-Pison, Ricardo Fernandez-Ramires
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Abstract

This study aimed to analyze the molecular characteristics of oral epithelial dysplasia (OED), highlighting the pathways and variants of genes that are frequently mutated in oral squamous cell carcinoma (OSCC) and other cancers. Ten archival OED cases were retrieved for retrospective clinicopathological analysis and exome sequencing. Comparative genomic analysis was performed between high-grade dysplasia (HGD) and low-grade dysplasia (LGD), focusing on 57 well-known cancer genes, of which 10 were previously described as the most mutated in OSCC. HGD cases had significantly more variants; however, a similar mutational landscape to OSCC was observed in both groups. CASP8+FAT1/HRAS, TP53, and miscellaneous molecular signatures were also present. FAT1 is the gene that is most affected by pathogenic variants. Hierarchical divisive clustering showed division between the two groups: "HGD-like cluster" with 4HGD and 2LGD and "LGD-like cluster" with 4 LGD. MLL4 pathogenic variants were exclusively in the "LGD-like cluster". TP53 was affected in one case of HGD; however, its pathway was usually altered. We describe new insights into the genetic basis of epithelial malignant transformation by genomic analysis, highlighting those associated with FAT1 and TP53. Some LGDs presented a similar mutational landscape to HGD after cluster analysis. Perhaps molecular alterations have not yet been reflected in histomorphology. The relative risk of malignant transformation in this molecular subgroup should be addressed in future studies.

基因组测序揭示了口腔上皮发育不良的分子亚群。
本研究旨在分析口腔上皮异常增生(oral epithelial dysplasia, OED)的分子特征,强调口腔鳞状细胞癌(oral squamous cell carcinoma, OSCC)和其他癌症中频繁突变的基因通路和变异。我们检索了10例OED档案病例进行回顾性临床病理分析和外显子组测序。对高级别发育不良(HGD)和低级别发育不良(LGD)进行比较基因组分析,重点关注57个已知的癌症基因,其中10个先前被描述为在OSCC中突变最多。HGD病例有更多的变异;然而,在两组中观察到与OSCC相似的突变景观。CASP8+FAT1/HRAS, TP53和其他分子特征也存在。FAT1是受致病性变异影响最大的基因。分层分裂聚类表现为两组之间的划分:“类类群”(4HGD和2LGD)和“类类群”(4lgd)。MLL4致病变异仅在“lgd样簇”中。1例HGD患者TP53受影响;然而,它的途径通常是改变的。我们通过基因组分析描述了对上皮恶性转化遗传基础的新见解,重点介绍了与FAT1和TP53相关的遗传基础。聚类分析显示,一些LGDs呈现出与HGD相似的突变格局。也许分子的改变还没有反映在组织形态学上。在这个分子亚群中恶性转化的相对风险应该在未来的研究中加以解决。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Brazilian Oral Research
Brazilian Oral Research DENTISTRY, ORAL SURGERY & MEDICINE-
CiteScore
3.70
自引率
4.00%
发文量
107
审稿时长
12 weeks
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