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成釉细胞瘤的基因组和转录组分析揭示了不同的分子侵袭性表型。

Genomic and Transcriptomic Analysis of Ameloblastoma Reveals Distinct Molecularly Aggressive Phenotypes.

作者信息

Marín-Márquez Constanza, Adisa Akinyele O, Niklander Sven E, Kirby Janine, Hunter Keith D

机构信息

Unit of Oral and Maxillofacial Medicine, Pathology and Surgery, University of Sheffield, Sheffield, UK; Facultad de Odontología y Ciencias de la Rehabilitación, Universidad San Sebastián, Puerto Montt, Chile.

Department of Oral Pathology, Faculty of Dentistry, University of Ibadan and University College Hospital Ibadan, Ibadan, Nigeria.

出版信息

Mod Pathol. 2025 Mar;38(3):100682. doi: 10.1016/j.modpat.2024.100682. Epub 2024 Dec 14.

DOI:10.1016/j.modpat.2024.100682
PMID:39675431
Abstract

Ameloblastoma (AM) is a benign but locally infiltrative epithelial odontogenic neoplasm of the jawbones that may reach grotesque proportions and be highly recurrent if inadequately removed. The BRAF mutation has been demonstrated as a key molecular event in its development; nevertheless, there are many queries about its etiopathogenesis, which are yet to be answered. In this study, we aimed to integrate the results from whole-exome sequencing (WES) and RNA sequencing in AM samples to identify novel candidate genes that may be relevant to its pathogenesis. Thirteen-matched tumors were subjected to WES and RNA-seq, respectively, to detect gene mutations and gene expression profiles, along with the presence of gene fusions. Mutations were validated using Sanger sequencing, whereas transcriptome results were validated using qPCR. The results from both molecular techniques were merged in order to identify novel candidate genes that were biologically validated with immunohistochemistry. BRAF mutation was present in 62% of the analyzed cases, and each AM presented at least 2 or 3 mutations affecting cancer-driver genes. RNA-seq showed different molecular subgroups associated with an aggressive and cancer-related phenotype (epithelial-mesenchymal transition and KRAS gene sets). No gene fusions were detected among the cases. CDH11 and TGM2, novel genes associated with epithelial-mesenchymal transition in AM, were selected and validated in tissues. Both WES and RNA-seq results showed gene alterations related to proliferation, cell differentiation, and metabolic processes. These results show that AM shares many of the hallmarks of cancer secondary to the presence of oncogenic mutations or activation of oncogenic signaling pathways.

摘要

成釉细胞瘤(AM)是一种发生于颌骨的良性但具有局部浸润性的上皮性牙源性肿瘤,若切除不彻底,肿瘤可能长得奇形怪状且极易复发。BRAF突变已被证明是其发生发展中的关键分子事件;然而,关于其病因发病机制仍有许多问题有待解答。在本研究中,我们旨在整合AM样本的全外显子组测序(WES)和RNA测序结果,以鉴定可能与其发病机制相关的新候选基因。分别对13对匹配的肿瘤样本进行WES和RNA测序,以检测基因突变、基因表达谱以及基因融合情况。使用桑格测序法验证突变,而转录组结果则通过qPCR进行验证。将两种分子技术的结果合并,以鉴定经免疫组织化学生物学验证的新候选基因。在62%的分析病例中存在BRAF突变,每个AM样本至少有2或3个影响癌症驱动基因的突变。RNA测序显示了与侵袭性和癌症相关表型(上皮-间质转化和KRAS基因集)相关的不同分子亚组。病例中未检测到基因融合。选择了与AM上皮-间质转化相关的新基因CDH11和TGM2,并在组织中进行了验证。WES和RNA测序结果均显示了与增殖、细胞分化和代谢过程相关的基因改变。这些结果表明,由于致癌突变的存在或致癌信号通路的激活,AM具有许多癌症的特征。

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