扩展癌外多形性腺瘤的分子谱:对84例新型HMGA2::LINC02389融合病例的分析

IF 4.5 1区 医学 Q1 PATHOLOGY American Journal of Surgical Pathology Pub Date : 2024-09-26 DOI:10.1097/PAS.0000000000002307
Reydson Alcides de Lima-Souza, Albina Altemani, Michal Michal, Fernanda Viviane Mariano, Ilmo Leivo, Alena Skálová
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引用次数: 0

摘要

多形性腺瘤癌(CXPA)是一种侵袭性上皮和/或肌上皮肿瘤,与多形性腺瘤(PA)同时发生。其发病机理目前仍不十分清楚,但据认为,这种肿瘤的发生是由于 PA 中基因、蛋白质、代谢和表观遗传学改变的累积所致。通过对比尔森唾液腺肿瘤登记处进行回顾性研究,发现了 84 例 CXPA,即 25/84 例唾液腺导管癌 (SDC)、15/84 例肌上皮癌 (MC)、1/84 例上皮-肌上皮癌 (EMC) 和 1/84 例腺样囊性癌 (AdCC)。对所有 84 例 CXPA 病例进行了新一代测序(NGS)和/或荧光原位杂交(FISH)分析。最初诊断为 CXPA 的 43 例肿瘤(43/84,51.2%)出现了一些分子改变。在 12/16 例(75%)CXPA 中发现了融合转录本,包括 LIFR::PLAG1、CTNNB1::PLAG1、FGFR1::PLAG1 和一种新型融合 HMGA2::LINC02389。大多数融合都通过使用 PLAG1(6/11)和 HMGA2(1/1)基因断裂探针进行 FISH 验证。FISH 鉴定出 PLAG1(12/17)、HMGA2(3/4)、EWSR1(7/22)和 MYB(2/7)的基因断裂分裂信号。关于致病基因突变,只有上皮分化的CXPA(SDC)出现了这些改变,包括HRAS突变(2/4)、TP53(1/4)、PTEN(1/4)和ATK1(1/4)。此外,还检测到ERBB2(17/35)、MDM2(1/4)和EWSR1(1/7)的扩增。一项新发现是在一名EMC ex-PA患者中发现了HMGA2::LINC02389融合。本研究结果表明,肌上皮分化型(MC)CXPA 的分子图谱分析倾向于揭示染色体融合事件,而上皮分化型(SDC)CXPA 的致病突变和基因扩增频率更高。
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Expanding the Molecular Spectrum of Carcinoma Ex Pleomorphic Adenoma: An Analysis of 84 Cases With a Novel HMGA2::LINC02389 Fusion.

Carcinoma ex pleomorphic adenoma (CXPA) is an aggressive epithelial and/or myoepithelial neoplasm that arises in association with a pleomorphic adenoma (PA). Its etiopathogenesis remains poorly understood, but it is believed that the development of this tumor is due to the accumulation of genetic, protein, metabolic, and epigenetic alterations in a PA. A retrospective review of the Salivary Gland Tumor Registry in Pilsen yielded 84 CXPA, namely 25/84 salivary duct carcinoma (SDC), 15/84 myoepithelial carcinoma (MC), 1/84 epithelial-myoepithelial carcinoma (EMC), and 1/84 adenoid cystic carcinoma (AdCC). All 84 CXPA cases were analyzed by next-generation sequencing (NGS) and/or fluorescence in situ hybridization (FISH). Forty-three tumors originally diagnosed as CXPA (43/84, 51.2%) showed some molecular alteration. Fusion transcripts were identified in 12/16 (75%) CXPA, including LIFR::PLAG1, CTNNB1::PLAG1, FGFR1::PLAG1, and a novel fusion, HMGA2::LINC02389. Most of the fusions were confirmed by FISH using PLAG1 (6/11) and HMGA2 (1/1) gene break probes. Split signals indicating gene break were identified by FISH for PLAG1 (12/17), HMGA2 (3/4), EWSR1 (7/22), and MYB (2/7). Concerning pathogenic mutations, only CXPA with epithelial differentiation (SDC) presented these alterations, including HRAS mutation (2/4), TP53 (1/4), PTEN (1/4), and ATK1 (1/4). In addition, amplifications in ERBB2 (17/35), MDM2 (1/4), and EWSR1 (1/7) were detected. A novel finding was the discovery of an HMGA2::LINC02389 fusion in 1 patient with EMC ex-PA. The present results indicate that molecular profiling of CXPA with myoepithelial differentiation (MC) tends to reveal chromosomal fusion events, whereas CXPA with epithelial differentiation (SDC) tends to have a higher frequency of pathogenic mutations and gene amplifications.

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来源期刊
CiteScore
10.30
自引率
5.40%
发文量
295
审稿时长
1 months
期刊介绍: The American Journal of Surgical Pathology has achieved worldwide recognition for its outstanding coverage of the state of the art in human surgical pathology. In each monthly issue, experts present original articles, review articles, detailed case reports, and special features, enhanced by superb illustrations. Coverage encompasses technical methods, diagnostic aids, and frozen-section diagnosis, in addition to detailed pathologic studies of a wide range of disease entities. Official Journal of The Arthur Purdy Stout Society of Surgical Pathologists and The Gastrointestinal Pathology Society.
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