Comprehensive molecular characterization of adenoid cystic carcinoma reveals tumor suppressors as novel drivers and prognostic biomarkers

IF 5.6 2区 医学 Q1 ONCOLOGY
Marta Persson, Mattias K Andersson, Per-Erik Sahlin, Yoshitsugu Mitani, Margaret S Brandwein-Weber, Henry F Frierson Jr, Christopher Moskaluk, Isabel Fonseca, Renata Ferrarotto, Werner Boecker, Thomas Loening, Adel K El-Naggar, Göran Stenman
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引用次数: 0

Abstract

Adenoid cystic carcinoma (ACC) is a MYB-driven head and neck malignancy with high rates of local recurrence and distant metastasis and poor long-term survival. New effective targeted therapies and clinically useful biomarkers for patient stratification are needed to improve ACC patient survival. Here, we present an integrated copy number and transcriptomic analysis of ACC to identify novel driver genes and prognostic biomarkers. A total of 598 ACCs were studied. Clinical follow-up was available from 366 patients, the largest cohort analyzed to date. Copy number losses of 1p36 (70/492; 14%) and of the tumor suppressor gene PARK2 (6q26) (85/343; 25%) were prognostic biomarkers; patients with concurrent losses (n = 20) had significantly shorter overall survival (OS) than those with one or no deletions (p < 0.0001). Deletion of 1p36 independently predicted short OS in multivariate analysis (p = 0.02). Two pro-apoptotic genes, TP73 and KIF1B, were identified as putative 1p36 tumor suppressor genes whose reduced expression was associated with poor survival and increased resistance to apoptosis. PARK2 expression was markedly reduced in tumors with 6q deletions, and PARK2 knockdown increased spherogenesis and decreased apoptosis, indicating that PARK2 is a tumor suppressor in ACC. Moreover, analysis of the global gene expression pattern in 30 ACCs revealed a transcriptomic signature associated with short OS, multiple copy number alterations including 1p36 deletions, and reduced expression of TP73. Taken together, the results indicate that TP73 and PARK2 are novel putative tumor suppressor genes and potential prognostic biomarkers in ACC. Our studies provide new important insights into the pathogenesis of ACC. The results have important implications for biomarker-driven stratification of patients in clinical trials. © 2023 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland.

Abstract Image

Abstract Image

腺样囊性癌的综合分子特征揭示肿瘤抑制剂是新的驱动因素和预后生物标志物
腺样囊性癌(ACC)是一种MYB驱动的头颈部恶性肿瘤,局部复发率高,远处转移率高,长期生存率低。需要新的有效靶向治疗和临床有用的患者分层生物标志物来提高ACC患者的生存率。在这里,我们提出了ACC的综合拷贝数和转录组学分析,以确定新的驱动基因和预后生物标志物。共研究了598个ACC。366名患者进行了临床随访,这是迄今为止分析的最大队列。1p36(70/492;14%)和肿瘤抑制基因PARK2(6q26)(85/343;25%)的拷贝数损失是预后生物标志物;同时发生损失的患者(n = 20) 总生存期(OS)明显短于有一个或没有缺失的患者(p <; 0.0001)。在多变量分析中,1p36的缺失独立预测短OS(p = 0.02)。两个促凋亡基因TP73和KIF1B被鉴定为推定的1p36肿瘤抑制基因,其表达减少与生存率低和对凋亡的抵抗力增加有关。在6q缺失的肿瘤中,PARK2的表达显著降低,PARK2敲低增加了球形发生并减少了细胞凋亡,表明PARK2是ACC中的肿瘤抑制因子。此外,对30个ACC的整体基因表达模式的分析显示,转录组特征与短OS、包括1p36缺失在内的多拷贝数改变有关,并且TP73的表达减少。总之,研究结果表明,TP73和PARK2是ACC中新的假定肿瘤抑制基因和潜在的预后生物标志物。我们的研究为ACC的发病机制提供了新的重要见解。研究结果对临床试验中生物标志物驱动的患者分层具有重要意义。©2023作者。病理学杂志由John Wiley&;代表大不列颠及爱尔兰病理学会的Sons有限公司。
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
The Journal of Pathology
The Journal of Pathology 医学-病理学
CiteScore
14.10
自引率
1.40%
发文量
144
审稿时长
3-8 weeks
期刊介绍: The Journal of Pathology aims to serve as a translational bridge between basic biomedical science and clinical medicine with particular emphasis on, but not restricted to, tissue based studies. The main interests of the Journal lie in publishing studies that further our understanding the pathophysiological and pathogenetic mechanisms of human disease. The Journal of Pathology welcomes investigative studies on human tissues, in vitro and in vivo experimental studies, and investigations based on animal models with a clear relevance to human disease, including transgenic systems. As well as original research papers, the Journal seeks to provide rapid publication in a variety of other formats, including editorials, review articles, commentaries and perspectives and other features, both contributed and solicited.
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