Mutational and copy number asset of primary sporadic neuroendocrine tumors of the small intestine

被引:0
作者
Michele Simbolo
Caterina Vicentini
Andrea Mafficini
Matteo Fassan
Serena Pedron
Vincenzo Corbo
Luca Mastracci
Borislav Rusev
Corrado Pedrazzani
Luca Landoni
Federica Grillo
Sara Cingarlini
Guido Rindi
Claudio Luchini
Aldo Scarpa
Rita T. Lawlor
机构
[1] University and Hospital Trust of Verona,ARC
[2] University and Hospital Trust of Verona,Net Research Centre
[3] University of Padua,Department of Diagnostics and Public Health, Section of Pathology
[4] University of Genoa and IRCCS S. Martino-IST University Hospital,Department of Medicine (DIMED), Surgical Pathology and Cytopathology Unit
[5] University and Hospital Trust of Verona,Department of Surgical and Diagnostic Sciences (DISC)
[6] University and Hospital Trust of Verona,Department of Surgery, General and Hepatobiliary Surgery
[7] University and Hospital Trust of Verona,Department of Surgery and Oncology, Unit of Surgery B, The Pancreas Institute
[8] Università Cattolica-IRCCS Fondazione Policlinico A. Gemelli,Department of Medicine, Section of Medical Oncology
来源
Virchows Archiv | 2018年 / 473卷
关键词
Neuroendocrine tumors; Small intestine; Prognostic markers;
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中图分类号
学科分类号
摘要
Small intestine neuroendocrine tumors (SI-NETs) represent the most common histotype among small intestine neoplasms, and metastatic disease is usually present at diagnosis. A retrospective series of 52 sporadic primary surgically resected SI-NETs, which were metastatic at diagnosis, was analyzed by high-coverage target sequencing (HCTS) for the mutational status of 57 genes and copy number status of 40 genes selected from recently published genome sequencing data. Seven genes were found to be recurrently mutated: CDKN1B (9.6%), APC and CDKN2C (each 7.7%), BRAF, KRAS, PIK3CA, and TP53 (each 3.8%). Copy number analysis showed frequent allelic loss of 4 genes located on chromosome 18 (BCL2, CDH19, DCC, and SMAD4) in 23/52 (44.2%) and losses on chromosomes 11 (38%) and 16 (15%). Other recurrent copy number variations were gains for genes located on chromosomes 4 (31%), 5 (27%), 14 (36%), and 20 (20%). Univariate survival analysis showed that SRC gene copy number gains were associated with a poorer prognosis (p = 0.047). Recurrent copy number variations are important events in SI-NET and SRC may represent a novel prognostic biomarker for this tumor type.
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页码:709 / 717
页数:8
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