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Primary intracranial spindle cell sarcoma with rhabdomyosarcoma-like features share a highly distinct methylation profile and DICER1 mutations

胚胎性横纹肌肉瘤 神经母细胞瘤RAS病毒癌基因同源物 横纹肌肉瘤 肉瘤 癌症研究 克拉斯 生物 病理 赫拉 种系突变 生殖系 周围神经鞘恶性肿瘤 突变 医学 遗传学 基因 免疫组织化学
作者
Christian Koelsche,Martin Mynarek,Daniel Schrimpf,Luca Bertero,Jonathan Serrano,Felix Sahm,David Reuß,Yanghao Hou,Daniel Baumhoer,Christian Vokuhl,Uta Flucke,Iver Petersen,Wolfgang Brück,Stefan Rutkowski,Sandro Casavilca‐Zambrano,Juan Luis García León,Rosdali Yesenia Diaz Coronado,Manfred Gessler,Óscar M. Tirado,Jaume Mora,Javier Alonso,Xavier García del Muro,Manel Esteller,Dominik Sturm,Jonas Ecker,Till Milde,Stefan M. Pfister,Andrey Korshunov,Matija Snuderl,Gunhild Mechtersheimer,Ulrich Schüller,David Jones,Andreas von Deimling
出处
期刊:Acta Neuropathologica [Springer Nature]
卷期号:136 (2): 327-337 被引量:116
标识
DOI:10.1007/s00401-018-1871-6
摘要

Patients with DICER1 predisposition syndrome have an increased risk to develop pleuropulmonary blastoma, cystic nephroma, embryonal rhabdomyosarcoma, and several other rare tumor entities. In this study, we identified 22 primary intracranial sarcomas, including 18 in pediatric patients, with a distinct methylation signature detected by array-based DNA-methylation profiling. In addition, two uterine rhabdomyosarcomas sharing identical features were identified. Gene panel sequencing of the 22 intracranial sarcomas revealed the almost unifying feature of DICER1 hotspot mutations (21/22; 95%) and a high frequency of co-occurring TP53 mutations (12/22; 55%). In addition, 17/22 (77%) sarcomas exhibited alterations in the mitogen-activated protein kinase pathway, most frequently affecting the mutational hotspots of KRAS (8/22; 36%) and mutations or deletions of NF1 (7/22; 32%), followed by mutations of FGFR4 (2/22; 9%), NRAS (2/22; 9%), and amplification of EGFR (1/22; 5%). A germline DICER1 mutation was detected in two of five cases with constitutional DNA available. Notably, none of the patients showed evidence of a cancer-related syndrome at the time of diagnosis. In contrast to the genetic findings, the morphological features of these tumors were less distinctive, although rhabdomyoblasts or rhabdomyoblast-like cells could retrospectively be detected in all cases. The identified combination of genetic events indicates a relationship between the intracranial tumors analyzed and DICER1 predisposition syndrome-associated sarcomas such as embryonal rhabdomyosarcoma or the recently described group of anaplastic sarcomas of the kidney. However, the intracranial tumors in our series were initially interpreted to represent various tumor types, but rhabdomyosarcoma was not among the typical differential diagnoses considered. Given the rarity of intracranial sarcomas, this molecularly clearly defined group comprises a considerable fraction thereof. We therefore propose the designation “spindle cell sarcoma with rhabdomyosarcoma-like features, DICER1 mutant” for this intriguing group.
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