Intracranial mesenchymal tumor, FET::CREB fusion-positive: an integrative analysis of 81 cases

Sharika Rajan; Hye-Jung Chung; Zhichao Wu; Omkar Singh; Karen Dazelle; Zied Abdullaev; Manoj Tyagi; Christina K Ferrone; Mark Raffeld; Ina Lee; Jeffrey Gagan; Jie Chen; Sahara Cathcart; Caterina Giannini; Aivi Nguyen; Murat Gokden; Arie Perry; Igor Lima Fernandes; Angelica R Putnam; Kyle Kurek; Richard M Green; Charles Eberhart; Calixto-Hope Lucas; Ignacio Gonzalez-Gomez; Giselle Yvette Lopez; Karra Jones; Richard Prayson; Gabrielle Yeaney; Josephine Kam Tai Dermawan; Rati Chkheidze; Christina Appin; Erik J Uhlmann; Alisa Taliansky; Melissa Blessing; Carrie Mohila; Jennifer Cotter; Jeremy Deisch; Felipe Andreiuolo; John R Crawford; Christopher Mount; Anat O Stemmer-Rachamimov; Nelli S Lakis; Robert Schmidt; Geeta Chacko; Robert Newbury; Stewart Neill; Bryan Morales; Roger Fecher; Emily A Sloan; David A Solomon; MacLean Nasrallah; Martha Quezado; Adriana Fonseca; Kenneth Aldape

doi:10.1093/neuonc/noag001

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Intracranial mesenchymal tumor, FET::CREB fusion-positive: an integrative analysis of 81 cases

Journal article

Peer reviewed

Intracranial mesenchymal tumor, FET::CREB fusion-positive: an integrative analysis of 81 cases

Sharika Rajan, Hye-Jung Chung, Zhichao Wu, Omkar Singh, Karen Dazelle, Zied Abdullaev, Manoj Tyagi, Christina K Ferrone, Mark Raffeld, Ina Lee, …

Neuro-oncology (Charlottesville, Va.)

01/22/2026

DOI: 10.1093/neuonc/noag001

PMID: 41569358

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Abstract

Intracranial mesenchymal tumors, FET::CREB fusion-positive (ICMT), show fusions involving FET RNA-binding protein family genes (EWSR1 or FUS) and CREB family of transcription factors (ATF1, CREB1 or CREM). The methylation signature(s), gene expression characteristics and clinical behavior of this important tumor type require further characterization. We study the methylation profiles of 81 ICMT cases (61 newly profiled cases and 20 cases from publicly available sources). Clinicopathologic and genomic data were recorded for each case when available. ICMT showed a relatively distinct methylation signature compared to related tumors. Among the 65 cases where fusion types were documented, the identified fusions included EWSR1::ATF1 (25 cases), EWSR1::CREB1 (12 cases), EWSR1::CREM (21 cases), FUS::CREM (3 cases) and SMARCA2::CREM (4 cases). We confirmed the prior description of two distinct subgroups of ICMT (subclasses A and B). The majority of the cases belonged to subclass A (n = 69; 85%), which showed higher median age compared to subclass B patients (26 years vs. 15 years). Subclass B cases (n = 12; 15%) showed shorter progression-free survival (p < 0.01). Gene expression analysis of ICMT showed key overexpressed markers in ICMT, with significant CREM overexpression regardless of fusion type, when compared to either meningioma alone, or a larger group of CNS tumors. This work provides further characterization of ICMT as an important CNS mesenchymal neoplasm that is prone to tumor recurrence, showing 2 prognostically relevant methylation subclasses, and warranting diagnostic distinction from other epigenetically and histologically related tumors. ICMTs show substantial overexpression of the CREM gene, independent of fusion type.

FET-CREB fusion-positive

Intracranial mesenchymal tumor

Details

Title: Subtitle: Intracranial mesenchymal tumor, FET::CREB fusion-positive: an integrative analysis of 81 cases
Creators: Sharika Rajan - National Cancer Institute
Hye-Jung Chung - Laboratory of Pathology, Center for Cancer Research, National Cancer Institute, Bethesda, MD, 20892, USA
Zhichao Wu - National Cancer Institute
Omkar Singh - National Cancer Institute
Karen Dazelle - National Cancer Institute
Zied Abdullaev - Laboratory of Pathology, Center for Cancer Research, National Cancer Institute, Bethesda, MD, 20892, USA
Manoj Tyagi - National Cancer Institute
Christina K Ferrone - National Cancer Institute
Mark Raffeld - National Cancer Institute
Ina Lee - National Cancer Institute
Jeffrey Gagan - National Cancer Institute
Jie Chen - University of Nebraska Medical Center
Sahara Cathcart - University of Nebraska Medical Center
Caterina Giannini - Mayo Clinic
Aivi Nguyen - Mayo Clinic
Murat Gokden - University of Arkansas for Medical Sciences
Arie Perry - University of California, San Francisco
Igor Lima Fernandes - Laboratório Bacchi
Angelica R Putnam - Primary Children's Hospital
Kyle Kurek - Primary Children's Hospital
Richard M Green - Los Angeles Medical Center
Charles Eberhart - Johns Hopkins Hospital
Calixto-Hope Lucas - Johns Hopkins Hospital
Ignacio Gonzalez-Gomez - Johns Hopkins All Children's Hospital
Giselle Yvette Lopez - Duke University
Karra Jones - Duke University
Richard Prayson - Cleveland Clinic
Gabrielle Yeaney - Cleveland Clinic
Josephine Kam Tai Dermawan - Cleveland Clinic
Rati Chkheidze - University of Alabama at Birmingham
Christina Appin - University of Alabama at Birmingham
Erik J Uhlmann - Beth Israel Deaconess Medical Center
Alisa Taliansky - Sheba Medical Center
Melissa Blessing - Texas Children's Hospital
Carrie Mohila - Texas Children's Hospital
Jennifer Cotter - University of Southern California
Jeremy Deisch - Loma Linda University
Felipe Andreiuolo - Department of Pathology, Rede D'Or, Rio de Janeiro, RJ, Brazil
John R Crawford - Children's Hospital of Orange County
Christopher Mount - Massachusetts General Hospital
Anat O Stemmer-Rachamimov - Massachusetts General Hospital
Nelli S Lakis - The University of Kansas Health System
Robert Schmidt - Washington University Medical Center
Geeta Chacko - Christian Medical College, Vellore
Robert Newbury - Rady Children's Hospital-San Diego
Stewart Neill - Emory University Hospital
Bryan Morales - Emory University Hospital
Roger Fecher - Albert Einstein College of Medicine
Emily A Sloan - Georgetown University
David A Solomon - Stanford Medicine
MacLean Nasrallah - University of Pennsylvania
Martha Quezado - National Cancer Institute
Adriana Fonseca - Children's National
Kenneth Aldape - National Cancer Institute
Resource Type: Journal article
Publication Details: Neuro-oncology (Charlottesville, Va.)
DOI: 10.1093/neuonc/noag001
PMID: 41569358
NLM abbreviation: Neuro Oncol
ISSN: 1523-5866
eISSN: 1523-5866
Publisher: Oxford University Press
Language: English
Electronic publication date: 01/22/2026
Academic Unit: Pathology
Record Identifier: 9985130056602771

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