Giant Cell Tumors With HMGA2::NCOR2 Fusion-Reference-Cited by-同舟云学术

Giant Cell Tumors With HMGA2::NCOR2 Fusion

Published:2023-05-12 Issue:7 Volume:47 Page:801-811
ISSN:0147-5185
Container-title:American Journal of Surgical Pathology
language:en
Short-container-title:

Author:

Perret Raul¹²^ORCID,Malaka Zaki¹³,Velasco Valérie¹,Llamas-Gutierrez Francisco⁴,Ropars Mickael⁵,Linck Pierre-Antoine⁶,Hostein Isabelle¹,Azmani Rihab⁷,Valo Isabelle⁸,Galmiche Louise⁹,Moreau Anne⁹,de Pinieux Gonzague¹⁰,Michot Audrey¹¹,Bochaton Dorian,Coindre Jean-Michel¹,Le Loarer François¹²³

Affiliation:

1. Department of Biopathology, Institut Bergonié, Comprehensive Cancer Center, Bordeaux, France

2. Bordeaux Institute of Oncology, BRIC, INSERM, Bordeaux University, Bergonié Institute, Bordeaux, France

3. University of Bordeaux, Talence, France

4. Department of Pathology, Rennes University Hospital, University of Rennes 1, Rennes, France

5. Orthopedic surgery department, Rennes University Hospital, Rennes, France

6. Department of Radiology, Bergonié Institute, Comprehensive Cancer Center, Bordeaux, France

7. Department of Bioinformatics, Bergonie Institute, Comprehensive Cancer Center, Bordeaux, France

8. Department of Pathology, Institute of Cancerology of the West, Angers, France

9. Department of Pathology, Nantes University Hospital, Nantes, France

10. Department of Pathology, Trousseau Hospital-Tours University Hospital, Chambray-lés-Tours, France

11. Plastic and Reconstructive Surgery Department, Bergonié Institute, Bordeaux, France

Abstract

Giant cell tumors (GCTs) with high mobility group AT-Hook 2 (HMGA2)::nuclear receptor corepressor 2 (NCOR2) fusion are rare mesenchymal tumors of controversial nosology, which have been anecdotally reported to respond to CSFR1 inhibitors. Here, we performed a comprehensive study of 6 GCTs withHMGA2::NCOR2fusion and explored their relationship with other giant cell-rich neoplasms. Tumors occurred in 4 females and 2 males ranging in age from 17 to 32 years old (median 24). Three lesions originated in subcutaneous soft tissue and 3 in bone. Tumor size ranged from 20 to 33 mm (median 27 mm). The lesions had a nodular/multinodular architecture and were composed of sheets of mononuclear “histiocytoid” cells with uniform nuclei intermingled with multinucleated giant cells. Mitotic activity was low and nuclear atypia and metaplastic bone were absent. Variable findings included necrosis, cystic degeneration, lymphocytic infiltrate (sometimes forming nodules), and xanthogranulomatous inflammation. On immunohistochemistry, all cases focally expressed pan-keratin and were negative with SATB2 and H3.3G34W. Whole RNA-sequencing was performed in all cases of GCT withHMGA2::NCOR2fusion and a subset of giant cell-rich tumors (tenosynovial-GCT, n = 19 and “wild-type” GCT of soft tissue, n = 9). Hierarchical clustering of RNA-sequencing data showed that GCT withHMGA2::NCOR2fusion formed a single cluster, independent of the other 2 entities. Methylome profiling showed similar results, but the distinction from “wild-type” GCT of soft tissue was less flagrant. Gene expression analysis showed similar levels of expression of the CSF1/CSFR1 axis between GCT withHMGA2::NCOR2fusion and tenosynovial-GCT, supporting their potential sensitivity to CSFR1 inhibitors. Clinical follow-up was available for 5 patients (range: 10 to 64 mo; median 32 mo). Three patients (60%) experienced local recurrences, whereas none had distant metastases or died of disease. Overall, our study confirms and expands previous knowledge on GCT withHMGA2::NCOR2fusion and supports its inclusion as an independent entity.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Pathology and Forensic Medicine,Surgery,Anatomy

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