Infantile Rhabdomyosarcomas With VGLL2 Rearrangement Are Not Always an Indolent Disease: A Study of 4 Aggressive Cases With Clinical, Pathologic, Molecular, and Radiologic Findings.

VGLL2-rearranged rhabdomyosarcomas (RMS) are rare low-grade tumors with only favorable outcomes reported to date. We describe 4 patients with VGLL2-rearranged RMS confirmed by molecular studies, who experienced local progression and distant metastases, including 2 with fatal outcomes. Tumors were diagnosed at birth (n=3) or at 12 months of age (n=1), and were all localized at initial diagnosis, but unresectable and therefore managed with chemotherapy and surveillance. Metastatic progression occurred from 1 to 8 years from diagnosis (median, 3.5 y). Three patients experienced multimetastatic... Mehr ...

Verfasser: Cyrta, Joanna
Gauthier, Arnaud
Karanian, Marie
Vieira, Andre F
Cardoen, Liesbeth
Jehanno, Nina
Bouvet, Mégane
Bouvier, Corinne
Komuta, Mina
Le Loarer, François
Orbach, Daniel
Rome, Angélique
Minard-Colin, Véronique
Brichard, Bénédicte
Pluchart, Claire
Thebaud, Estelle
Renard, Marleen
Pannier, Stéphanie
Brisse, Hervé
Petit, Philippe
Benoist, Camille
Schleiermacher, Gudrun
Geoerger, Birgit
Vincent-Salomon, Anne
Fréneaux, Paul
Pierron, Gaëlle
Dokumenttyp: Artikel
Erscheinungsdatum: 2021
Verlag/Hrsg.: Wolters Kluwer Health
Inc.
Schlagwörter: Belgium / Biomarkers / Tumor / Disease Progression / Fatal Outcome / Female / France / Gene Rearrangement / Genetic Predisposition to Disease / Humans / Immunohistochemistry / Infant / Newborn / Male / Muscle Proteins / Neoplasm Grading / Phenotype / RNA-Seq / Rhabdomyosarcoma / Transcription Factors / Treatment Outcome / Exome Sequencing
Sprache: Englisch
Permalink: https://search.fid-benelux.de/Record/base-28944576
Datenquelle: BASE; Originalkatalog
Powered By: BASE
Link(s) : http://hdl.handle.net/2078.1/275765

VGLL2-rearranged rhabdomyosarcomas (RMS) are rare low-grade tumors with only favorable outcomes reported to date. We describe 4 patients with VGLL2-rearranged RMS confirmed by molecular studies, who experienced local progression and distant metastases, including 2 with fatal outcomes. Tumors were diagnosed at birth (n=3) or at 12 months of age (n=1), and were all localized at initial diagnosis, but unresectable and therefore managed with chemotherapy and surveillance. Metastatic progression occurred from 1 to 8 years from diagnosis (median, 3.5 y). Three patients experienced multimetastatic spread and one showed an isolated adrenal metastasis. At initial diagnosis, 3 tumors displaying bland morphology were misdiagnosed as fibromatosis or infantile fibrosarcoma and initially managed as such, while 1 was a high-grade sarcoma. At relapse, 3 tumors showed high-grade morphology, while 1 retained a low-grade phenotype. Low-grade primary tumors showed only very focal positivity for desmin, myogenin, and/or MyoD1, while high-grade tumors were heterogenously or diffusely positive. Whole-exome sequencing, performed on primary and relapse samples for 3 patients, showed increased genomic instability and additional genomic alterations (eg, TP53, CDKN2A/B, FGFR4) at relapse, but no recurrent events. RNA sequencing confirmed that high-grade tumors retained VGLL2 fusion transcripts and transcriptomic profiles consistent with VGLL2-rearranged RMS. High-grade samples showed a high expression of genes encoding cell cycle proteins, desmin, and some developmental factors. These 4 cases with distinct medical history imply the importance of complete surgical resection, and suggest that RMS-type chemotherapy should be considered in unresectable cases, given the risk of high-grade transformation. They also emphasize the importance of correct initial diagnosis.