A subset of epithelioid and spindle cell rhabdomyosarcomas is associated with TFCP2 fusions and common ALK upregulation.
François Le LoarerArjen H G ClevenCorinne BouvierMarie-Pierre CastexCleofe RomagosaAnne MoreauSébastien SalasBenjamin BonhommeAnne Gomez-BrouchetCamille LaurentSophie Le GuellecVirginie AudardAntoine GiraudIrma Ramos-OliverAnne-Marie Cleton-JansenDilara C Savci-HeijinkHerman M KroonJessica BaudDaniel PissalouxGaëlle PierronI Anand SherwoodJean Michel CoindreJudith V M G BovéeFrédérique LarousserieFranck TirodePublished in: Modern pathology : an official journal of the United States and Canadian Academy of Pathology, Inc (2019)
Rhabdomyosarcomas with TFCP2 fusions represent an emerging subtype of tumors, initially discovered by RNA-sequencing. We report herein the clinicopathological, transcriptional, and genomic features of a series of 14 cases. Cases were retrospectively and prospectively recruited and studied by immunohistochemistry (MYF4, MYOD1, S100, AE1/E3, ALK), fluorescence in situ hybridization with TFCP2 break-apart probe (n = 10/14), array-comparative genomic hybridization (Agilent), whole RNA-sequencing (Truseq Exome, Illumina), or anchored multiplex PCR-based targeted next-generation sequencing (Archer® FusionPlex® Sarcoma kit). Patient's age ranged between 11 and 86 years, including 5 pediatric cases. Tumors were located in the bone (n = 12/14) and soft tissue (n = 2/14). Most bone tumors invaded surrounding soft tissue. Craniofacial bones were over-represented (n = 8/12). Median survival was 8 months and five patients are currently alive with a median follow-up of 20 months. Most tumors displayed a mixed spindle cell and epithelioid pattern with frequent vesicular nuclei. All tumors expressed keratins and showed a rhabdomyogenic phenotype (defined as expression of MYF4 and/or MYOD1). ALK was overexpressed in all but three cases without underlying ALK fusion on break-apart FISH (n = 5) nor next-generation sequencing (n = 14). ALK upregulation was frequently associated with an internal deletion at genomic level. TFCP2 was fused in 5' either to EWSR1 (n = 6) or FUS (n = 8). EWSR1 was involved in both soft tissue cases. FISH with TFCP2 break-apart probe was positive in all tested cases (n = 8), including one case with unbalanced signal. On array-CGH, all tested tumors displayed complex genetic profiles with genomic indexes ranging from 13 to 107.55 and recurrent CDKN2A deletions. FET-TFCP2 rhabdomyosarcomas clustered together and distinctly from other rhabdomyosarcomas subgroups. Altogether, our data confirm and expand the spectrum of the new family of FET-TFCP2 rhabdomyosarcomas, which are associated with a predilection for the craniofacial bones, an aggressive course, and recurrent pathological features. Their association with ALK overexpression might represent a therapeutic vulnerability.
Keyphrases
- soft tissue
- copy number
- advanced non small cell lung cancer
- single cell
- poor prognosis
- high throughput
- end stage renal disease
- cell proliferation
- newly diagnosed
- chronic kidney disease
- cell therapy
- single molecule
- bone mineral density
- genome wide
- transcription factor
- ejection fraction
- case report
- electronic health record
- living cells
- machine learning
- big data
- cancer therapy
- prognostic factors
- drug delivery
- oxidative stress
- peritoneal dialysis
- quantum dots
- deep learning
- binding protein
- nucleic acid
- fluorescent probe