Comprehensive multi-platform tyrosine kinase profiling reveals novel actionable FGFR aberrations across pediatric and AYA sarcomas
Author:
Fordham Ashleigh M, Brown Lauren M, Mayoh Chelsea, Salib Alice, Barger Zara A, Wong Marie, Sian Terry C.C. Lim Kam, Xie Jinhan, Gunther Kate, Trebilcock Peter, Terry Rachael L, Barahona Paulette, Ajuyah Pamela, Sherstyuk Alexandra, Avila Anica, Cadiz Roxanne, Perkins Callum M, Gifford Andrew J, Mao Jie, Zhao Andrea, O’Regan Luke P, Gorgels Daniel, Lau Loretta MS, Ziegler David S, Haber Michelle, Tyrrell Vanessa, Lock Richard B, Cowley Mark JORCID, Nicholls Wayne, Daly Roger JORCID, Ekert Paul G, Fleuren Emmy DGORCID
Abstract
AbstractNo targeted agents are approved for pediatric sarcomas. Tyrosine kinase (TK) inhibitors represent attractive therapeutic candidates, however, beyond rare TK-activating fusions or mutations, predictive biomarkers are lacking. RNA overexpression of TKs is more commonly observed in pediatric sarcomas, however, an unresolved question is when upregulated TK expression is associated with kinase activation and signaling dependence. We explored the TK molecular landscape of 107 sarcoma patients from the ZERO Childhood Cancer precision medicine program using whole genomic and transcriptomic sequencing. Phosphoproteomic analyses of tyrosine phosphorylation (pY) and functionalin vitroandin vivoassays were also performed in cell lines and patient-derived xenografts (PDXs). Our integrated analysis shows that although novel genomic driver lesions are rare, they are present and therapeutically actionable in selected patients as exemplified by a novelLSM1-FGFR1fusion identified in an osteosarcoma patient. We further show that in certain contexts, TK expression data can be used to indicate TK pathway activity and predict TK-inhibitor sensitivity. We exemplify the utility of FGFR-inhibitors inPAX3-FOXO1fusion-positive rhabdomyosarcomas (FP-RMS) mediated by highFGFR4andFGF8RNA expression levels, and overt activation of FGFR4 (FGFR4_pY). We demonstrate marked tumor growth inhibition in all FP-RMS PDXs treated with single agent FGF401 (FGFR4-specific inhibitor) and single agent lenvatinib (multi-kinase FGFR-inhibitor). Clinical benefit of lenvatinib in a relapsed metastatic FP-RMS patient further exemplifies that FGFR-inhibitors deserve additional investigation in FP-RMS patients.Statement of significanceOur multi-omic interrogation of sarcomas in the ZERO Childhood Cancer program illustrates how an RNA-expression biomarker signature (FGFR4+/FGF8+) in association with FGFR4 activation identifies thatPAX3-FOXO1-positive rhabdomyosarcoma patients could benefit from FGFR-inhibitors.
Publisher
Cold Spring Harbor Laboratory
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