FGF7–FGFR2 autocrine signaling increases growth and chemoresistance of fusion‐positive rhabdomyosarcomas

Christopher I. Milton; Joanna Selfe; Ewa Aladowicz; Stella Y. K. Man; Carolina Bernauer; Edoardo Missiaglia; Zoë S. Walters; Susanne A. Gatz; Anna Kelsey; Melanie Generali; Gary Box; Melanie Valenti; Alexis deHaven‐Brandon; David Galiwango; Angela Hayes; Matthew Clarke; Elisa Izquierdo; David Gonzalez De Castro; Florence I. Raynaud; Vladimir Kirkin; Janet M. Shipley

doi:10.1002/1878-0261.13145

Molecular Oncology (Mar 2022)

FGF7–FGFR2 autocrine signaling increases growth and chemoresistance of fusion‐positive rhabdomyosarcomas

Christopher I. Milton,
Joanna Selfe,
Ewa Aladowicz,
Stella Y. K. Man,
Carolina Bernauer,
Edoardo Missiaglia,
Zoë S. Walters,
Susanne A. Gatz,
Anna Kelsey,
Melanie Generali,
Gary Box,
Melanie Valenti,
Alexis deHaven‐Brandon,
David Galiwango,
Angela Hayes,
Matthew Clarke,
Elisa Izquierdo,
David Gonzalez De Castro,
Florence I. Raynaud,
Vladimir Kirkin,
Janet M. Shipley

Affiliations

Christopher I. Milton: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Joanna Selfe: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Ewa Aladowicz: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Stella Y. K. Man: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Carolina Bernauer: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Edoardo Missiaglia: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Zoë S. Walters: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Susanne A. Gatz: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Anna Kelsey: Department of Paediatric Histopathology Manchester University NHS Foundation Trust Royal Manchester Children’s Hospital UK
Melanie Generali: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK
Gary Box: Cancer Pharmacology and Stress Response Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Melanie Valenti: Cancer Pharmacology and Stress Response Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Alexis deHaven‐Brandon: Cancer Pharmacology and Stress Response Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
David Galiwango: Drug Metabolism and Pharmacokinetics Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Angela Hayes: Drug Metabolism and Pharmacokinetics Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Matthew Clarke: Glioma Team Division of Molecular Pathology The Institute of Cancer Research London UK
Elisa Izquierdo: Glioma Team Division of Molecular Pathology The Institute of Cancer Research London UK
David Gonzalez De Castro: Molecular Haematology Division of Molecular Pathology The Institute of Cancer Research London UK
Florence I. Raynaud: Drug Metabolism and Pharmacokinetics Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Vladimir Kirkin: Cancer Pharmacology and Stress Response Team Division of Cancer Therapeutics The Institute of Cancer Research London UK
Janet M. Shipley: Sarcoma Molecular Pathology Team Divisions of Molecular Pathology and Cancer Therapeutics The Institute of Cancer Research London UK

DOI: https://doi.org/10.1002/1878-0261.13145
Journal volume & issue: Vol. 16, no. 6
pp. 1272 – 1289

Abstract

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Rhabdomyosarcomas are aggressive pediatric soft‐tissue sarcomas and include high‐risk PAX3–FOXO1 fusion‐gene‐positive cases. Fibroblast growth factor receptor 4 (FGFR4) is known to contribute to rhabdomyosarcoma progression; here, we sought to investigate the involvement and potential for therapeutic targeting of other FGFRs in this disease. Cell‐based screening of FGFR inhibitors with potential for clinical repurposing (NVP‐BGJ398, nintedanib, dovitinib, and ponatinib) revealed greater sensitivity of fusion‐gene‐positive versus fusion‐gene‐negative rhabdomyosarcoma cell lines and was shown to be correlated with high expression of FGFR2 and its specific ligand, FGF7. Furthermore, patient samples exhibit higher mRNA levels of FGFR2 and FGF7 in fusion‐gene‐positive versus fusion‐gene‐negative rhabdomyosarcomas. Sustained intracellular mitogen‐activated protein kinase (MAPK) activity and FGF7 secretion into culture media during serum starvation of PAX3–FOXO1 rhabdomyosarcoma cells together with decreased cell viability after genetic silencing of FGFR2 or FGF7 was in keeping with a novel FGF7–FGFR2 autocrine loop. FGFR inhibition with NVP‐BGJ398 reduced viability and was synergistic with SN38, the active metabolite of irinotecan. In vivo, NVP‐BGJ398 abrogated xenograft growth and warrants further investigation in combination with irinotecan as a therapeutic strategy for fusion‐gene‐positive rhabdomyosarcomas.

Published in Molecular Oncology

ISSN: 1574-7891 (Print); 1878-0261 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://febs.onlinelibrary.wiley.com/journal/18780261

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