Journal of Experimental & Clinical Cancer Research (Nov 2024)

Drug prioritization identifies panobinostat as a tailored treatment element for patients with metastatic hepatoblastoma

  • Salih Demir,
  • Alina Hotes,
  • Tanja Schmid,
  • Stefano Cairo,
  • Emilie Indersie,
  • Claudio Pisano,
  • Eiso Hiyama,
  • Tomoro Hishiki,
  • Christian Vokuhl,
  • Sophie Branchereau,
  • Penelope Brock,
  • Irene Schmid,
  • József Zsiros,
  • Roland Kappler

DOI
https://doi.org/10.1186/s13046-024-03221-6
Journal volume & issue
Vol. 43, no. 1
pp. 1 – 16

Abstract

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Abstract Background Patients with metastatic hepatoblastoma are treated with severely toxic first-line chemotherapies in combination with surgery. Yet, inadequate response of lung metastases to neo-adjuvant chemotherapy still compromises patient outcomes making new treatment strategies, tailored to more efficient lung clearance, mandatory. Methods We harnessed a comprehensive patient-derived xenograft platform and a variety of in vitro and in vivo assays to establish the preclinical and biological rationale for a new drug for patients with metastatic hepatoblastoma. Results The testing of a library of established drugs on patient-derived xenografts identified histone deacetylase inhibitors, most notably panobinostat, to be highly efficacious on hepatoblastoma cells, as compared to non-cancerous cells. Molecularly, the anti-tumor effect of panobinostat is mediated by posttranslational obstruction of the MYC oncoprotein as a result of dual specificity phosphatase 1 upregulation, thereby leading to growth inhibition and programmed cell death. Of clinical importance, upregulation of the MYC target gene nucleophosmin 1 is indicative of response to panobinostat and associated with metastatic disease in patients with hepatoblastoma. The combination of panobinostat with the current SIOPEL 4 induction protocol, consisting of cisplatin and doxorubicin, revealed high synergies already at low nanomolar levels. The simulation of a clinical trial, with this combination therapy, in patient-derived xenograft models, and ultimately heterotypic lung metastasis mimics clearly underscored the potency of this approach. Conclusion Integrated studies define MYC inhibition by panobinostat as a novel treatment element to be introduced into the therapeutic strategy for patients with metastatic hepatoblastoma.

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