Rare histologic transformation of a CTNNB1 (β-catenin) mutated prostate cancer with aggressive clinical course.

Akhoundova, Dilara; Fischer, Stefanie; Triscott, Joanna; Lehner, Marika; Thienger, Phillip; Maletti, Sina; Jacquet, Muriel; Lubis, Dinda S H; Bubendorf, Lukas; Jochum, Wolfram; Rubin, Mark A (2024). Rare histologic transformation of a CTNNB1 (β-catenin) mutated prostate cancer with aggressive clinical course. Diagnostic pathology, 19(1) BioMed Central 10.1186/s13000-024-01511-3

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BACKGROUND

Catenin (Cadherin-Associated Protein), Beta 1 (CTNNB1) genomic alterations are rare in prostate cancer (PCa). Gain-of-function mutations lead to overexpression of β-catenin, with consequent hyperactivation of the Wnt/β-catenin signaling pathway, implicated in PCa progression and treatment resistance. To date, successful targeted treatment options for Wnt/β-catenin - driven PCa are lacking.

METHODS

We report a rare histologic transformation of a CTNNB1 (β-catenin) mutated metastatic castration resistant prostate cancer (mCRPC), clinically characterized by highly aggressive disease course. We histologically and molecularly characterized the liver metastatic tumor samples, as well as successfully generated patient-derived organoids (PDOs) and patient-derived xenograft (PDX) from a liver metastasis. We used the generated cell models for further molecular characterization and drug response assays.

RESULTS

Immunohistochemistry of liver metastatic biopsies and PDX tumor showed lack of expression of typical PCa (e.g., AR, PSA, PSAP, ERG) or neuroendocrine markers (synaptophysin), compatible with double-negative CRPC, but was positive for nuclear β-catenin expression, keratin 7 and 34βE12. ERG rearrangement was confirmed by fluorescent in situ hybridization (FISH). Drug response assays confirmed, in line with the clinical disease course, lack of sensitivity to common drugs used in mCRPC (e.g., enzalutamide, docetaxel). The casein kinase 1 (CK1) inhibitor IC261 and the tankyrase 1/2 inhibitor G700-LK showed modest activity. Moreover, despite harbouring a CTNNB1 mutation, PDOs were largely insensitive to SMARCA2/4- targeting PROTAC degraders and inhibitor.

CONCLUSIONS

The reported CTNNB1-mutated mCRPC case highlights the potential challenges of double-negative CRPC diagnosis and underlines the relevance of further translational research to enable successful targeted treatment of rare molecular subtypes of mCRPC.

Item Type:

 Journal Article (Further Contribution)

Division/Institute:

 04 Faculty of Medicine > Pre-clinic Human Medicine > BioMedical Research (DBMR) > DBMR Forschung Mu35 > Forschungsgruppe Präzisionsonkologie
04 Faculty of Medicine > Pre-clinic Human Medicine > BioMedical Research (DBMR) > DBMR Forschung Mu35 > Forschungsgruppe Präzisionsonkologie
04 Faculty of Medicine > Pre-clinic Human Medicine > BioMedical Research (DBMR)
04 Faculty of Medicine > Department of Haematology, Oncology, Infectious Diseases, Laboratory Medicine and Hospital Pharmacy (DOLS) > Clinic of Medical Oncology

UniBE Contributor:

 Akhoundova Sanoyan, Dilara, Triscott, Joanna Catherine Caprio, Lehner, Marika, Thienger, Phillip Dominik, Maletti, Sina Laura, Rubin, Mark Andrew

Subjects:

 600 Technology > 610 Medicine & health

ISSN:

 1746-1596

Publisher:

 BioMed Central

Language:

 English

Submitter:

 Pubmed Import

Date Deposited:

 25 Jun 2024 11:56

Last Modified:

 25 Jun 2024 12:05

Publisher DOI:

 10.1186/s13000-024-01511-3

PubMed ID:

 38907236

Uncontrolled Keywords:

 CTNNB1 mutation CK1 inhibitors Histologic transformation Metastatic castration-resistant prostate cancer (mCRPC) Prostate cancer Tankyrase inhibitors Targeted treatment Wnt/β-catenin pathway

BORIS DOI:

 10.48350/198007

URI:

 https://boris.unibe.ch/id/eprint/198007

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