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

Dilara Akhoundova; Stefanie Fischer; Joanna Triscott; Marika Lehner; Phillip Thienger; Sina Maletti; Muriel Jacquet; Dinda S.H. Lubis; Lukas Bubendorf; Wolfram Jochum; Mark A. Rubin

doi:10.1186/s13000-024-01511-3

Diagnostic Pathology (Jun 2024)

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

Dilara Akhoundova,
Stefanie Fischer,
Joanna Triscott,
Marika Lehner,
Phillip Thienger,
Sina Maletti,
Muriel Jacquet,
Dinda S.H. Lubis,
Lukas Bubendorf,
Wolfram Jochum,
Mark A. Rubin

Affiliations

Dilara Akhoundova: Department for BioMedical Research, University of Bern
Stefanie Fischer: Department of Medical Oncology and Hematology, Cantonal Hospital St. Gallen
Joanna Triscott: Department for BioMedical Research, University of Bern
Marika Lehner: Department for BioMedical Research, University of Bern
Phillip Thienger: Department for BioMedical Research, University of Bern
Sina Maletti: Department for BioMedical Research, University of Bern
Muriel Jacquet: Department for BioMedical Research, University of Bern
Dinda S.H. Lubis: Department for BioMedical Research, University of Bern
Lukas Bubendorf: Institute of Medical Genetics and Pathology, University Hospital of Basel
Wolfram Jochum: Institute of Pathology, Cantonal Hospital St. Gallen
Mark A. Rubin: Department for BioMedical Research, University of Bern

DOI: https://doi.org/10.1186/s13000-024-01511-3
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 10

Abstract

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Abstract 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.

Published in Diagnostic Pathology

ISSN: 1746-1596 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Pathology
Website: https://diagnosticpathology.biomedcentral.com/

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