In Vivo Efficacy of a Macrocyclic Peptoid‐Peptide Hybrid That Selectively Modulates the Beta‐Catenin/TCF Interaction to Inhibit Prostate Cancer | Zendy

Habault Justine | Zendy; Franco Jennifer L. | Zendy; Ha Susan | Zendy; Schneider Jeffry A. | Zendy; Voisin Maud | Zendy; Wise David R. | Zendy; Wong KwokKin | Zendy; Garabedian Michael J. | Zendy; Kirshenbaum Kent | Zendy; Logan Susan K. | Zendy

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In Vivo Efficacy of a Macrocyclic Peptoid‐Peptide Hybrid That Selectively Modulates the Beta‐Catenin/TCF Interaction to Inhibit Prostate Cancer

Author(s) -

Habault Justine,

Franco Jennifer L.,

Ha Susan,

Schneider Jeffry A.,

Voisin Maud,

Wise David R.,

Wong KwokKin,

Garabedian Michael J.,

Kirshenbaum Kent,

Logan Susan K.

Publication year - 2025

Publication title -

the prostate

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.295

H-Index - 123

eISSN - 1097-0045

pISSN - 0270-4137

DOI - 10.1002/pros.24868

Subject(s) - peptoid , in vivo , prostate cancer , peptide , cancer research , prostate , beta catenin , medicine , cancer , chemistry , oncology , biology , biochemistry , wnt signaling pathway , signal transduction , genetics

ABSTRACT Background Prostate cancer is the most common form of male cancer and can initially be treated as a localized disease. Although the 5‐year survival rate at diagnosis approaches 100 percent, a subset of patients will subsequently develop resistance to treatment. This may ultimately lead to metastatic castration resistant prostate cancer (mCRPC), for which the prognosis is much less favorable. The importance of the Wnt/β‐catenin pathway in treatment‐resistant prostate cancer has inspired efforts to exploit the interaction of β‐catenin with its transcription binding partners as a therapeutic strategy for prostate cancer. Methods Peptoid‐peptide macrocycles are attractive design scaffolds for disrupting protein‐protein interactions. In this study, we evaluate a library of these macrocycles and demonstrate their selectivity for the β‐catenin/TCF ( T C ell F actor) interaction. Results Importantly, we show that the macrocycles do not significantly alter the binding of β‐catenin to cell surface protein, E‐cadherin. Our lead sequence, Macrocycle 13, (MC13) was also tolerant of modifications aimed to improve aqueous solubility while retaining activity. Herein, we demonstrate in vivo proof of principle for using peptidomimetic macrocycles to target the β‐catenin/TCF interaction. Treated prostate cancer mouse xenografts show markedly diminished tumor growth and decreased levels of myc protein. MC13 also inhibits growth in an organoid model with genetic alterations frequently found in prostate cancer. Transcriptome analysis of prostate cancer cells treated with MC13 reveals downregulation of key pathways, including Wnt/β‐catenin and c‐myc. Furthermore, chromatin immunoprecipitation (ChIP) analysis shows reduced β‐catenin at its target genes, axin2 and c‐myc. Conclusion Our findings underscore the therapeutic potential of peptoid‐peptide macrocycle inhibition of β‐catenin in prostate cancer.

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