Hybrid Androgen Receptor Inhibitors Outperform Enzalutamide and EPI‐001 in in vitro Models of Prostate Cancer Drug Resistance

Abstract: Androgen receptor targeted therapies for prostate cancer have serious limitations in advanced stages of the disease. While resistance to the FDA‐approved enzalutamide is extensively documented, novel therapies based on epichlorohydrin scaffolds (EPI) are currently in clinical trials, but display suboptimal pharmacokinetics. Herein, we report the synthesis and biological characterisation of a novel class of compounds designed through covalently linking enzalutamide and EPI‐001 through various triazole based linkers. The compounds display an 18 to 53 fold improvement in the cell killing potency towards C4‐2b prostate cancer (PCa) cells compared to the gold standards of therapy, enzalutamide and EPI‐001. The most promising compounds were proven to exhibit their toxicity exclusively through androgen receptor (AR) mediated pathways. This work sets the basis for the first class of hybrid AR inhibitors which successfully combine two drug moieties – EPI‐001 and enzalutamide – into the same molecule.

Standort
Deutsche Nationalbibliothek Frankfurt am Main
Umfang
Online-Ressource
Sprache
Englisch

Erschienen in
Hybrid Androgen Receptor Inhibitors Outperform Enzalutamide and EPI‐001 in in vitro Models of Prostate Cancer Drug Resistance ; day:15 ; month:11 ; year:2022 ; extent:1
ChemMedChem ; (15.11.2022) (gesamt 1)

Urheber
Nicolescu, Radu Costin Bizga
Maylin, Zoe R.
Pérez‐Areales, Francisco Javier
Iegre, Jessica
Pandha, Hardev S.
Asim, Mohammad
Spring, David R.

DOI
10.1002/cmdc.202200548
URN
urn:nbn:de:101:1-2022111614021867952131
Rechteinformation
Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
Letzte Aktualisierung
15.08.2025, 07:21 MESZ

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Beteiligte

  • Nicolescu, Radu Costin Bizga
  • Maylin, Zoe R.
  • Pérez‐Areales, Francisco Javier
  • Iegre, Jessica
  • Pandha, Hardev S.
  • Asim, Mohammad
  • Spring, David R.

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