A vitamin D‐based strategy overcomes chemoresistance in prostate cancer

Author:

Len‐Tayon Kateryna1234ORCID,Beraud Claire5,Fauveau Clara12346,Belorusova Anna Y.1234,Chebaro Yassmine1234,Mouriño Antonio7,Massfelder Thierry8,Chauchereau Anne9,Metzger Daniel1234,Rochel Natacha1234,Laverny Gilles1234ORCID

Affiliation:

1. Institute of Genetics and Molecular and Cellular Biology (IGBMC) Illkirch‐Graffenstaden France

2. CNRS UMR 7104 Illkirch‐Graffenstaden France

3. Inserm U1258 Illkirch‐Graffenstaden France

4. University of Strasbourg Illkirch‐Graffenstaden France

5. Urosphere Toulouse France

6. Transgene SA Illkirch‐Graffenstaden France

7. Department of Chemistry University of Santiago de Compostela Santiago de Compostela Spain

8. INSERM U1260 Strasbourg France

9. INSERM U981, Gustave Roussy University of Paris‐Saclay Villejuif France

Abstract

Background and purposeCastration‐resistant prostate cancer (CRPC) is a common male malignancy that requires new therapeutic strategies due to acquired resistance to its first‐line treatment, docetaxel. The benefits of vitamin D on prostate cancer (PCa) progression have been previously reported. This study aimed to investigate the effects of vitamin D on chemoresistance in CRPC.Experimental approachStructure function relationships of potent vitamin D analogues were determined. The combination of the most potent analogue and docetaxel was explored in chemoresistant primary PCa spheroids and in a xenograft mouse model derived from a patient with a chemoresistant CRPC.Key resultsHere, we show that Xe4MeCF3 is more potent than the natural ligand to induce vitamin D receptor (VDR) transcriptional activities and that it has a larger therapeutic window. Moreover, we demonstrate that VDR agonists restore docetaxel sensitivity in PCa spheroids. Importantly, Xe4MeCF3 reduces tumour growth in a chemoresistant CRPC patient‐derived xenograft. In addition, this treatment targets signalling pathways associated with cancer progression in the remaining cells.Conclusion and implicationsTaken together, these results unravel the potency of VDR agonists to overcome chemoresistance in CRPC and open new avenues for the clinical management of PCa.

Funder

Agence Nationale de la Recherche

Ministère de l'Education Nationale, de l'Enseignement Superieur et de la Recherche

Fondation ARC pour la Recherche sur le Cancer

Publisher

Wiley

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