α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells

SIMPLE SUMMARY: Castration-resistant prostate cancer often develops in response to continued drug treatment and is characterized by mutations in the androgen receptor. Commonly used anti-androgen drugs are ineffective at targeting these cells; interestingly, our study evaluated a compound from Garci...

Descripción completa

Detalles Bibliográficos
Autores principales: Nauman, Mirielle C., Won, Jong Hoon, Petiwala, Sakina M., Vemu, Bhaskar, Lee, Hyun, Sverdlov, Maria, Johnson, Jeremy J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10093438/
https://www.ncbi.nlm.nih.gov/pubmed/37046780
http://dx.doi.org/10.3390/cancers15072118
_version_ 1785023586112634880
author Nauman, Mirielle C.
Won, Jong Hoon
Petiwala, Sakina M.
Vemu, Bhaskar
Lee, Hyun
Sverdlov, Maria
Johnson, Jeremy J.
author_facet Nauman, Mirielle C.
Won, Jong Hoon
Petiwala, Sakina M.
Vemu, Bhaskar
Lee, Hyun
Sverdlov, Maria
Johnson, Jeremy J.
author_sort Nauman, Mirielle C.
collection PubMed
description SIMPLE SUMMARY: Castration-resistant prostate cancer often develops in response to continued drug treatment and is characterized by mutations in the androgen receptor. Commonly used anti-androgen drugs are ineffective at targeting these cells; interestingly, our study evaluated a compound from Garcinia mangostana that has activity against castration-resistant prostate cancer cells. Our data shows that this compound effectively decreases cell viability and degrades the androgen receptor, regardless of mutations present in the androgen receptor. We suggest that this may be achieved through the activation of a cell stress chaperone protein, BiP, which our compound both binds to and promotes binding with the androgen receptor. Finally, this compound has in vivo anticancer activity and decreases mutant androgen receptor expression in vivo as well. Novel compounds that can degrade mutant androgen receptors present an opportunity to target castration-resistant prostate cancer cells through a unique mechanism. ABSTRACT: A major limitation of current prostate cancer pharmacotherapy approaches is the inability of these compounds to target androgen receptor variants or mutants that develop during prostate cancer progression. The demand for novel therapeutics to prevent, slow, and treat prostate cancer is significant because FDA approved anti-androgens are associated with adverse events and can eventually drive drug-resistant prostate cancer. This study evaluated α-mangostin for its novel ability to degrade the androgen receptor and androgen receptor variants. α-Mangostin is one of more than 70 isoprenylated xanthones isolated from Garcinia mangostana that we have been evaluating for their anticancer potential. Prostate cancer cells treated with α-mangostin exhibited decreased levels of wild-type and mutated androgen receptors. Immunoblot, immunoprecipitation, and transfection experiments demonstrated that the androgen receptor was ubiquitinated and subsequently degraded via the proteasome, which we hypothesize occurs with the assistance of BiP, an ER chaperone protein that we have shown to associate with the androgen receptor. We also evaluated α-mangostin for its antitumor activity and promotion of androgen receptor degradation in vivo. In summary, our study demonstrates that androgen receptor degradation occurs through the novel activation of BiP and suggests a new therapeutic approach for prostate cancer.
format Online
Article
Text
id pubmed-10093438
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-100934382023-04-13 α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells Nauman, Mirielle C. Won, Jong Hoon Petiwala, Sakina M. Vemu, Bhaskar Lee, Hyun Sverdlov, Maria Johnson, Jeremy J. Cancers (Basel) Article SIMPLE SUMMARY: Castration-resistant prostate cancer often develops in response to continued drug treatment and is characterized by mutations in the androgen receptor. Commonly used anti-androgen drugs are ineffective at targeting these cells; interestingly, our study evaluated a compound from Garcinia mangostana that has activity against castration-resistant prostate cancer cells. Our data shows that this compound effectively decreases cell viability and degrades the androgen receptor, regardless of mutations present in the androgen receptor. We suggest that this may be achieved through the activation of a cell stress chaperone protein, BiP, which our compound both binds to and promotes binding with the androgen receptor. Finally, this compound has in vivo anticancer activity and decreases mutant androgen receptor expression in vivo as well. Novel compounds that can degrade mutant androgen receptors present an opportunity to target castration-resistant prostate cancer cells through a unique mechanism. ABSTRACT: A major limitation of current prostate cancer pharmacotherapy approaches is the inability of these compounds to target androgen receptor variants or mutants that develop during prostate cancer progression. The demand for novel therapeutics to prevent, slow, and treat prostate cancer is significant because FDA approved anti-androgens are associated with adverse events and can eventually drive drug-resistant prostate cancer. This study evaluated α-mangostin for its novel ability to degrade the androgen receptor and androgen receptor variants. α-Mangostin is one of more than 70 isoprenylated xanthones isolated from Garcinia mangostana that we have been evaluating for their anticancer potential. Prostate cancer cells treated with α-mangostin exhibited decreased levels of wild-type and mutated androgen receptors. Immunoblot, immunoprecipitation, and transfection experiments demonstrated that the androgen receptor was ubiquitinated and subsequently degraded via the proteasome, which we hypothesize occurs with the assistance of BiP, an ER chaperone protein that we have shown to associate with the androgen receptor. We also evaluated α-mangostin for its antitumor activity and promotion of androgen receptor degradation in vivo. In summary, our study demonstrates that androgen receptor degradation occurs through the novel activation of BiP and suggests a new therapeutic approach for prostate cancer. MDPI 2023-04-01 /pmc/articles/PMC10093438/ /pubmed/37046780 http://dx.doi.org/10.3390/cancers15072118 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Nauman, Mirielle C.
Won, Jong Hoon
Petiwala, Sakina M.
Vemu, Bhaskar
Lee, Hyun
Sverdlov, Maria
Johnson, Jeremy J.
α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title_full α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title_fullStr α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title_full_unstemmed α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title_short α-Mangostin Promotes In Vitro and In Vivo Degradation of Androgen Receptor and AR-V7 Splice Variant in Prostate Cancer Cells
title_sort α-mangostin promotes in vitro and in vivo degradation of androgen receptor and ar-v7 splice variant in prostate cancer cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10093438/
https://www.ncbi.nlm.nih.gov/pubmed/37046780
http://dx.doi.org/10.3390/cancers15072118
work_keys_str_mv AT naumanmiriellec amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT wonjonghoon amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT petiwalasakinam amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT vemubhaskar amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT leehyun amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT sverdlovmaria amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells
AT johnsonjeremyj amangostinpromotesinvitroandinvivodegradationofandrogenreceptorandarv7splicevariantinprostatecancercells

Ejemplares similares