Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.

Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.

Tocopherylquinone (TQ), the oxidation product of alpha-tocopherol (AT), is a bioactive molecule with distinct properties from AT. In this study, AT and TQ are investigated for their comparative effects on growth and androgenic activity in prostate cancer cells. TQ potently inhibited the growth of an...

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Main Authors: Alexandra M Fajardo, Debra A MacKenzie, Sarah L Olguin, John K Scariano, Ian Rabinowitz, Todd A Thompson
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4795544?pdf=render
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spelling doaj-1fc0516e6b5d423ea55125d54d003d202020-11-24T22:16:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01113e015152510.1371/journal.pone.0151525Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.Alexandra M FajardoDebra A MacKenzieSarah L OlguinJohn K ScarianoIan RabinowitzTodd A ThompsonTocopherylquinone (TQ), the oxidation product of alpha-tocopherol (AT), is a bioactive molecule with distinct properties from AT. In this study, AT and TQ are investigated for their comparative effects on growth and androgenic activity in prostate cancer cells. TQ potently inhibited the growth of androgen-responsive prostate cancer cell lines (e.g., LAPC4 and LNCaP cells), whereas the growth of androgen-independent prostate cancer cells (e.g., DU145 cells) was not affected by TQ. Due to the growth inhibitory effects induced by TQ on androgen-responsive cells, the anti-androgenic properties of TQ were examined. TQ inhibited the androgen-induced activation of an androgen-responsive reporter and inhibited the release of prostate specific antigen from LNCaP cells. TQ pretreatment was also found to inhibit AR activation as measured using the Multifunctional Androgen Receptor Screening assay. Furthermore, TQ decreased androgen-responsive gene expression, including TM4SF1, KLK2, and PSA over 5-fold, whereas AT did not affect the expression of androgen-responsive genes. Of importance, the antiandrogenic effects of TQ on prostate cancer cells were found to result from androgen receptor protein down-regulation produced by TQ that was not observed with AT treatment. Moreover, none of the androgenic endpoints assessed were affected by AT. The down-regulation of androgen receptor protein by TQ was abrogated by co-treatment with antioxidants. Overall, the biological actions of TQ were found to be distinct from AT, where TQ was found to be a potent inhibitor of cell growth and androgenic activity in androgen-responsive prostate cancer cells.http://europepmc.org/articles/PMC4795544?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Alexandra M Fajardo
Debra A MacKenzie
Sarah L Olguin
John K Scariano
Ian Rabinowitz
Todd A Thompson
spellingShingle Alexandra M Fajardo
Debra A MacKenzie
Sarah L Olguin
John K Scariano
Ian Rabinowitz
Todd A Thompson
Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
PLoS ONE
author_facet Alexandra M Fajardo
Debra A MacKenzie
Sarah L Olguin
John K Scariano
Ian Rabinowitz
Todd A Thompson
author_sort Alexandra M Fajardo
title Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
title_short Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
title_full Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
title_fullStr Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
title_full_unstemmed Antioxidants Abrogate Alpha-Tocopherylquinone-Mediated Down-Regulation of the Androgen Receptor in Androgen-Responsive Prostate Cancer Cells.
title_sort antioxidants abrogate alpha-tocopherylquinone-mediated down-regulation of the androgen receptor in androgen-responsive prostate cancer cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2016-01-01
description Tocopherylquinone (TQ), the oxidation product of alpha-tocopherol (AT), is a bioactive molecule with distinct properties from AT. In this study, AT and TQ are investigated for their comparative effects on growth and androgenic activity in prostate cancer cells. TQ potently inhibited the growth of androgen-responsive prostate cancer cell lines (e.g., LAPC4 and LNCaP cells), whereas the growth of androgen-independent prostate cancer cells (e.g., DU145 cells) was not affected by TQ. Due to the growth inhibitory effects induced by TQ on androgen-responsive cells, the anti-androgenic properties of TQ were examined. TQ inhibited the androgen-induced activation of an androgen-responsive reporter and inhibited the release of prostate specific antigen from LNCaP cells. TQ pretreatment was also found to inhibit AR activation as measured using the Multifunctional Androgen Receptor Screening assay. Furthermore, TQ decreased androgen-responsive gene expression, including TM4SF1, KLK2, and PSA over 5-fold, whereas AT did not affect the expression of androgen-responsive genes. Of importance, the antiandrogenic effects of TQ on prostate cancer cells were found to result from androgen receptor protein down-regulation produced by TQ that was not observed with AT treatment. Moreover, none of the androgenic endpoints assessed were affected by AT. The down-regulation of androgen receptor protein by TQ was abrogated by co-treatment with antioxidants. Overall, the biological actions of TQ were found to be distinct from AT, where TQ was found to be a potent inhibitor of cell growth and androgenic activity in androgen-responsive prostate cancer cells.
url http://europepmc.org/articles/PMC4795544?pdf=render
work_keys_str_mv AT alexandramfajardo antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
AT debraamackenzie antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
AT sarahlolguin antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
AT johnkscariano antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
AT ianrabinowitz antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
AT toddathompson antioxidantsabrogatealphatocopherylquinonemediateddownregulationoftheandrogenreceptorinandrogenresponsiveprostatecancercells
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