ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.

All-trans retinoic acid (ATRA) has been widely investigated for treatments of many cancers including prostate cancer. HOXB13, silenced in androgen receptor-negative (AR(-)) prostate cancer cells, plays a role in AR(-) prostate cancer cell growth arrest. In this study we intended to elucidate the mec...

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Main Authors: Zhiwei Liu, Guoling Ren, Chenyan Shangguan, Lijing Guo, Zhixiong Dong, Yueyang Li, Weina Zhang, Li Zhao, Pingfu Hou, Yu Zhang, Xiuli Wang, Jun Lu, Baiqu Huang
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3396626?pdf=render
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spelling doaj-2108206c76da497699d7905561fda4b12020-11-25T02:40:00ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0177e4094310.1371/journal.pone.0040943ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.Zhiwei LiuGuoling RenChenyan ShangguanLijing GuoZhixiong DongYueyang LiWeina ZhangLi ZhaoPingfu HouYu ZhangXiuli WangJun LuBaiqu HuangAll-trans retinoic acid (ATRA) has been widely investigated for treatments of many cancers including prostate cancer. HOXB13, silenced in androgen receptor-negative (AR(-)) prostate cancer cells, plays a role in AR(-) prostate cancer cell growth arrest. In this study we intended to elucidate the mechanisms that are involved in the proliferation inhibition of AR(-) prostate cancer cells triggered by ATRA. We discovered that ATRA was able to induce the growth arrest and to increase HOXB13 expression in AR(-) prostate cancer cells. Both EZH2 and DNMT3b participated in the repression of HOXB13 expression through an epigenetic mechanism involving DNA and histone methylation modifications. Specifically, EZH2 recruited DNMT3b to HOXB13 promoter to form a repression complex. Moreover, ATRA could upregulate HOXB13 through decreasing EZH2 and DNMT3b expressions and reducing their interactions with the HOXB13 promoter. Concurrently, the methylation level of the HOXB13 promoter was reduced upon the treatment of ATRA. Results from this study implicated a novel effect of ATRA in inhibition of the growth of AR(-) resistant human prostate cancer cells through alteration of HOXB13 expression as a result of epigenetic modifications.http://europepmc.org/articles/PMC3396626?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Zhiwei Liu
Guoling Ren
Chenyan Shangguan
Lijing Guo
Zhixiong Dong
Yueyang Li
Weina Zhang
Li Zhao
Pingfu Hou
Yu Zhang
Xiuli Wang
Jun Lu
Baiqu Huang
spellingShingle Zhiwei Liu
Guoling Ren
Chenyan Shangguan
Lijing Guo
Zhixiong Dong
Yueyang Li
Weina Zhang
Li Zhao
Pingfu Hou
Yu Zhang
Xiuli Wang
Jun Lu
Baiqu Huang
ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
PLoS ONE
author_facet Zhiwei Liu
Guoling Ren
Chenyan Shangguan
Lijing Guo
Zhixiong Dong
Yueyang Li
Weina Zhang
Li Zhao
Pingfu Hou
Yu Zhang
Xiuli Wang
Jun Lu
Baiqu Huang
author_sort Zhiwei Liu
title ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
title_short ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
title_full ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
title_fullStr ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
title_full_unstemmed ATRA inhibits the proliferation of DU145 prostate cancer cells through reducing the methylation level of HOXB13 gene.
title_sort atra inhibits the proliferation of du145 prostate cancer cells through reducing the methylation level of hoxb13 gene.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description All-trans retinoic acid (ATRA) has been widely investigated for treatments of many cancers including prostate cancer. HOXB13, silenced in androgen receptor-negative (AR(-)) prostate cancer cells, plays a role in AR(-) prostate cancer cell growth arrest. In this study we intended to elucidate the mechanisms that are involved in the proliferation inhibition of AR(-) prostate cancer cells triggered by ATRA. We discovered that ATRA was able to induce the growth arrest and to increase HOXB13 expression in AR(-) prostate cancer cells. Both EZH2 and DNMT3b participated in the repression of HOXB13 expression through an epigenetic mechanism involving DNA and histone methylation modifications. Specifically, EZH2 recruited DNMT3b to HOXB13 promoter to form a repression complex. Moreover, ATRA could upregulate HOXB13 through decreasing EZH2 and DNMT3b expressions and reducing their interactions with the HOXB13 promoter. Concurrently, the methylation level of the HOXB13 promoter was reduced upon the treatment of ATRA. Results from this study implicated a novel effect of ATRA in inhibition of the growth of AR(-) resistant human prostate cancer cells through alteration of HOXB13 expression as a result of epigenetic modifications.
url http://europepmc.org/articles/PMC3396626?pdf=render
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