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Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells

Prostate cancer progression to castration refractory disease is associated with anomalous transcriptional activity of the androgen receptor (AR) in an androgen-depleted milieu. To identify novel gene products whose downregulation transactivates AR in prostate cancer cells, we performed a screen of e...

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Autores principales: Levina, Elina, Ji, Hao, Chen, Mengqiang, Baig, Mirza, Oliver, David, Ohouo, Patrice, Lim, Chang-uk, Schools, Garry, Carmack, Steven, Ding, Ye, Broude, Eugenia V., Roninson, Igor B., Buttyan, Ralph, Shtutman, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4537001/
https://www.ncbi.nlm.nih.gov/pubmed/26036626
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author Levina, Elina
Ji, Hao
Chen, Mengqiang
Baig, Mirza
Oliver, David
Ohouo, Patrice
Lim, Chang-uk
Schools, Garry
Carmack, Steven
Ding, Ye
Broude, Eugenia V.
Roninson, Igor B.
Buttyan, Ralph
Shtutman, Michael
author_facet Levina, Elina
Ji, Hao
Chen, Mengqiang
Baig, Mirza
Oliver, David
Ohouo, Patrice
Lim, Chang-uk
Schools, Garry
Carmack, Steven
Ding, Ye
Broude, Eugenia V.
Roninson, Igor B.
Buttyan, Ralph
Shtutman, Michael
author_sort Levina, Elina
collection PubMed
description Prostate cancer progression to castration refractory disease is associated with anomalous transcriptional activity of the androgen receptor (AR) in an androgen-depleted milieu. To identify novel gene products whose downregulation transactivates AR in prostate cancer cells, we performed a screen of enzymatically-generated shRNA lenti-libraries selecting for transduced LNCaP cells with elevated expression of a fluorescent reporter gene under the control of an AR-responsive promoter. The shRNAs present in selected populations were analyzed using high-throughput sequencing to identify target genes. Highly enriched gene targets were then validated with siRNAs against selected genes, testing first for increased expression of luciferase from an AR-responsive promoter and then for altered expression of endogenous androgen-regulated genes in LNCaP cells. We identified 20 human genes whose silencing affected the expression of exogenous and endogenous androgen-responsive genes in prostate cancer cells grown in androgen-depleted medium. Knockdown of four of these genes upregulated the expression of endogenous AR targets and siRNAs targeting two of these genes (IGSF8 and RTN1) enabled androgen-independent proliferation of androgen-dependent cells. The effects of IGSF8 appear to be mediated through its interaction with a tetraspanin protein, CD9, previously implicated in prostate cancer progression. Remarkably, homozygous deletions of IGSF8 are found almost exclusively in prostate cancers but not in other cancer types. Our study shows that androgen independence can be achieved through the inhibition of specific genes and reveals a novel set of genes that regulate AR signaling in prostate cancers.
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spelling pubmed-45370012015-08-26 Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells Levina, Elina Ji, Hao Chen, Mengqiang Baig, Mirza Oliver, David Ohouo, Patrice Lim, Chang-uk Schools, Garry Carmack, Steven Ding, Ye Broude, Eugenia V. Roninson, Igor B. Buttyan, Ralph Shtutman, Michael Oncotarget Research Paper Prostate cancer progression to castration refractory disease is associated with anomalous transcriptional activity of the androgen receptor (AR) in an androgen-depleted milieu. To identify novel gene products whose downregulation transactivates AR in prostate cancer cells, we performed a screen of enzymatically-generated shRNA lenti-libraries selecting for transduced LNCaP cells with elevated expression of a fluorescent reporter gene under the control of an AR-responsive promoter. The shRNAs present in selected populations were analyzed using high-throughput sequencing to identify target genes. Highly enriched gene targets were then validated with siRNAs against selected genes, testing first for increased expression of luciferase from an AR-responsive promoter and then for altered expression of endogenous androgen-regulated genes in LNCaP cells. We identified 20 human genes whose silencing affected the expression of exogenous and endogenous androgen-responsive genes in prostate cancer cells grown in androgen-depleted medium. Knockdown of four of these genes upregulated the expression of endogenous AR targets and siRNAs targeting two of these genes (IGSF8 and RTN1) enabled androgen-independent proliferation of androgen-dependent cells. The effects of IGSF8 appear to be mediated through its interaction with a tetraspanin protein, CD9, previously implicated in prostate cancer progression. Remarkably, homozygous deletions of IGSF8 are found almost exclusively in prostate cancers but not in other cancer types. Our study shows that androgen independence can be achieved through the inhibition of specific genes and reveals a novel set of genes that regulate AR signaling in prostate cancers. Impact Journals LLC 2015-04-23 /pmc/articles/PMC4537001/ /pubmed/26036626 Text en Copyright: © 2015 Levina et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Levina, Elina
Ji, Hao
Chen, Mengqiang
Baig, Mirza
Oliver, David
Ohouo, Patrice
Lim, Chang-uk
Schools, Garry
Carmack, Steven
Ding, Ye
Broude, Eugenia V.
Roninson, Igor B.
Buttyan, Ralph
Shtutman, Michael
Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title_full Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title_fullStr Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title_full_unstemmed Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title_short Identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
title_sort identification of novel genes that regulate androgen receptor signaling and growth of androgen-deprived prostate cancer cells
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4537001/
https://www.ncbi.nlm.nih.gov/pubmed/26036626
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