Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome

Androgens drive the onset and progression of prostate cancer (PCa) by modulating androgen receptor (AR) transcriptional activity. Although several microarray-based studies have identified androgen-regulated genes, here we identify in-parallel global androgen-dependent changes in both gene and altern...

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Autores principales: Rajan, Prabhakar, Dalgliesh, Caroline, Carling, Phillippa J., Buist, Thomas, Zhang, Chaolin, Grellscheid, Sushma N., Armstrong, Kelly, Stockley, Jacqueline, Simillion, Cedric, Gaughan, Luke, Kalna, Gabriela, Zhang, Michael Q., Robson, Craig N., Leung, Hing Y., Elliott, David J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3237596/
https://www.ncbi.nlm.nih.gov/pubmed/22194994
http://dx.doi.org/10.1371/journal.pone.0029088
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author Rajan, Prabhakar
Dalgliesh, Caroline
Carling, Phillippa J.
Buist, Thomas
Zhang, Chaolin
Grellscheid, Sushma N.
Armstrong, Kelly
Stockley, Jacqueline
Simillion, Cedric
Gaughan, Luke
Kalna, Gabriela
Zhang, Michael Q.
Robson, Craig N.
Leung, Hing Y.
Elliott, David J.
author_facet Rajan, Prabhakar
Dalgliesh, Caroline
Carling, Phillippa J.
Buist, Thomas
Zhang, Chaolin
Grellscheid, Sushma N.
Armstrong, Kelly
Stockley, Jacqueline
Simillion, Cedric
Gaughan, Luke
Kalna, Gabriela
Zhang, Michael Q.
Robson, Craig N.
Leung, Hing Y.
Elliott, David J.
author_sort Rajan, Prabhakar
collection PubMed
description Androgens drive the onset and progression of prostate cancer (PCa) by modulating androgen receptor (AR) transcriptional activity. Although several microarray-based studies have identified androgen-regulated genes, here we identify in-parallel global androgen-dependent changes in both gene and alternative mRNA isoform expression by exon-level analyses of the LNCaP transcriptome. While genome-wide gene expression changes correlated well with previously-published studies, we additionally uncovered a subset of 226 novel androgen-regulated genes. Gene expression pathway analysis of this subset revealed gene clusters associated with, and including the tyrosine kinase LYN, as well as components of the mTOR (mammalian target of rapamycin) pathway, which is commonly dysregulated in cancer. We also identified 1279 putative androgen-regulated alternative events, of which 325 (∼25%) mapped to known alternative splicing events or alternative first/last exons. We selected 30 androgen-dependent alternative events for RT-PCR validation, including mRNAs derived from genes encoding tumour suppressors and cell cycle regulators. Of seven positively-validating events (∼23%), five events involved transcripts derived from alternative promoters of known AR gene targets. In particular, we found a novel androgen-dependent mRNA isoform derived from an alternative internal promoter within the TSC2 tumour suppressor gene, which is predicted to encode a protein lacking an interaction domain required for mTOR inhibition. We confirmed that expression of this alternative TSC2 mRNA isoform was directly regulated by androgens, and chromatin immunoprecipitation indicated recruitment of AR to the alternative promoter region at early timepoints following androgen stimulation, which correlated with expression of alternative transcripts. Together, our data suggest that alternative mRNA isoform expression might mediate the cellular response to androgens, and may have roles in clinical PCa.
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spelling pubmed-32375962011-12-22 Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome Rajan, Prabhakar Dalgliesh, Caroline Carling, Phillippa J. Buist, Thomas Zhang, Chaolin Grellscheid, Sushma N. Armstrong, Kelly Stockley, Jacqueline Simillion, Cedric Gaughan, Luke Kalna, Gabriela Zhang, Michael Q. Robson, Craig N. Leung, Hing Y. Elliott, David J. PLoS One Research Article Androgens drive the onset and progression of prostate cancer (PCa) by modulating androgen receptor (AR) transcriptional activity. Although several microarray-based studies have identified androgen-regulated genes, here we identify in-parallel global androgen-dependent changes in both gene and alternative mRNA isoform expression by exon-level analyses of the LNCaP transcriptome. While genome-wide gene expression changes correlated well with previously-published studies, we additionally uncovered a subset of 226 novel androgen-regulated genes. Gene expression pathway analysis of this subset revealed gene clusters associated with, and including the tyrosine kinase LYN, as well as components of the mTOR (mammalian target of rapamycin) pathway, which is commonly dysregulated in cancer. We also identified 1279 putative androgen-regulated alternative events, of which 325 (∼25%) mapped to known alternative splicing events or alternative first/last exons. We selected 30 androgen-dependent alternative events for RT-PCR validation, including mRNAs derived from genes encoding tumour suppressors and cell cycle regulators. Of seven positively-validating events (∼23%), five events involved transcripts derived from alternative promoters of known AR gene targets. In particular, we found a novel androgen-dependent mRNA isoform derived from an alternative internal promoter within the TSC2 tumour suppressor gene, which is predicted to encode a protein lacking an interaction domain required for mTOR inhibition. We confirmed that expression of this alternative TSC2 mRNA isoform was directly regulated by androgens, and chromatin immunoprecipitation indicated recruitment of AR to the alternative promoter region at early timepoints following androgen stimulation, which correlated with expression of alternative transcripts. Together, our data suggest that alternative mRNA isoform expression might mediate the cellular response to androgens, and may have roles in clinical PCa. Public Library of Science 2011-12-14 /pmc/articles/PMC3237596/ /pubmed/22194994 http://dx.doi.org/10.1371/journal.pone.0029088 Text en Rajan et al. http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Rajan, Prabhakar
Dalgliesh, Caroline
Carling, Phillippa J.
Buist, Thomas
Zhang, Chaolin
Grellscheid, Sushma N.
Armstrong, Kelly
Stockley, Jacqueline
Simillion, Cedric
Gaughan, Luke
Kalna, Gabriela
Zhang, Michael Q.
Robson, Craig N.
Leung, Hing Y.
Elliott, David J.
Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title_full Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title_fullStr Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title_full_unstemmed Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title_short Identification of Novel Androgen-Regulated Pathways and mRNA Isoforms through Genome-Wide Exon-Specific Profiling of the LNCaP Transcriptome
title_sort identification of novel androgen-regulated pathways and mrna isoforms through genome-wide exon-specific profiling of the lncap transcriptome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3237596/
https://www.ncbi.nlm.nih.gov/pubmed/22194994
http://dx.doi.org/10.1371/journal.pone.0029088
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