Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer

BACKGROUND: Ultraconserved regions (UCR) are genomic segments of more than 200 base pairs that are evolutionarily conserved among mammalian species. They are thought to have functions as transcriptional enhancers and regulators of alternative splicing. Recently, it was shown that numerous RNAs are t...

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Autores principales: Hudson, Robert S, Yi, Ming, Volfovsky, Natalia, Prueitt, Robyn L, Esposito, Dominic, Volinia, Stefano, Liu, Chang-Gong, Schetter, Aaron J, Van Roosbroeck, Katrien, Stephens, Robert M, Calin, George A, Croce, Carlo M, Ambs, Stefan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3626580/
https://www.ncbi.nlm.nih.gov/pubmed/23409773
http://dx.doi.org/10.1186/1476-4598-12-13
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author Hudson, Robert S
Yi, Ming
Volfovsky, Natalia
Prueitt, Robyn L
Esposito, Dominic
Volinia, Stefano
Liu, Chang-Gong
Schetter, Aaron J
Van Roosbroeck, Katrien
Stephens, Robert M
Calin, George A
Croce, Carlo M
Ambs, Stefan
author_facet Hudson, Robert S
Yi, Ming
Volfovsky, Natalia
Prueitt, Robyn L
Esposito, Dominic
Volinia, Stefano
Liu, Chang-Gong
Schetter, Aaron J
Van Roosbroeck, Katrien
Stephens, Robert M
Calin, George A
Croce, Carlo M
Ambs, Stefan
author_sort Hudson, Robert S
collection PubMed
description BACKGROUND: Ultraconserved regions (UCR) are genomic segments of more than 200 base pairs that are evolutionarily conserved among mammalian species. They are thought to have functions as transcriptional enhancers and regulators of alternative splicing. Recently, it was shown that numerous RNAs are transcribed from these regions. These UCR-encoded transcripts (ucRNAs) were found to be expressed in a tissue- and disease-specific manner and may interfere with the function of other RNAs through RNA: RNA interactions. We hypothesized that ucRNAs have unidentified roles in the pathogenesis of human prostate cancer. In a pilot study, we examined ucRNA expression profiles in human prostate tumors. METHODS: Using a custom microarray with 962 probesets representing sense and antisense sequences for the 481 human UCRs, we examined ucRNA expression in resected, fresh-frozen human prostate tissues (57 tumors, 7 non-cancerous prostate tissues) and in cultured prostate cancer cells treated with either epigenetic drugs (the hypomethylating agent, 5-Aza 2(′)deoxycytidine, and the histone deacetylase inhibitor, trichostatin A) or a synthetic androgen, R1881. Expression of selected ucRNAs was also assessed by qRT-PCR and NanoString®-based assays. Because ucRNAs may function as RNAs that target protein-coding genes through direct and inhibitory RNA: RNA interactions, computational analyses were applied to identify candidate ucRNA:mRNA binding pairs. RESULTS: We observed altered ucRNA expression in prostate cancer (e.g., uc.106+, uc.477+, uc.363 + A, uc.454 + A) and found that these ucRNAs were associated with cancer development, Gleason score, and extraprostatic extension after controlling for false discovery (false discovery rate < 5% for many of the transcripts). We also identified several ucRNAs that were responsive to treatment with either epigenetic drugs or androgen (R1881). For example, experiments with LNCaP human prostate cancer cells showed that uc.287+ is induced by R1881 (P < 0.05) whereas uc.283 + A was up-regulated following treatment with combined 5-Aza 2(′)deoxycytidine and trichostatin A (P < 0.05). Additional computational analyses predicted RNA loop-loop interactions of 302 different sense and antisense ucRNAs with 1058 different mRNAs, inferring possible functions of ucRNAs via direct interactions with mRNAs. CONCLUSIONS: This first study of ucRNA expression in human prostate cancer indicates an altered transcript expression in the disease.
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spelling pubmed-36265802013-04-16 Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer Hudson, Robert S Yi, Ming Volfovsky, Natalia Prueitt, Robyn L Esposito, Dominic Volinia, Stefano Liu, Chang-Gong Schetter, Aaron J Van Roosbroeck, Katrien Stephens, Robert M Calin, George A Croce, Carlo M Ambs, Stefan Mol Cancer Research BACKGROUND: Ultraconserved regions (UCR) are genomic segments of more than 200 base pairs that are evolutionarily conserved among mammalian species. They are thought to have functions as transcriptional enhancers and regulators of alternative splicing. Recently, it was shown that numerous RNAs are transcribed from these regions. These UCR-encoded transcripts (ucRNAs) were found to be expressed in a tissue- and disease-specific manner and may interfere with the function of other RNAs through RNA: RNA interactions. We hypothesized that ucRNAs have unidentified roles in the pathogenesis of human prostate cancer. In a pilot study, we examined ucRNA expression profiles in human prostate tumors. METHODS: Using a custom microarray with 962 probesets representing sense and antisense sequences for the 481 human UCRs, we examined ucRNA expression in resected, fresh-frozen human prostate tissues (57 tumors, 7 non-cancerous prostate tissues) and in cultured prostate cancer cells treated with either epigenetic drugs (the hypomethylating agent, 5-Aza 2(′)deoxycytidine, and the histone deacetylase inhibitor, trichostatin A) or a synthetic androgen, R1881. Expression of selected ucRNAs was also assessed by qRT-PCR and NanoString®-based assays. Because ucRNAs may function as RNAs that target protein-coding genes through direct and inhibitory RNA: RNA interactions, computational analyses were applied to identify candidate ucRNA:mRNA binding pairs. RESULTS: We observed altered ucRNA expression in prostate cancer (e.g., uc.106+, uc.477+, uc.363 + A, uc.454 + A) and found that these ucRNAs were associated with cancer development, Gleason score, and extraprostatic extension after controlling for false discovery (false discovery rate < 5% for many of the transcripts). We also identified several ucRNAs that were responsive to treatment with either epigenetic drugs or androgen (R1881). For example, experiments with LNCaP human prostate cancer cells showed that uc.287+ is induced by R1881 (P < 0.05) whereas uc.283 + A was up-regulated following treatment with combined 5-Aza 2(′)deoxycytidine and trichostatin A (P < 0.05). Additional computational analyses predicted RNA loop-loop interactions of 302 different sense and antisense ucRNAs with 1058 different mRNAs, inferring possible functions of ucRNAs via direct interactions with mRNAs. CONCLUSIONS: This first study of ucRNA expression in human prostate cancer indicates an altered transcript expression in the disease. BioMed Central 2013-02-14 /pmc/articles/PMC3626580/ /pubmed/23409773 http://dx.doi.org/10.1186/1476-4598-12-13 Text en Copyright © 2013 Hudson et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Hudson, Robert S
Yi, Ming
Volfovsky, Natalia
Prueitt, Robyn L
Esposito, Dominic
Volinia, Stefano
Liu, Chang-Gong
Schetter, Aaron J
Van Roosbroeck, Katrien
Stephens, Robert M
Calin, George A
Croce, Carlo M
Ambs, Stefan
Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title_full Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title_fullStr Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title_full_unstemmed Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title_short Transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
title_sort transcription signatures encoded by ultraconserved genomic regions in human prostate cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3626580/
https://www.ncbi.nlm.nih.gov/pubmed/23409773
http://dx.doi.org/10.1186/1476-4598-12-13
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