Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells

Long non-coding RNAs (lncRNAs) are transcripts of a recently discovered class of genes which do not code for proteins. LncRNA genes are approximately as numerous as protein-coding genes in the human genome. However, comparatively little remains known about lncRNA functions. We globally interrogated...

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Autores principales: Lin, Chin-Yo, Kleinbrink, Erica L., Dachet, Fabien, Cai, Juan, Ju, Donghong, Goldstone, Amanda, Wood, Emily J., Liu, Ka, Jia, Hui, Goustin, Anton-Scott, Kosir, Mary A., Thepsuwan, Pattaraporn, Lipovich, Leonard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society 2016
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5204119/
https://www.ncbi.nlm.nih.gov/pubmed/28003470
http://dx.doi.org/10.1098/rsob.150262
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author Lin, Chin-Yo
Kleinbrink, Erica L.
Dachet, Fabien
Cai, Juan
Ju, Donghong
Goldstone, Amanda
Wood, Emily J.
Liu, Ka
Jia, Hui
Goustin, Anton-Scott
Kosir, Mary A.
Thepsuwan, Pattaraporn
Lipovich, Leonard
author_facet Lin, Chin-Yo
Kleinbrink, Erica L.
Dachet, Fabien
Cai, Juan
Ju, Donghong
Goldstone, Amanda
Wood, Emily J.
Liu, Ka
Jia, Hui
Goustin, Anton-Scott
Kosir, Mary A.
Thepsuwan, Pattaraporn
Lipovich, Leonard
author_sort Lin, Chin-Yo
collection PubMed
description Long non-coding RNAs (lncRNAs) are transcripts of a recently discovered class of genes which do not code for proteins. LncRNA genes are approximately as numerous as protein-coding genes in the human genome. However, comparatively little remains known about lncRNA functions. We globally interrogated changes in the lncRNA transcriptome of oestrogen receptor positive human breast cancer cells following treatment with oestrogen, and identified 127 oestrogen-responsive lncRNAs. Consistent with the emerging evidence that most human lncRNA genes lack homologues outside of primates, our evolutionary analysis revealed primate-specific lncRNAs downstream of oestrogen signalling. We demonstrate, using multiple functional assays to probe gain- and loss-of-function phenotypes in two oestrogen receptor positive human breast cancer cell lines, that two primate-specific oestrogen-responsive lncRNAs identified in this study (the oestrogen-repressed lncRNA BC041455, which reduces cell viability, and the oestrogen-induced lncRNA CR593775, which increases cell viability) exert previously unrecognized functions in cell proliferation and growth factor signalling pathways. The results suggest that oestrogen-responsive lncRNAs are capable of altering the proliferation and viability of human breast cancer cells. No effects on cellular phenotypes were associated with control transfections. As heretofore unappreciated components of key signalling pathways in cancers, including the MAP kinase pathway, lncRNAs hence represent a novel mechanism of action for oestrogen effects on cellular proliferation and viability phenotypes. This finding warrants further investigation in basic and translational studies of breast and potentially other types of cancers, has broad relevance to lncRNAs in other nuclear hormone receptor pathways, and should facilitate exploiting and targeting these cell viability modulating lncRNAs in post-genomic therapeutics.
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spelling pubmed-52041192017-01-05 Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells Lin, Chin-Yo Kleinbrink, Erica L. Dachet, Fabien Cai, Juan Ju, Donghong Goldstone, Amanda Wood, Emily J. Liu, Ka Jia, Hui Goustin, Anton-Scott Kosir, Mary A. Thepsuwan, Pattaraporn Lipovich, Leonard Open Biol Research Long non-coding RNAs (lncRNAs) are transcripts of a recently discovered class of genes which do not code for proteins. LncRNA genes are approximately as numerous as protein-coding genes in the human genome. However, comparatively little remains known about lncRNA functions. We globally interrogated changes in the lncRNA transcriptome of oestrogen receptor positive human breast cancer cells following treatment with oestrogen, and identified 127 oestrogen-responsive lncRNAs. Consistent with the emerging evidence that most human lncRNA genes lack homologues outside of primates, our evolutionary analysis revealed primate-specific lncRNAs downstream of oestrogen signalling. We demonstrate, using multiple functional assays to probe gain- and loss-of-function phenotypes in two oestrogen receptor positive human breast cancer cell lines, that two primate-specific oestrogen-responsive lncRNAs identified in this study (the oestrogen-repressed lncRNA BC041455, which reduces cell viability, and the oestrogen-induced lncRNA CR593775, which increases cell viability) exert previously unrecognized functions in cell proliferation and growth factor signalling pathways. The results suggest that oestrogen-responsive lncRNAs are capable of altering the proliferation and viability of human breast cancer cells. No effects on cellular phenotypes were associated with control transfections. As heretofore unappreciated components of key signalling pathways in cancers, including the MAP kinase pathway, lncRNAs hence represent a novel mechanism of action for oestrogen effects on cellular proliferation and viability phenotypes. This finding warrants further investigation in basic and translational studies of breast and potentially other types of cancers, has broad relevance to lncRNAs in other nuclear hormone receptor pathways, and should facilitate exploiting and targeting these cell viability modulating lncRNAs in post-genomic therapeutics. The Royal Society 2016-12-21 /pmc/articles/PMC5204119/ /pubmed/28003470 http://dx.doi.org/10.1098/rsob.150262 Text en © 2016 The Authors. http://creativecommons.org/licenses/by/4.0/ Published by the Royal Society under the terms of the Creative Commons Attribution License http://creativecommons.org/licenses/by/4.0/, which permits unrestricted use, provided the original author and source are credited.
spellingShingle Research
Lin, Chin-Yo
Kleinbrink, Erica L.
Dachet, Fabien
Cai, Juan
Ju, Donghong
Goldstone, Amanda
Wood, Emily J.
Liu, Ka
Jia, Hui
Goustin, Anton-Scott
Kosir, Mary A.
Thepsuwan, Pattaraporn
Lipovich, Leonard
Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title_full Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title_fullStr Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title_full_unstemmed Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title_short Primate-specific oestrogen-responsive long non-coding RNAs regulate proliferation and viability of human breast cancer cells
title_sort primate-specific oestrogen-responsive long non-coding rnas regulate proliferation and viability of human breast cancer cells
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5204119/
https://www.ncbi.nlm.nih.gov/pubmed/28003470
http://dx.doi.org/10.1098/rsob.150262
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