The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.

The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.

Myoglobin (MB) is not only strongly expressed in myocytes, but also at much lower levels in different cancer entities. 40% of breast tumors are MB-positive, with the globin being co-expressed with markers of tumor hypoxia in a proportion of cases. In breast cancer, MB expression is associated with a...

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Main Authors: Anne Bicker, Alexandra M Brahmer, Sebastian Meller, Glen Kristiansen, Thomas A Gorr, Thomas Hankeln
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4641586?pdf=render
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spelling doaj-b8700db7624544cb99df1d8f644b64d22020-11-24T21:30:00ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-011011e014266210.1371/journal.pone.0142662The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.Anne BickerAlexandra M BrahmerSebastian MellerGlen KristiansenThomas A GorrThomas HankelnMyoglobin (MB) is not only strongly expressed in myocytes, but also at much lower levels in different cancer entities. 40% of breast tumors are MB-positive, with the globin being co-expressed with markers of tumor hypoxia in a proportion of cases. In breast cancer, MB expression is associated with a positive hormone receptor status and patient prognosis. In prostate cancer, another hormone-dependent cancer type, 53% of tumors were recently shown to express MB. Especially in more aggressive prostate cancer specimen MB expression also correlates with increased patient survival rates. Both findings might be due to tumor-suppressing properties of MB in cancer cells. In contrast to muscle, MB transcription in breast and prostate cancer mainly depends on a novel, alternative promoter site. We show here that its associated transcripts can be upregulated by hypoxia and downregulated by estrogens and androgens in MCF7 breast and LNCaP prostate cancer cells, respectively. Bioinformatic data mining of epigenetic histone marks and experimental verification reveal a hitherto uncharacterized transcriptional network that drives the regulation of the MB gene in cancer cells. We identified candidate hormone-receptor binding elements that may interact with the cancer-associated MB promoter to decrease its activity in breast and prostate cancer cells. Additionally, a regulatory element, 250 kb downstream of the promoter, acts as a hypoxia-inducible site within the transcriptional machinery. Understanding the distinct regulation of MB in tumors will improve unraveling the respiratory protein's function in the cancer context and may provide new starting points for developing therapeutic strategies.http://europepmc.org/articles/PMC4641586?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Anne Bicker
Alexandra M Brahmer
Sebastian Meller
Glen Kristiansen
Thomas A Gorr
Thomas Hankeln
spellingShingle Anne Bicker
Alexandra M Brahmer
Sebastian Meller
Glen Kristiansen
Thomas A Gorr
Thomas Hankeln
The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
PLoS ONE
author_facet Anne Bicker
Alexandra M Brahmer
Sebastian Meller
Glen Kristiansen
Thomas A Gorr
Thomas Hankeln
author_sort Anne Bicker
title The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
title_short The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
title_full The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
title_fullStr The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
title_full_unstemmed The Distinct Gene Regulatory Network of Myoglobin in Prostate and Breast Cancer.
title_sort distinct gene regulatory network of myoglobin in prostate and breast cancer.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Myoglobin (MB) is not only strongly expressed in myocytes, but also at much lower levels in different cancer entities. 40% of breast tumors are MB-positive, with the globin being co-expressed with markers of tumor hypoxia in a proportion of cases. In breast cancer, MB expression is associated with a positive hormone receptor status and patient prognosis. In prostate cancer, another hormone-dependent cancer type, 53% of tumors were recently shown to express MB. Especially in more aggressive prostate cancer specimen MB expression also correlates with increased patient survival rates. Both findings might be due to tumor-suppressing properties of MB in cancer cells. In contrast to muscle, MB transcription in breast and prostate cancer mainly depends on a novel, alternative promoter site. We show here that its associated transcripts can be upregulated by hypoxia and downregulated by estrogens and androgens in MCF7 breast and LNCaP prostate cancer cells, respectively. Bioinformatic data mining of epigenetic histone marks and experimental verification reveal a hitherto uncharacterized transcriptional network that drives the regulation of the MB gene in cancer cells. We identified candidate hormone-receptor binding elements that may interact with the cancer-associated MB promoter to decrease its activity in breast and prostate cancer cells. Additionally, a regulatory element, 250 kb downstream of the promoter, acts as a hypoxia-inducible site within the transcriptional machinery. Understanding the distinct regulation of MB in tumors will improve unraveling the respiratory protein's function in the cancer context and may provide new starting points for developing therapeutic strategies.
url http://europepmc.org/articles/PMC4641586?pdf=render
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