Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism

INTRODUCTION: Liver × receptors (LXRs) are members of the nuclear receptor family of ligand-dependent transcription factors and have established functions as regulators of cholesterol, glucose, and fatty acid metabolism and inflammatory responses. Published reports of anti-proliferative effects of s...

Descripción completa

Detalles Bibliográficos
Autores principales: Nguyen-Vu, Trang, Vedin, Lise-Lotte, Liu, Ka, Jonsson, Philip, Lin, Jean Z, Candelaria, Nicholes R, Candelaria, Lindsay P, Addanki, Sridevi, Williams, Cecilia, Gustafsson, Jan-Åke, Steffensen, Knut R, Lin, Chin-Yo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053202/
https://www.ncbi.nlm.nih.gov/pubmed/23809258
http://dx.doi.org/10.1186/bcr3443
_version_ 1782320335075409920
author Nguyen-Vu, Trang
Vedin, Lise-Lotte
Liu, Ka
Jonsson, Philip
Lin, Jean Z
Candelaria, Nicholes R
Candelaria, Lindsay P
Addanki, Sridevi
Williams, Cecilia
Gustafsson, Jan-Åke
Steffensen, Knut R
Lin, Chin-Yo
author_facet Nguyen-Vu, Trang
Vedin, Lise-Lotte
Liu, Ka
Jonsson, Philip
Lin, Jean Z
Candelaria, Nicholes R
Candelaria, Lindsay P
Addanki, Sridevi
Williams, Cecilia
Gustafsson, Jan-Åke
Steffensen, Knut R
Lin, Chin-Yo
author_sort Nguyen-Vu, Trang
collection PubMed
description INTRODUCTION: Liver × receptors (LXRs) are members of the nuclear receptor family of ligand-dependent transcription factors and have established functions as regulators of cholesterol, glucose, and fatty acid metabolism and inflammatory responses. Published reports of anti-proliferative effects of synthetic LXR ligands on breast, prostate, ovarian, lung, skin, and colorectal cancer cells suggest that LXRs are potential targets in cancer prevention and treatment. METHODS: To further determine the effects of LXR ligands and identify their potential mechanisms of action in breast cancer cells, we carried out microarray analysis of gene expression in four breast cancer cell lines following treatments with the synthetic LXR ligand GW3965. Differentially expressed genes were further subjected to gene ontology and pathway analyses, and their expression profiles and associations with disease parameters and outcomes were examined in clinical samples. Response of E2F target genes were validated by real-time PCR, and the posited role of E2F2 in breast cancer cell proliferation was tested by RNA interference experiments. RESULTS: We observed cell line-specific transcriptional responses as well as a set of common responsive genes. In the common responsive gene set, upregulated genes tend to function in the known metabolic effects of LXR ligands and LXRs whereas the downregulated genes mostly include those which function in cell cycle regulation, DNA replication, and other cell proliferation-related processes. Transcription factor binding site analysis of the downregulated genes revealed an enrichment of E2F binding site sequence motifs. Correspondingly, E2F2 transcript levels are downregulated following LXR ligand treatment. Knockdown of E2F2 expression, similar to LXR ligand treatment, resulted in a significant disruption of estrogen receptor positive breast cancer cell proliferation. Ligand treatment also decreased E2F2 binding to cis-regulatory regions of target genes. Hierarchical clustering of breast cancer patients based on the expression profiles of the commonly downregulated LXR ligand-responsive genes showed a strong association of these genes with patient survival. CONCLUSIONS: Taken together, these results indicate that LXR ligands target gene networks, including those regulated by E2F family members, are critical for tumor biology and disease progression and merit further consideration as potential agents in the prevention and treatment of breast cancers.
format Online
Article
Text
id pubmed-4053202
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-40532022014-06-12 Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism Nguyen-Vu, Trang Vedin, Lise-Lotte Liu, Ka Jonsson, Philip Lin, Jean Z Candelaria, Nicholes R Candelaria, Lindsay P Addanki, Sridevi Williams, Cecilia Gustafsson, Jan-Åke Steffensen, Knut R Lin, Chin-Yo Breast Cancer Res Research Article INTRODUCTION: Liver × receptors (LXRs) are members of the nuclear receptor family of ligand-dependent transcription factors and have established functions as regulators of cholesterol, glucose, and fatty acid metabolism and inflammatory responses. Published reports of anti-proliferative effects of synthetic LXR ligands on breast, prostate, ovarian, lung, skin, and colorectal cancer cells suggest that LXRs are potential targets in cancer prevention and treatment. METHODS: To further determine the effects of LXR ligands and identify their potential mechanisms of action in breast cancer cells, we carried out microarray analysis of gene expression in four breast cancer cell lines following treatments with the synthetic LXR ligand GW3965. Differentially expressed genes were further subjected to gene ontology and pathway analyses, and their expression profiles and associations with disease parameters and outcomes were examined in clinical samples. Response of E2F target genes were validated by real-time PCR, and the posited role of E2F2 in breast cancer cell proliferation was tested by RNA interference experiments. RESULTS: We observed cell line-specific transcriptional responses as well as a set of common responsive genes. In the common responsive gene set, upregulated genes tend to function in the known metabolic effects of LXR ligands and LXRs whereas the downregulated genes mostly include those which function in cell cycle regulation, DNA replication, and other cell proliferation-related processes. Transcription factor binding site analysis of the downregulated genes revealed an enrichment of E2F binding site sequence motifs. Correspondingly, E2F2 transcript levels are downregulated following LXR ligand treatment. Knockdown of E2F2 expression, similar to LXR ligand treatment, resulted in a significant disruption of estrogen receptor positive breast cancer cell proliferation. Ligand treatment also decreased E2F2 binding to cis-regulatory regions of target genes. Hierarchical clustering of breast cancer patients based on the expression profiles of the commonly downregulated LXR ligand-responsive genes showed a strong association of these genes with patient survival. CONCLUSIONS: Taken together, these results indicate that LXR ligands target gene networks, including those regulated by E2F family members, are critical for tumor biology and disease progression and merit further consideration as potential agents in the prevention and treatment of breast cancers. BioMed Central 2013 2013-06-20 /pmc/articles/PMC4053202/ /pubmed/23809258 http://dx.doi.org/10.1186/bcr3443 Text en Copyright © 2013 Nguyen-Vu 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 Article
Nguyen-Vu, Trang
Vedin, Lise-Lotte
Liu, Ka
Jonsson, Philip
Lin, Jean Z
Candelaria, Nicholes R
Candelaria, Lindsay P
Addanki, Sridevi
Williams, Cecilia
Gustafsson, Jan-Åke
Steffensen, Knut R
Lin, Chin-Yo
Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title_full Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title_fullStr Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title_full_unstemmed Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title_short Liver × receptor ligands disrupt breast cancer cell proliferation through an E2F-mediated mechanism
title_sort liver × receptor ligands disrupt breast cancer cell proliferation through an e2f-mediated mechanism
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053202/
https://www.ncbi.nlm.nih.gov/pubmed/23809258
http://dx.doi.org/10.1186/bcr3443
work_keys_str_mv AT nguyenvutrang liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT vedinliselotte liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT liuka liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT jonssonphilip liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT linjeanz liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT candelarianicholesr liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT candelarialindsayp liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT addankisridevi liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT williamscecilia liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT gustafssonjanake liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT steffensenknutr liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism
AT linchinyo liverreceptorligandsdisruptbreastcancercellproliferationthroughane2fmediatedmechanism

Ejemplares similares