Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer

INTRODUCTION: Given the role of estrogen in breast carcinogenesis and the modification of estrogen receptor (ER) activity by its biochemical cofactors, we hypothesize that genetic variation within ER cofactor genes alters cellular response to estrogen exposure and consequently modifies the risk for...

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Autores principales: Li, Yuqing, Li, Yi, Wedrén, Sara, Li, Guoliang, Charn, Tze Howe, Desai, Kartiki Vasant, Bonnard, Carine, Czene, Kamila, Humphreys, Keith, Darabi, Hatef, Einarsdóttir, Kristjana, Heikkinen, Tuomas, Aittomäki, Kristiina, Blomqvist, Carl, Chia, Kee Seng, Nevanlinna, Heli, Hall, Per, Liu, Edison T, Liu, Jianjun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3109578/
https://www.ncbi.nlm.nih.gov/pubmed/21269472
http://dx.doi.org/10.1186/bcr2817
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author Li, Yuqing
Li, Yi
Wedrén, Sara
Li, Guoliang
Charn, Tze Howe
Desai, Kartiki Vasant
Bonnard, Carine
Czene, Kamila
Humphreys, Keith
Darabi, Hatef
Einarsdóttir, Kristjana
Heikkinen, Tuomas
Aittomäki, Kristiina
Blomqvist, Carl
Chia, Kee Seng
Nevanlinna, Heli
Hall, Per
Liu, Edison T
Liu, Jianjun
author_facet Li, Yuqing
Li, Yi
Wedrén, Sara
Li, Guoliang
Charn, Tze Howe
Desai, Kartiki Vasant
Bonnard, Carine
Czene, Kamila
Humphreys, Keith
Darabi, Hatef
Einarsdóttir, Kristjana
Heikkinen, Tuomas
Aittomäki, Kristiina
Blomqvist, Carl
Chia, Kee Seng
Nevanlinna, Heli
Hall, Per
Liu, Edison T
Liu, Jianjun
author_sort Li, Yuqing
collection PubMed
description INTRODUCTION: Given the role of estrogen in breast carcinogenesis and the modification of estrogen receptor (ER) activity by its biochemical cofactors, we hypothesize that genetic variation within ER cofactor genes alters cellular response to estrogen exposure and consequently modifies the risk for ER-positive breast cancer. METHODS: We genotyped 790 tagging SNPs within 60 ER cofactor genes in 1,257 cases and 1,464 controls from Sweden and in 2,215 cases and 1,265 controls from Finland, and tested their associations with either ER-positive or ER-negative breast cancer. RESULTS: Seven SNPs showed consistent association with ER-positive breast cancer in the two independent samples, and six of them were located within PPARGC1B, encoding an ER co-activator, with the strongest association at rs741581 (odds ratio = 1.41, P = 4.84 × 10(-5)) that survived Bonferroni correction for multiple testing in the combined ER-positive breast cancer sample (P(corrected )= 0.03). Moreover, we also observed significant synergistic interaction (P(interaction )= 0.008) between the genetic polymorphisms within PPARGC1B and ESR1 in ER-positive breast cancer. By contrast, no consistent association was observed in ER-negative breast cancer. Furthermore, we found that administration of estrogen in the MCF-7 cell line induced PPARGC1B expression and enhanced occupancies of ER and RNA polymerase II within the region of SNP association, suggesting the upregulation of PPARGC1B expression by ESR1 activation. CONCLUSIONS: Our study revealed that DNA polymorphisms of PPARGC1B, coding a bona fide ER co-activator, are associated with ER-positive breast cancer risk. The feed-forward transcriptional regulatory loop between PPARGC1B and ESR1 further augments their protein interaction, which provides a plausible mechanistic explanation for the synergistic genetic interaction between PPARGC1B and ESR1 in ER-positive breast cancer. Our study also highlights that biochemically and genomically informed candidate gene studies can enhance the discovery of interactive disease susceptibility genes.
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spelling pubmed-31095782011-06-08 Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer Li, Yuqing Li, Yi Wedrén, Sara Li, Guoliang Charn, Tze Howe Desai, Kartiki Vasant Bonnard, Carine Czene, Kamila Humphreys, Keith Darabi, Hatef Einarsdóttir, Kristjana Heikkinen, Tuomas Aittomäki, Kristiina Blomqvist, Carl Chia, Kee Seng Nevanlinna, Heli Hall, Per Liu, Edison T Liu, Jianjun Breast Cancer Res Research Article INTRODUCTION: Given the role of estrogen in breast carcinogenesis and the modification of estrogen receptor (ER) activity by its biochemical cofactors, we hypothesize that genetic variation within ER cofactor genes alters cellular response to estrogen exposure and consequently modifies the risk for ER-positive breast cancer. METHODS: We genotyped 790 tagging SNPs within 60 ER cofactor genes in 1,257 cases and 1,464 controls from Sweden and in 2,215 cases and 1,265 controls from Finland, and tested their associations with either ER-positive or ER-negative breast cancer. RESULTS: Seven SNPs showed consistent association with ER-positive breast cancer in the two independent samples, and six of them were located within PPARGC1B, encoding an ER co-activator, with the strongest association at rs741581 (odds ratio = 1.41, P = 4.84 × 10(-5)) that survived Bonferroni correction for multiple testing in the combined ER-positive breast cancer sample (P(corrected )= 0.03). Moreover, we also observed significant synergistic interaction (P(interaction )= 0.008) between the genetic polymorphisms within PPARGC1B and ESR1 in ER-positive breast cancer. By contrast, no consistent association was observed in ER-negative breast cancer. Furthermore, we found that administration of estrogen in the MCF-7 cell line induced PPARGC1B expression and enhanced occupancies of ER and RNA polymerase II within the region of SNP association, suggesting the upregulation of PPARGC1B expression by ESR1 activation. CONCLUSIONS: Our study revealed that DNA polymorphisms of PPARGC1B, coding a bona fide ER co-activator, are associated with ER-positive breast cancer risk. The feed-forward transcriptional regulatory loop between PPARGC1B and ESR1 further augments their protein interaction, which provides a plausible mechanistic explanation for the synergistic genetic interaction between PPARGC1B and ESR1 in ER-positive breast cancer. Our study also highlights that biochemically and genomically informed candidate gene studies can enhance the discovery of interactive disease susceptibility genes. BioMed Central 2011 2011-01-26 /pmc/articles/PMC3109578/ /pubmed/21269472 http://dx.doi.org/10.1186/bcr2817 Text en Copyright ©2011 Li 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
Li, Yuqing
Li, Yi
Wedrén, Sara
Li, Guoliang
Charn, Tze Howe
Desai, Kartiki Vasant
Bonnard, Carine
Czene, Kamila
Humphreys, Keith
Darabi, Hatef
Einarsdóttir, Kristjana
Heikkinen, Tuomas
Aittomäki, Kristiina
Blomqvist, Carl
Chia, Kee Seng
Nevanlinna, Heli
Hall, Per
Liu, Edison T
Liu, Jianjun
Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title_full Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title_fullStr Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title_full_unstemmed Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title_short Genetic variation of ESR1 and its co-activator PPARGC1B is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
title_sort genetic variation of esr1 and its co-activator ppargc1b is synergistic in augmenting the risk of estrogen receptor-positive breast cancer
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3109578/
https://www.ncbi.nlm.nih.gov/pubmed/21269472
http://dx.doi.org/10.1186/bcr2817
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