Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold

Cell-specific expression of many genes is conveyed by multiple enhancers, with each individual enhancer controlling a particular expression domain. In contrast, multiple enhancers drive similar expression patterns of some genes involved in embryonic development, suggesting regulatory redundancy. Wor...

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Autores principales: Lam, Daniel D., de Souza, Flavio S. J., Nasif, Sofia, Yamashita, Miho, López-Leal, Rodrigo, Otero-Corchon, Veronica, Meece, Kana, Sampath, Harini, Mercer, Aaron J., Wardlaw, Sharon L., Rubinstein, Marcelo, Low, Malcolm J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4335486/
https://www.ncbi.nlm.nih.gov/pubmed/25671638
http://dx.doi.org/10.1371/journal.pgen.1004935
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author Lam, Daniel D.
de Souza, Flavio S. J.
Nasif, Sofia
Yamashita, Miho
López-Leal, Rodrigo
Otero-Corchon, Veronica
Meece, Kana
Sampath, Harini
Mercer, Aaron J.
Wardlaw, Sharon L.
Rubinstein, Marcelo
Low, Malcolm J.
author_facet Lam, Daniel D.
de Souza, Flavio S. J.
Nasif, Sofia
Yamashita, Miho
López-Leal, Rodrigo
Otero-Corchon, Veronica
Meece, Kana
Sampath, Harini
Mercer, Aaron J.
Wardlaw, Sharon L.
Rubinstein, Marcelo
Low, Malcolm J.
author_sort Lam, Daniel D.
collection PubMed
description Cell-specific expression of many genes is conveyed by multiple enhancers, with each individual enhancer controlling a particular expression domain. In contrast, multiple enhancers drive similar expression patterns of some genes involved in embryonic development, suggesting regulatory redundancy. Work in Drosophila has indicated that functionally overlapping enhancers canalize development by buffering gene expression against environmental and genetic disturbances. However, little is known about regulatory redundancy in vertebrates and in genes mainly expressed during adulthood. Here we study nPE1 and nPE2, two phylogenetically conserved mammalian enhancers that drive expression of the proopiomelanocortin gene (Pomc) to the same set of hypothalamic neurons. The simultaneous deletion of both enhancers abolished Pomc expression at all ages and induced a profound metabolic dysfunction including early-onset extreme obesity. Targeted inactivation of either nPE1 or nPE2 led to very low levels of Pomc expression during early embryonic development indicating that both enhancers function synergistically. In adult mice, however, Pomc expression is controlled additively by both enhancers, with nPE1 being responsible for ∼80% and nPE2 for ∼20% of Pomc transcription. Consequently, nPE1 knockout mice exhibit mild obesity whereas nPE2-deficient mice maintain a normal body weight. These results suggest that nPE2-driven Pomc expression is compensated by nPE1 at later stages of development, essentially rescuing the earlier phenotype of nPE2 deficiency. Together, these results reveal that cooperative interactions between the enhancers confer robustness of Pomc expression against gene regulatory disturbances and preclude deleterious metabolic phenotypes caused by Pomc deficiency in adulthood. Thus, our study demonstrates that enhancer redundancy can be used by genes that control adult physiology in mammals and underlines the potential significance of regulatory sequence mutations in common diseases.
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spelling pubmed-43354862015-03-04 Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold Lam, Daniel D. de Souza, Flavio S. J. Nasif, Sofia Yamashita, Miho López-Leal, Rodrigo Otero-Corchon, Veronica Meece, Kana Sampath, Harini Mercer, Aaron J. Wardlaw, Sharon L. Rubinstein, Marcelo Low, Malcolm J. PLoS Genet Research Article Cell-specific expression of many genes is conveyed by multiple enhancers, with each individual enhancer controlling a particular expression domain. In contrast, multiple enhancers drive similar expression patterns of some genes involved in embryonic development, suggesting regulatory redundancy. Work in Drosophila has indicated that functionally overlapping enhancers canalize development by buffering gene expression against environmental and genetic disturbances. However, little is known about regulatory redundancy in vertebrates and in genes mainly expressed during adulthood. Here we study nPE1 and nPE2, two phylogenetically conserved mammalian enhancers that drive expression of the proopiomelanocortin gene (Pomc) to the same set of hypothalamic neurons. The simultaneous deletion of both enhancers abolished Pomc expression at all ages and induced a profound metabolic dysfunction including early-onset extreme obesity. Targeted inactivation of either nPE1 or nPE2 led to very low levels of Pomc expression during early embryonic development indicating that both enhancers function synergistically. In adult mice, however, Pomc expression is controlled additively by both enhancers, with nPE1 being responsible for ∼80% and nPE2 for ∼20% of Pomc transcription. Consequently, nPE1 knockout mice exhibit mild obesity whereas nPE2-deficient mice maintain a normal body weight. These results suggest that nPE2-driven Pomc expression is compensated by nPE1 at later stages of development, essentially rescuing the earlier phenotype of nPE2 deficiency. Together, these results reveal that cooperative interactions between the enhancers confer robustness of Pomc expression against gene regulatory disturbances and preclude deleterious metabolic phenotypes caused by Pomc deficiency in adulthood. Thus, our study demonstrates that enhancer redundancy can be used by genes that control adult physiology in mammals and underlines the potential significance of regulatory sequence mutations in common diseases. Public Library of Science 2015-02-11 /pmc/articles/PMC4335486/ /pubmed/25671638 http://dx.doi.org/10.1371/journal.pgen.1004935 Text en © 2015 Lam et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Lam, Daniel D.
de Souza, Flavio S. J.
Nasif, Sofia
Yamashita, Miho
López-Leal, Rodrigo
Otero-Corchon, Veronica
Meece, Kana
Sampath, Harini
Mercer, Aaron J.
Wardlaw, Sharon L.
Rubinstein, Marcelo
Low, Malcolm J.
Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title_full Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title_fullStr Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title_full_unstemmed Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title_short Partially Redundant Enhancers Cooperatively Maintain Mammalian Pomc Expression Above a Critical Functional Threshold
title_sort partially redundant enhancers cooperatively maintain mammalian pomc expression above a critical functional threshold
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4335486/
https://www.ncbi.nlm.nih.gov/pubmed/25671638
http://dx.doi.org/10.1371/journal.pgen.1004935
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