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Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains

Maternal care is essential in mammals, and variations in the environment provided by mothers may directly influence the viability of newborns and emotional behavior later in life. A previous study investigated genetic variations associated with maternal care in an intercross of LG/J and SM/J inbred...

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Autores principales: Chiavegatto, Silvana, Sauce, Bruno, Ambar, Guilherme, Cheverud, James M, Peripato, Andrea C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Inc 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3432959/
https://www.ncbi.nlm.nih.gov/pubmed/22950040
http://dx.doi.org/10.1002/brb3.58
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author Chiavegatto, Silvana
Sauce, Bruno
Ambar, Guilherme
Cheverud, James M
Peripato, Andrea C
author_facet Chiavegatto, Silvana
Sauce, Bruno
Ambar, Guilherme
Cheverud, James M
Peripato, Andrea C
author_sort Chiavegatto, Silvana
collection PubMed
description Maternal care is essential in mammals, and variations in the environment provided by mothers may directly influence the viability of newborns and emotional behavior later in life. A previous study investigated genetic variations associated with maternal care in an intercross of LG/J and SM/J inbred mouse strains and identified two single-locus QTLs (quantitative trait loci). Here, we selected three candidate genes located within these QTLs intervals; Oxt on chromosome 2, and FosB and Peg3 on chromosome 7 and tested their association with maternal care. LG/J females showed impaired postpartum nest building and pup retrieval, a one-day delay in milk ejection, reduced exploratory activity, and higher anxiety-like behavior when compared to SM/J females. The nucleotide sequences of Oxt and FosB were similar between strains, as were their hypothalamic expression levels. Conversely, Peg3 nucleotide sequences showed four nonsynonymous replacement substitutions on LG/J dams, T11062G, G13744A, A13808G, and G13813A, and a 30 base pair (10 aa) in tandem repeat in the coding region with three copies in SM/J and five copies in LG/J. Maternal care impaired LG/J mothers express 37% lower Peg3 mRNA levels in the hypothalamus on the second postpartum day. We also found an association of the Peg3 repeat-variant and poor maternal care in F(2) heterozygote females derived from a LG/J × SM/J intercross. These results may suggest that the maternally imprinted Peg3 gene is responsible for the single-locus QTL on chromosome 7 that has been shown to influence maternal care in these strains. Furthermore, these data provide additional support for an epigenetic regulation of maternal behavior.
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spelling pubmed-34329592012-09-04 Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains Chiavegatto, Silvana Sauce, Bruno Ambar, Guilherme Cheverud, James M Peripato, Andrea C Brain Behav Original Research Maternal care is essential in mammals, and variations in the environment provided by mothers may directly influence the viability of newborns and emotional behavior later in life. A previous study investigated genetic variations associated with maternal care in an intercross of LG/J and SM/J inbred mouse strains and identified two single-locus QTLs (quantitative trait loci). Here, we selected three candidate genes located within these QTLs intervals; Oxt on chromosome 2, and FosB and Peg3 on chromosome 7 and tested their association with maternal care. LG/J females showed impaired postpartum nest building and pup retrieval, a one-day delay in milk ejection, reduced exploratory activity, and higher anxiety-like behavior when compared to SM/J females. The nucleotide sequences of Oxt and FosB were similar between strains, as were their hypothalamic expression levels. Conversely, Peg3 nucleotide sequences showed four nonsynonymous replacement substitutions on LG/J dams, T11062G, G13744A, A13808G, and G13813A, and a 30 base pair (10 aa) in tandem repeat in the coding region with three copies in SM/J and five copies in LG/J. Maternal care impaired LG/J mothers express 37% lower Peg3 mRNA levels in the hypothalamus on the second postpartum day. We also found an association of the Peg3 repeat-variant and poor maternal care in F(2) heterozygote females derived from a LG/J × SM/J intercross. These results may suggest that the maternally imprinted Peg3 gene is responsible for the single-locus QTL on chromosome 7 that has been shown to influence maternal care in these strains. Furthermore, these data provide additional support for an epigenetic regulation of maternal behavior. Blackwell Publishing Inc 2012-07 /pmc/articles/PMC3432959/ /pubmed/22950040 http://dx.doi.org/10.1002/brb3.58 Text en © 2012 The Authors. Published by Wiley Periodicals, Inc. http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Original Research
Chiavegatto, Silvana
Sauce, Bruno
Ambar, Guilherme
Cheverud, James M
Peripato, Andrea C
Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title_full Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title_fullStr Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title_full_unstemmed Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title_short Hypothalamic expression of Peg3 gene is associated with maternal care differences between SM/J and LG/J mouse strains
title_sort hypothalamic expression of peg3 gene is associated with maternal care differences between sm/j and lg/j mouse strains
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3432959/
https://www.ncbi.nlm.nih.gov/pubmed/22950040
http://dx.doi.org/10.1002/brb3.58
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