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High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring

OBJECTIVES: Chronic and high consumption of fat constitutes an environmental stress that leads to metabolic diseases. We hypothesized that high-fat diet (HFD) transgenerationally remodels the epigenome of spermatozoa and metabolism of the offspring. METHODS: F0-male rats fed either HFD or chow diet...

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Autores principales: de Castro Barbosa, Thais, Ingerslev, Lars R., Alm, Petter S., Versteyhe, Soetkin, Massart, Julie, Rasmussen, Morten, Donkin, Ida, Sjögren, Rasmus, Mudry, Jonathan M., Vetterli, Laurène, Gupta, Shashank, Krook, Anna, Zierath, Juleen R., Barrès, Romain
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4770269/
https://www.ncbi.nlm.nih.gov/pubmed/26977389
http://dx.doi.org/10.1016/j.molmet.2015.12.002
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author de Castro Barbosa, Thais
Ingerslev, Lars R.
Alm, Petter S.
Versteyhe, Soetkin
Massart, Julie
Rasmussen, Morten
Donkin, Ida
Sjögren, Rasmus
Mudry, Jonathan M.
Vetterli, Laurène
Gupta, Shashank
Krook, Anna
Zierath, Juleen R.
Barrès, Romain
author_facet de Castro Barbosa, Thais
Ingerslev, Lars R.
Alm, Petter S.
Versteyhe, Soetkin
Massart, Julie
Rasmussen, Morten
Donkin, Ida
Sjögren, Rasmus
Mudry, Jonathan M.
Vetterli, Laurène
Gupta, Shashank
Krook, Anna
Zierath, Juleen R.
Barrès, Romain
author_sort de Castro Barbosa, Thais
collection PubMed
description OBJECTIVES: Chronic and high consumption of fat constitutes an environmental stress that leads to metabolic diseases. We hypothesized that high-fat diet (HFD) transgenerationally remodels the epigenome of spermatozoa and metabolism of the offspring. METHODS: F0-male rats fed either HFD or chow diet for 12 weeks were mated with chow-fed dams to generate F1 and F2 offspring. Motile spermatozoa were isolated from F0 and F1 breeders to determine DNA methylation and small non-coding RNA (sncRNA) expression pattern by deep sequencing. RESULTS: Newborn offspring of HFD-fed fathers had reduced body weight and pancreatic beta-cell mass. Adult female, but not male, offspring of HFD-fed fathers were glucose intolerant and resistant to HFD-induced weight gain. This phenotype was perpetuated in the F2 progeny, indicating transgenerational epigenetic inheritance. The epigenome of spermatozoa from HFD-fed F0 and their F1 male offspring showed common DNA methylation and small non-coding RNA expression signatures. Altered expression of sperm miRNA let-7c was passed down to metabolic tissues of the offspring, inducing a transcriptomic shift of the let-7c predicted targets. CONCLUSION: Our results provide insight into mechanisms by which HFD transgenerationally reprograms the epigenome of sperm cells, thereby affecting metabolic tissues of offspring throughout two generations.
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spelling pubmed-47702692016-03-14 High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring de Castro Barbosa, Thais Ingerslev, Lars R. Alm, Petter S. Versteyhe, Soetkin Massart, Julie Rasmussen, Morten Donkin, Ida Sjögren, Rasmus Mudry, Jonathan M. Vetterli, Laurène Gupta, Shashank Krook, Anna Zierath, Juleen R. Barrès, Romain Mol Metab Original Article OBJECTIVES: Chronic and high consumption of fat constitutes an environmental stress that leads to metabolic diseases. We hypothesized that high-fat diet (HFD) transgenerationally remodels the epigenome of spermatozoa and metabolism of the offspring. METHODS: F0-male rats fed either HFD or chow diet for 12 weeks were mated with chow-fed dams to generate F1 and F2 offspring. Motile spermatozoa were isolated from F0 and F1 breeders to determine DNA methylation and small non-coding RNA (sncRNA) expression pattern by deep sequencing. RESULTS: Newborn offspring of HFD-fed fathers had reduced body weight and pancreatic beta-cell mass. Adult female, but not male, offspring of HFD-fed fathers were glucose intolerant and resistant to HFD-induced weight gain. This phenotype was perpetuated in the F2 progeny, indicating transgenerational epigenetic inheritance. The epigenome of spermatozoa from HFD-fed F0 and their F1 male offspring showed common DNA methylation and small non-coding RNA expression signatures. Altered expression of sperm miRNA let-7c was passed down to metabolic tissues of the offspring, inducing a transcriptomic shift of the let-7c predicted targets. CONCLUSION: Our results provide insight into mechanisms by which HFD transgenerationally reprograms the epigenome of sperm cells, thereby affecting metabolic tissues of offspring throughout two generations. Elsevier 2015-12-25 /pmc/articles/PMC4770269/ /pubmed/26977389 http://dx.doi.org/10.1016/j.molmet.2015.12.002 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
de Castro Barbosa, Thais
Ingerslev, Lars R.
Alm, Petter S.
Versteyhe, Soetkin
Massart, Julie
Rasmussen, Morten
Donkin, Ida
Sjögren, Rasmus
Mudry, Jonathan M.
Vetterli, Laurène
Gupta, Shashank
Krook, Anna
Zierath, Juleen R.
Barrès, Romain
High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title_full High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title_fullStr High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title_full_unstemmed High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title_short High-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
title_sort high-fat diet reprograms the epigenome of rat spermatozoa and transgenerationally affects metabolism of the offspring
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4770269/
https://www.ncbi.nlm.nih.gov/pubmed/26977389
http://dx.doi.org/10.1016/j.molmet.2015.12.002
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