P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates

AIMS: Familial partial lipodystrophic syndrome 3 (FPLD3) is associated with mutations in the transcription factor PPARγ. One of these mutations, the P467L, confers a dominant negative effect. We and others have previously investigated the pathophysiology associated with this mutation using a humaniz...

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Autores principales: Rodriguez‐Cuenca, Sergio, Carobbio, Stefania, Barceló‐Coblijn, Gwendolyn, Prieur, Xavier, Relat, Joana, Amat, Ramon, Campbell, Mark, Dias, Ana Rita, Bahri, Myriam, Gray, Sarah L., Vidal‐Puig, Antonio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2018
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Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6589924/
https://www.ncbi.nlm.nih.gov/pubmed/29790245
http://dx.doi.org/10.1111/dom.13370
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author Rodriguez‐Cuenca, Sergio
Carobbio, Stefania
Barceló‐Coblijn, Gwendolyn
Prieur, Xavier
Relat, Joana
Amat, Ramon
Campbell, Mark
Dias, Ana Rita
Bahri, Myriam
Gray, Sarah L.
Vidal‐Puig, Antonio
author_facet Rodriguez‐Cuenca, Sergio
Carobbio, Stefania
Barceló‐Coblijn, Gwendolyn
Prieur, Xavier
Relat, Joana
Amat, Ramon
Campbell, Mark
Dias, Ana Rita
Bahri, Myriam
Gray, Sarah L.
Vidal‐Puig, Antonio
author_sort Rodriguez‐Cuenca, Sergio
collection PubMed
description AIMS: Familial partial lipodystrophic syndrome 3 (FPLD3) is associated with mutations in the transcription factor PPARγ. One of these mutations, the P467L, confers a dominant negative effect. We and others have previously investigated the pathophysiology associated with this mutation using a humanized mouse model that recapitulates most of the clinical symptoms observed in patients who have been phenotyped under different experimental conditions. One of the key clinical manifestations observed, both in humans and mouse models, is the ectopic accumulation of fat in the liver. With this study we aim to dissect the molecular mechanisms that contribute to the excessive accumulation of lipids in the liver and characterize the negative effect of this PPARγ mutation on the activity of PPARα in vivo when activated by fibrates. MATERIAL AND METHODS: P465L‐PPAR mutant and wild‐type mice were divided into 8 experimental groups, 4 different conditions per genotype. Briefly, mice were fed a chow diet or a high‐fat diet (HFD 45% Kcal from fat) for a period of 28 days and treated with WY14643 or vehicle for five days before culling. At the end of the experiment, tissues and plasma were collected. We performed extensive gene expression, fatty acid composition and histological analysis in the livers. The serum collected was used to measure several metabolites and to perform basic lipoprotein profile. RESULTS: P465L mice showed increased levels of insulin and free fatty acids (FFA) as well as increased liver steatosis. They also exhibit decreased levels of very low density lipoproteins (VLDL) when fed an HFD. We also provide evidence of impaired expression of a number of well‐established PPARα target genes in the P465L mutant livers. CONCLUSION: Our data demonstrate that P465L confers partial resistance to the hypolipidemic action of fibrates. These results show that the fatty liver phenotype observed in P465L mutant mice is not only the consequence of dysfunctional adipose tissue, but also involves defective liver metabolism. All in all, the deleterious effects of P465L‐PPARγ mutation may be magnified by their collateral negative effect on PPARα function.
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spelling pubmed-65899242019-07-08 P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates Rodriguez‐Cuenca, Sergio Carobbio, Stefania Barceló‐Coblijn, Gwendolyn Prieur, Xavier Relat, Joana Amat, Ramon Campbell, Mark Dias, Ana Rita Bahri, Myriam Gray, Sarah L. Vidal‐Puig, Antonio Diabetes Obes Metab Original Articles AIMS: Familial partial lipodystrophic syndrome 3 (FPLD3) is associated with mutations in the transcription factor PPARγ. One of these mutations, the P467L, confers a dominant negative effect. We and others have previously investigated the pathophysiology associated with this mutation using a humanized mouse model that recapitulates most of the clinical symptoms observed in patients who have been phenotyped under different experimental conditions. One of the key clinical manifestations observed, both in humans and mouse models, is the ectopic accumulation of fat in the liver. With this study we aim to dissect the molecular mechanisms that contribute to the excessive accumulation of lipids in the liver and characterize the negative effect of this PPARγ mutation on the activity of PPARα in vivo when activated by fibrates. MATERIAL AND METHODS: P465L‐PPAR mutant and wild‐type mice were divided into 8 experimental groups, 4 different conditions per genotype. Briefly, mice were fed a chow diet or a high‐fat diet (HFD 45% Kcal from fat) for a period of 28 days and treated with WY14643 or vehicle for five days before culling. At the end of the experiment, tissues and plasma were collected. We performed extensive gene expression, fatty acid composition and histological analysis in the livers. The serum collected was used to measure several metabolites and to perform basic lipoprotein profile. RESULTS: P465L mice showed increased levels of insulin and free fatty acids (FFA) as well as increased liver steatosis. They also exhibit decreased levels of very low density lipoproteins (VLDL) when fed an HFD. We also provide evidence of impaired expression of a number of well‐established PPARα target genes in the P465L mutant livers. CONCLUSION: Our data demonstrate that P465L confers partial resistance to the hypolipidemic action of fibrates. These results show that the fatty liver phenotype observed in P465L mutant mice is not only the consequence of dysfunctional adipose tissue, but also involves defective liver metabolism. All in all, the deleterious effects of P465L‐PPARγ mutation may be magnified by their collateral negative effect on PPARα function. Blackwell Publishing Ltd 2018-06-27 2018-10 /pmc/articles/PMC6589924/ /pubmed/29790245 http://dx.doi.org/10.1111/dom.13370 Text en © 2018 The Authors. Diabetes, Obesity and Metabolism Published by John Wiley & Sons Ltd This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Rodriguez‐Cuenca, Sergio
Carobbio, Stefania
Barceló‐Coblijn, Gwendolyn
Prieur, Xavier
Relat, Joana
Amat, Ramon
Campbell, Mark
Dias, Ana Rita
Bahri, Myriam
Gray, Sarah L.
Vidal‐Puig, Antonio
P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title_full P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title_fullStr P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title_full_unstemmed P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title_short P465L‐PPARγ mutation confers partial resistance to the hypolipidaemic action of fibrates
title_sort p465l‐pparγ mutation confers partial resistance to the hypolipidaemic action of fibrates
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6589924/
https://www.ncbi.nlm.nih.gov/pubmed/29790245
http://dx.doi.org/10.1111/dom.13370
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