Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance

OBJECTIVE: The nuclear receptor TAK1/TR4/NR2C2 is expressed in several tissues that are important in the control of energy homeostasis. In this study, we investigate whether TAK1 functions as a regulator of lipid and energy homeostasis and has a role in metabolic syndrome. RESEARCH DESIGN AND METHOD...

Descripción completa

Detalles Bibliográficos
Autores principales: Kang, Hong Soon, Okamoto, Kyoko, Kim, Yong-Sik, Takeda, Yukimasa, Bortner, Carl D., Dang, Huaixin, Wada, Taira, Xie, Wen, Yang, Xiao-Ping, Liao, Grace, Jetten, Anton M.
Formato: Texto
Lenguaje:English
Publicado: American Diabetes Association 2011
Materias:
Obesity Studies
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3012170/
https://www.ncbi.nlm.nih.gov/pubmed/20864514
http://dx.doi.org/10.2337/db10-0628
_version_ 1782195089136680960
author Kang, Hong Soon
Okamoto, Kyoko
Kim, Yong-Sik
Takeda, Yukimasa
Bortner, Carl D.
Dang, Huaixin
Wada, Taira
Xie, Wen
Yang, Xiao-Ping
Liao, Grace
Jetten, Anton M.
author_facet Kang, Hong Soon
Okamoto, Kyoko
Kim, Yong-Sik
Takeda, Yukimasa
Bortner, Carl D.
Dang, Huaixin
Wada, Taira
Xie, Wen
Yang, Xiao-Ping
Liao, Grace
Jetten, Anton M.
author_sort Kang, Hong Soon
collection PubMed
description OBJECTIVE: The nuclear receptor TAK1/TR4/NR2C2 is expressed in several tissues that are important in the control of energy homeostasis. In this study, we investigate whether TAK1 functions as a regulator of lipid and energy homeostasis and has a role in metabolic syndrome. RESEARCH DESIGN AND METHODS: We generated TAK1-deficient (TAK1(−/−)) mice to study the function of TAK1 in the development of metabolic syndrome in aged mice and mice fed a high-fat diet (HFD). (Immuno)histochemical, biochemical, and gene expression profile analyses were performed to determine the effect of the loss of TAK1 expression on lipid homeostasis in liver and adipose tissues. In addition, insulin sensitivity, energy expenditure, and adipose-associated inflammation were compared in wild-type (WT) and TAK1(−/−) mice fed a HFD. RESULTS: TAK1-deficient (TAK1(−/−)) mice are resistant to the development of age- and HFD-induced metabolic syndrome. Histo- and biochemical analyses showed significantly lower hepatic triglyceride levels and reduced lipid accumulation in adipose tissue in TAK1(−/−) mice compared with WT mice. Gene expression profiling analysis revealed that the expression of several genes encoding proteins involved in lipid uptake and triglyceride synthesis and storage, including Cidea, Cidec, Mogat1, and CD36, was greatly decreased in the liver and primary hepatocytes of TAK1(−/−) mice. Restoration of TAK1 expression in TAK1(−/−) hepatocytes induced expression of several lipogenic genes. Moreover, TAK1(−/−) mice exhibited reduced infiltration of inflammatory cells and expression of inflammatory genes in white adipose tissue, and were resistant to the development of glucose intolerance and insulin resistance. TAK1(−/−) mice consume more oxygen and produce more carbon dioxide than WT mice, suggesting increased energy expenditure. CONCLUSIONS: Our data reveal that TAK1 plays a critical role in the regulation of energy and lipid homeostasis, and promotes the development of metabolic syndrome. TAK1 may provide a new therapeutic target in the management of obesity, diabetes, and liver steatosis.
format Text
id pubmed-3012170
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher American Diabetes Association
record_format MEDLINE/PubMed
spelling pubmed-30121702012-01-01 Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance Kang, Hong Soon Okamoto, Kyoko Kim, Yong-Sik Takeda, Yukimasa Bortner, Carl D. Dang, Huaixin Wada, Taira Xie, Wen Yang, Xiao-Ping Liao, Grace Jetten, Anton M. Diabetes Obesity Studies OBJECTIVE: The nuclear receptor TAK1/TR4/NR2C2 is expressed in several tissues that are important in the control of energy homeostasis. In this study, we investigate whether TAK1 functions as a regulator of lipid and energy homeostasis and has a role in metabolic syndrome. RESEARCH DESIGN AND METHODS: We generated TAK1-deficient (TAK1(−/−)) mice to study the function of TAK1 in the development of metabolic syndrome in aged mice and mice fed a high-fat diet (HFD). (Immuno)histochemical, biochemical, and gene expression profile analyses were performed to determine the effect of the loss of TAK1 expression on lipid homeostasis in liver and adipose tissues. In addition, insulin sensitivity, energy expenditure, and adipose-associated inflammation were compared in wild-type (WT) and TAK1(−/−) mice fed a HFD. RESULTS: TAK1-deficient (TAK1(−/−)) mice are resistant to the development of age- and HFD-induced metabolic syndrome. Histo- and biochemical analyses showed significantly lower hepatic triglyceride levels and reduced lipid accumulation in adipose tissue in TAK1(−/−) mice compared with WT mice. Gene expression profiling analysis revealed that the expression of several genes encoding proteins involved in lipid uptake and triglyceride synthesis and storage, including Cidea, Cidec, Mogat1, and CD36, was greatly decreased in the liver and primary hepatocytes of TAK1(−/−) mice. Restoration of TAK1 expression in TAK1(−/−) hepatocytes induced expression of several lipogenic genes. Moreover, TAK1(−/−) mice exhibited reduced infiltration of inflammatory cells and expression of inflammatory genes in white adipose tissue, and were resistant to the development of glucose intolerance and insulin resistance. TAK1(−/−) mice consume more oxygen and produce more carbon dioxide than WT mice, suggesting increased energy expenditure. CONCLUSIONS: Our data reveal that TAK1 plays a critical role in the regulation of energy and lipid homeostasis, and promotes the development of metabolic syndrome. TAK1 may provide a new therapeutic target in the management of obesity, diabetes, and liver steatosis. American Diabetes Association 2011-01 2010-09-23 /pmc/articles/PMC3012170/ /pubmed/20864514 http://dx.doi.org/10.2337/db10-0628 Text en © 2011 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Obesity Studies
Kang, Hong Soon
Okamoto, Kyoko
Kim, Yong-Sik
Takeda, Yukimasa
Bortner, Carl D.
Dang, Huaixin
Wada, Taira
Xie, Wen
Yang, Xiao-Ping
Liao, Grace
Jetten, Anton M.
Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title_full Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title_fullStr Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title_full_unstemmed Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title_short Nuclear Orphan Receptor TAK1/TR4-Deficient Mice Are Protected Against Obesity-Linked Inflammation, Hepatic Steatosis, and Insulin Resistance
title_sort nuclear orphan receptor tak1/tr4-deficient mice are protected against obesity-linked inflammation, hepatic steatosis, and insulin resistance
topic Obesity Studies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3012170/
https://www.ncbi.nlm.nih.gov/pubmed/20864514
http://dx.doi.org/10.2337/db10-0628
work_keys_str_mv AT kanghongsoon nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT okamotokyoko nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT kimyongsik nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT takedayukimasa nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT bortnercarld nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT danghuaixin nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT wadataira nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT xiewen nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT yangxiaoping nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT liaograce nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance
AT jettenantonm nuclearorphanreceptortak1tr4deficientmiceareprotectedagainstobesitylinkedinflammationhepaticsteatosisandinsulinresistance

Ejemplares similares