Hepatocyte toll-like receptor 4 regulates obesity-induced inflammation and insulin resistance

Lin Jia; Claudia R. Vianna; Makoto Fukuda; Eric D. Berglund; Chen Liu; Caroline Tao; Kai Sun; Tiemin Liu; Matthew J. Harper; Charlotte E. Lee; Syann Lee; Philipp E. Scherer; Joel K. Elmquist

doi:10.1038/ncomms4878

Hepatocyte toll-like receptor 4 regulates obesity-induced inflammation and insulin resistance

Lin Jia, Claudia R. Vianna, Makoto Fukuda, Eric D. Berglund, Chen Liu, Caroline Tao, Kai Sun, Tiemin Liu, Matthew J. Harper, Charlotte E. Lee, Syann Lee, Philipp E. Scherer, Joel K. Elmquist

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Abstract

Chronic low-grade inflammation is a hallmark of obesity and thought to contribute to the development of obesity-related insulin resistance. Toll-like receptor 4 (Tlr4) is a key mediator of pro-inflammatory responses. Mice lacking Tlr4s are protected from diet-induced insulin resistance and inflammation; however, which Tlr4-expressing cells mediate this effect is unknown. Here we show that mice deficient in hepatocyte Tlr4 (Tlr4^LKO) exhibit improved glucose tolerance, enhanced insulin sensitivity and ameliorated hepatic steatosis despite the development of obesity after a high-fat diet (HFD) challenge. Furthermore, Tlr4^LKO mice have reduced macrophage content in white adipose tissue, as well as decreased tissue and circulating inflammatory markers. In contrast, the loss of Tlr4 activity in myeloid cells has little effect on insulin sensitivity. Collectively, these data indicate that the activation of Tlr4 on hepatocytes contributes to obesity-associated inflammation and insulin resistance, and suggest that targeting hepatocyte Tlr4 might be a useful therapeutic strategy for the treatment of type 2 diabetes.

Original language	English (US)
Article number	3878
Journal	Nature communications
Volume	5
DOIs	https://doi.org/10.1038/ncomms4878
State	Published - May 12 2014

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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title = "Hepatocyte toll-like receptor 4 regulates obesity-induced inflammation and insulin resistance",

abstract = "Chronic low-grade inflammation is a hallmark of obesity and thought to contribute to the development of obesity-related insulin resistance. Toll-like receptor 4 (Tlr4) is a key mediator of pro-inflammatory responses. Mice lacking Tlr4s are protected from diet-induced insulin resistance and inflammation; however, which Tlr4-expressing cells mediate this effect is unknown. Here we show that mice deficient in hepatocyte Tlr4 (Tlr4LKO) exhibit improved glucose tolerance, enhanced insulin sensitivity and ameliorated hepatic steatosis despite the development of obesity after a high-fat diet (HFD) challenge. Furthermore, Tlr4LKO mice have reduced macrophage content in white adipose tissue, as well as decreased tissue and circulating inflammatory markers. In contrast, the loss of Tlr4 activity in myeloid cells has little effect on insulin sensitivity. Collectively, these data indicate that the activation of Tlr4 on hepatocytes contributes to obesity-associated inflammation and insulin resistance, and suggest that targeting hepatocyte Tlr4 might be a useful therapeutic strategy for the treatment of type 2 diabetes.",

author = "Lin Jia and Vianna, {Claudia R.} and Makoto Fukuda and Berglund, {Eric D.} and Chen Liu and Caroline Tao and Kai Sun and Tiemin Liu and Harper, {Matthew J.} and Lee, {Charlotte E.} and Syann Lee and Scherer, {Philipp E.} and Elmquist, {Joel K.}",

note = "Funding Information: We thank the employees at the Mouse Metabolic Phenotyping Core of UTSW for their technical assistance. These studies were supported by the National Institutes of Health grant P01-DK088761 to P.E.S and J.K.E. L.J. was supported by a Ruth L. Kirschstein National Research Service Award (RL9 DK081180 Postdoctoral Training grant).",

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AU - Jia, Lin

AU - Vianna, Claudia R.

AU - Fukuda, Makoto

AU - Berglund, Eric D.

AU - Liu, Chen

AU - Tao, Caroline

AU - Sun, Kai

AU - Liu, Tiemin

AU - Harper, Matthew J.

AU - Lee, Charlotte E.

AU - Lee, Syann

AU - Scherer, Philipp E.

AU - Elmquist, Joel K.

N1 - Funding Information: We thank the employees at the Mouse Metabolic Phenotyping Core of UTSW for their technical assistance. These studies were supported by the National Institutes of Health grant P01-DK088761 to P.E.S and J.K.E. L.J. was supported by a Ruth L. Kirschstein National Research Service Award (RL9 DK081180 Postdoctoral Training grant).

PY - 2014/5/12

Y1 - 2014/5/12

N2 - Chronic low-grade inflammation is a hallmark of obesity and thought to contribute to the development of obesity-related insulin resistance. Toll-like receptor 4 (Tlr4) is a key mediator of pro-inflammatory responses. Mice lacking Tlr4s are protected from diet-induced insulin resistance and inflammation; however, which Tlr4-expressing cells mediate this effect is unknown. Here we show that mice deficient in hepatocyte Tlr4 (Tlr4LKO) exhibit improved glucose tolerance, enhanced insulin sensitivity and ameliorated hepatic steatosis despite the development of obesity after a high-fat diet (HFD) challenge. Furthermore, Tlr4LKO mice have reduced macrophage content in white adipose tissue, as well as decreased tissue and circulating inflammatory markers. In contrast, the loss of Tlr4 activity in myeloid cells has little effect on insulin sensitivity. Collectively, these data indicate that the activation of Tlr4 on hepatocytes contributes to obesity-associated inflammation and insulin resistance, and suggest that targeting hepatocyte Tlr4 might be a useful therapeutic strategy for the treatment of type 2 diabetes.

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Hepatocyte toll-like receptor 4 regulates obesity-induced inflammation and insulin resistance

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