Elevated resistin levels induce central leptin resistance and increased atherosclerotic progression in mice

Ingrid W. Asterholm; Joseph M. Rutkowski; Teppei Fujikawa; You Ree Cho; Makoto Fukuda; Caroline Tao; Zhao Wang; Rana K Gupta; Joel K Elmquist; Philipp E Scherer

doi:10.1007/s00125-014-3210-3

Elevated resistin levels induce central leptin resistance and increased atherosclerotic progression in mice

Ingrid W. Asterholm, Joseph M. Rutkowski, Teppei Fujikawa, You Ree Cho, Makoto Fukuda, Caroline Tao, Zhao Wang, Rana K Gupta, Joel K Elmquist, Philipp E Scherer

Research output: Contribution to journal › Article › peer-review

42 Scopus citations

Abstract

Aims/hypothesis: Resistin was originally identified as an adipocyte-derived factor upregulated during obesity and as a contributor to obesity-associated insulin resistance. Clinically, resistin has also been implicated in cardiovascular disease in a number of different patient populations. Our aim was to simultaneously address these phenomena. Methods: We generated mice with modest adipocyte-specific resistin overexpression. These mice were crossed with mice deficient in the LDL receptor (Ldlr ^-/-) to probe the physiological role of resistin. Both metabolic and atherosclerotic assessments were performed. Results: Resistin overexpression led to increased atherosclerotic progression in Ldlr ^-/- mice. This was in part related to elevated serum triacylglycerol levels and a reduced ability to clear triacylglycerol upon a challenge. Additional phenotypic changes, such as increased body weight and reduced glucose clearance, independent of the Ldlr ^-/- background, confirmed increased adiposity associated with a more pronounced insulin resistance. A hallmark of elevated resistin was the disproportionate increase in circulating leptin levels. These mice thus recapitulated both the proposed negative cardiovascular correlation and the insulin resistance. A unifying mechanism for this complex phenotype was a resistin-mediated central leptin resistance, which we demonstrate directly both in vivo and in organotypic brain slices. In line with reduced sympathetic nervous system outflow, we found decreased brown adipose tissue (BAT) activity. The resulting elevated triacylglycerol levels provide a likely explanation for accelerated atherosclerosis. Conclusions/interpretation: Resistin overexpression leads to a complex metabolic phenotype driven by resistin-mediated central leptin resistance and reduced BAT activity. Hypothalamic leptin resistance thus provides a unifying mechanism for both resistin-mediated insulin resistance and enhanced atherosclerosis.

Original language	English (US)
Pages (from-to)	1209-1218
Number of pages	10
Journal	Diabetologia
Volume	57
Issue number	6
DOIs	https://doi.org/10.1007/s00125-014-3210-3
State	Published - Jun 2014

Keywords

Adipose tissue
Atherosclerosis
Brown adipose tissue
Insulin resistance
Leptin
Leptin resistance
Obesity
Resistin
Triacylglycerol
Type 2 diabetes

ASJC Scopus subject areas

Internal Medicine
Endocrinology, Diabetes and Metabolism

Access to Document

10.1007/s00125-014-3210-3

Cite this

@article{afbdda10791f486bbe9fd424563a448d,

title = "Elevated resistin levels induce central leptin resistance and increased atherosclerotic progression in mice",

abstract = "Aims/hypothesis: Resistin was originally identified as an adipocyte-derived factor upregulated during obesity and as a contributor to obesity-associated insulin resistance. Clinically, resistin has also been implicated in cardiovascular disease in a number of different patient populations. Our aim was to simultaneously address these phenomena. Methods: We generated mice with modest adipocyte-specific resistin overexpression. These mice were crossed with mice deficient in the LDL receptor (Ldlr -/-) to probe the physiological role of resistin. Both metabolic and atherosclerotic assessments were performed. Results: Resistin overexpression led to increased atherosclerotic progression in Ldlr -/- mice. This was in part related to elevated serum triacylglycerol levels and a reduced ability to clear triacylglycerol upon a challenge. Additional phenotypic changes, such as increased body weight and reduced glucose clearance, independent of the Ldlr -/- background, confirmed increased adiposity associated with a more pronounced insulin resistance. A hallmark of elevated resistin was the disproportionate increase in circulating leptin levels. These mice thus recapitulated both the proposed negative cardiovascular correlation and the insulin resistance. A unifying mechanism for this complex phenotype was a resistin-mediated central leptin resistance, which we demonstrate directly both in vivo and in organotypic brain slices. In line with reduced sympathetic nervous system outflow, we found decreased brown adipose tissue (BAT) activity. The resulting elevated triacylglycerol levels provide a likely explanation for accelerated atherosclerosis. Conclusions/interpretation: Resistin overexpression leads to a complex metabolic phenotype driven by resistin-mediated central leptin resistance and reduced BAT activity. Hypothalamic leptin resistance thus provides a unifying mechanism for both resistin-mediated insulin resistance and enhanced atherosclerosis.",

keywords = "Adipose tissue, Atherosclerosis, Brown adipose tissue, Insulin resistance, Leptin, Leptin resistance, Obesity, Resistin, Triacylglycerol, Type 2 diabetes",

author = "Asterholm, {Ingrid W.} and Rutkowski, {Joseph M.} and Teppei Fujikawa and Cho, {You Ree} and Makoto Fukuda and Caroline Tao and Zhao Wang and Gupta, {Rana K} and Elmquist, {Joel K} and Scherer, {Philipp E}",

note = "Funding Information: Funding sources The study was supported by the National Institutes of Health (grants R01-DK55758 and R01-DK099110 to PES and P01-DK088761 to PES and JKE). IWA was supported by the Throne-Holst Foundation, the Swedish Research Council (2006-3931 and 2012-1601), VINNOVA (2011-01336) and a NovoNordisk Excellence Project Award. JMR was supported by the American Heart Association (12SDG12050287). TF was supported by Juvenile Diabetes Research Foundation (3-2011-405). MF was supported by the AHA (09SDG2080223). RKG was supported by the NIH (grants K01-DK090120-02 and R03-DK099428) and Searle Scholars Program (Chicago, Illinois).",

year = "2014",

month = jun,

doi = "10.1007/s00125-014-3210-3",

language = "English (US)",

volume = "57",

pages = "1209--1218",

journal = "Diabetologia",

issn = "0012-186X",

publisher = "Springer Verlag",

number = "6",

}

TY - JOUR

T1 - Elevated resistin levels induce central leptin resistance and increased atherosclerotic progression in mice

AU - Asterholm, Ingrid W.

AU - Rutkowski, Joseph M.

AU - Fujikawa, Teppei

AU - Cho, You Ree

AU - Fukuda, Makoto

AU - Tao, Caroline

AU - Wang, Zhao

AU - Gupta, Rana K

AU - Elmquist, Joel K

AU - Scherer, Philipp E

N1 - Funding Information: Funding sources The study was supported by the National Institutes of Health (grants R01-DK55758 and R01-DK099110 to PES and P01-DK088761 to PES and JKE). IWA was supported by the Throne-Holst Foundation, the Swedish Research Council (2006-3931 and 2012-1601), VINNOVA (2011-01336) and a NovoNordisk Excellence Project Award. JMR was supported by the American Heart Association (12SDG12050287). TF was supported by Juvenile Diabetes Research Foundation (3-2011-405). MF was supported by the AHA (09SDG2080223). RKG was supported by the NIH (grants K01-DK090120-02 and R03-DK099428) and Searle Scholars Program (Chicago, Illinois).

PY - 2014/6

Y1 - 2014/6

N2 - Aims/hypothesis: Resistin was originally identified as an adipocyte-derived factor upregulated during obesity and as a contributor to obesity-associated insulin resistance. Clinically, resistin has also been implicated in cardiovascular disease in a number of different patient populations. Our aim was to simultaneously address these phenomena. Methods: We generated mice with modest adipocyte-specific resistin overexpression. These mice were crossed with mice deficient in the LDL receptor (Ldlr -/-) to probe the physiological role of resistin. Both metabolic and atherosclerotic assessments were performed. Results: Resistin overexpression led to increased atherosclerotic progression in Ldlr -/- mice. This was in part related to elevated serum triacylglycerol levels and a reduced ability to clear triacylglycerol upon a challenge. Additional phenotypic changes, such as increased body weight and reduced glucose clearance, independent of the Ldlr -/- background, confirmed increased adiposity associated with a more pronounced insulin resistance. A hallmark of elevated resistin was the disproportionate increase in circulating leptin levels. These mice thus recapitulated both the proposed negative cardiovascular correlation and the insulin resistance. A unifying mechanism for this complex phenotype was a resistin-mediated central leptin resistance, which we demonstrate directly both in vivo and in organotypic brain slices. In line with reduced sympathetic nervous system outflow, we found decreased brown adipose tissue (BAT) activity. The resulting elevated triacylglycerol levels provide a likely explanation for accelerated atherosclerosis. Conclusions/interpretation: Resistin overexpression leads to a complex metabolic phenotype driven by resistin-mediated central leptin resistance and reduced BAT activity. Hypothalamic leptin resistance thus provides a unifying mechanism for both resistin-mediated insulin resistance and enhanced atherosclerosis.

AB - Aims/hypothesis: Resistin was originally identified as an adipocyte-derived factor upregulated during obesity and as a contributor to obesity-associated insulin resistance. Clinically, resistin has also been implicated in cardiovascular disease in a number of different patient populations. Our aim was to simultaneously address these phenomena. Methods: We generated mice with modest adipocyte-specific resistin overexpression. These mice were crossed with mice deficient in the LDL receptor (Ldlr -/-) to probe the physiological role of resistin. Both metabolic and atherosclerotic assessments were performed. Results: Resistin overexpression led to increased atherosclerotic progression in Ldlr -/- mice. This was in part related to elevated serum triacylglycerol levels and a reduced ability to clear triacylglycerol upon a challenge. Additional phenotypic changes, such as increased body weight and reduced glucose clearance, independent of the Ldlr -/- background, confirmed increased adiposity associated with a more pronounced insulin resistance. A hallmark of elevated resistin was the disproportionate increase in circulating leptin levels. These mice thus recapitulated both the proposed negative cardiovascular correlation and the insulin resistance. A unifying mechanism for this complex phenotype was a resistin-mediated central leptin resistance, which we demonstrate directly both in vivo and in organotypic brain slices. In line with reduced sympathetic nervous system outflow, we found decreased brown adipose tissue (BAT) activity. The resulting elevated triacylglycerol levels provide a likely explanation for accelerated atherosclerosis. Conclusions/interpretation: Resistin overexpression leads to a complex metabolic phenotype driven by resistin-mediated central leptin resistance and reduced BAT activity. Hypothalamic leptin resistance thus provides a unifying mechanism for both resistin-mediated insulin resistance and enhanced atherosclerosis.

KW - Adipose tissue

KW - Atherosclerosis

KW - Brown adipose tissue

KW - Insulin resistance

KW - Leptin

KW - Leptin resistance

KW - Obesity

KW - Resistin

KW - Triacylglycerol

KW - Type 2 diabetes

UR - http://www.scopus.com/inward/record.url?scp=84901196379&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84901196379&partnerID=8YFLogxK

U2 - 10.1007/s00125-014-3210-3

DO - 10.1007/s00125-014-3210-3

M3 - Article

C2 - 24623101

AN - SCOPUS:84901196379

SN - 0012-186X

VL - 57

SP - 1209

EP - 1218

JO - Diabetologia

JF - Diabetologia

IS - 6

ER -

Elevated resistin levels induce central leptin resistance and increased atherosclerotic progression in mice

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this