Adipocyte lipid chaperone aP2 Is a secreted adipokine regulating hepatic glucose production

Haiming Cao; Motohiro Sekiya; Meric Erikci Ertunc; M. Furkan Burak; Jared R. Mayers; Ariel White; Karen Inouye; Lisa M. Rickey; Baris C. Ercal; Masato Furuhashi; Gürol Tuncman; Gökhan S. Hotamisligil

doi:10.1016/j.cmet.2013.04.012

Adipocyte lipid chaperone aP2 Is a secreted adipokine regulating hepatic glucose production

Haiming Cao, Motohiro Sekiya, Meric Erikci Ertunc, M. Furkan Burak, Jared R. Mayers, Ariel White, Karen Inouye, Lisa M. Rickey, Baris C. Ercal, Masato Furuhashi, Gürol Tuncman, Gökhan S. Hotamisligil

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223 Scopus citations

Abstract

Proper control of hepatic glucose production is central to whole-body glucose homeostasis, and its disruption plays a major role in diabetes. Here, we demonstrate that although established as an intracellular lipid chaperone, aP2 is in fact actively secreted from adipocytes to control liver glucose metabolism. Secretion of aP2 from adipocytes is regulated by fasting- and lipolysis-related signals, and circulating aP2 levels are markedly elevated in mouse and human obesity. Recombinant aP2 stimulates glucose production and gluconeogenic activity in primary hepatocytes in vitro and in lean mice in vivo. In contrast, neutralization of secreted aP2 reduces glucose production and corrects the diabetic phenotype of obese mice. Hyperinsulinemic-euglycemic and pancreatic clamp studies upon aP2 administration or neutralization demonstrated actions of aP2 in liver. We conclude that aP2 is an adipokine linking adipocytes to hepatic glucose production and that neutralizing secreted aP2 may represent an effective therapeutic strategy against diabetes.

Original language	English
Pages (from-to)	768-778
Number of pages	11
Journal	Cell metabolism
Volume	17
Issue number	5
DOIs	https://doi.org/10.1016/j.cmet.2013.04.012
State	Published - May 7 2013

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title = "Adipocyte lipid chaperone aP2 Is a secreted adipokine regulating hepatic glucose production",

abstract = "Proper control of hepatic glucose production is central to whole-body glucose homeostasis, and its disruption plays a major role in diabetes. Here, we demonstrate that although established as an intracellular lipid chaperone, aP2 is in fact actively secreted from adipocytes to control liver glucose metabolism. Secretion of aP2 from adipocytes is regulated by fasting- and lipolysis-related signals, and circulating aP2 levels are markedly elevated in mouse and human obesity. Recombinant aP2 stimulates glucose production and gluconeogenic activity in primary hepatocytes in vitro and in lean mice in vivo. In contrast, neutralization of secreted aP2 reduces glucose production and corrects the diabetic phenotype of obese mice. Hyperinsulinemic-euglycemic and pancreatic clamp studies upon aP2 administration or neutralization demonstrated actions of aP2 in liver. We conclude that aP2 is an adipokine linking adipocytes to hepatic glucose production and that neutralizing secreted aP2 may represent an effective therapeutic strategy against diabetes.",

author = "Haiming Cao and Motohiro Sekiya and Ertunc, {Meric Erikci} and Burak, {M. Furkan} and Mayers, {Jared R.} and Ariel White and Karen Inouye and Rickey, {Lisa M.} and Ercal, {Baris C.} and Masato Furuhashi and G{\"u}rol Tuncman and Hotamisligil, {G{\"o}khan S.}",

note = "Funding Information: This work was supported in part by a National Institutes of Health (NIH) grant DK064360 (to G.S.H.). H.C. was supported by fellowships from the NIH Roadmap (DK71507-04) and the American Diabetes Association. M.E.E. was supported by the Roadmap Grant R90 DK071507 from NIH. M.S. was supported by a fellowship from the Manpei Suzuki Diabetes Foundation. M.F. was supported by fellowships from the Japan Society for the Promotion of Science and the American Diabetes Association. We thank Michael Alcala for technical help, Eric Rimm for providing human samples, Fahri Saatcioglu for scientific insights and discussion, Megan Washack for editorial assistance, and Ana Paula Arruda for the graphical abstract. The technology described in this manuscript is licensed to the biopharmaceutical company UCB, Union Chimique Belge. ",

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AU - Cao, Haiming

AU - Sekiya, Motohiro

AU - Ertunc, Meric Erikci

AU - Burak, M. Furkan

AU - Mayers, Jared R.

AU - White, Ariel

AU - Inouye, Karen

AU - Rickey, Lisa M.

AU - Ercal, Baris C.

AU - Furuhashi, Masato

AU - Tuncman, Gürol

AU - Hotamisligil, Gökhan S.

N1 - Funding Information: This work was supported in part by a National Institutes of Health (NIH) grant DK064360 (to G.S.H.). H.C. was supported by fellowships from the NIH Roadmap (DK71507-04) and the American Diabetes Association. M.E.E. was supported by the Roadmap Grant R90 DK071507 from NIH. M.S. was supported by a fellowship from the Manpei Suzuki Diabetes Foundation. M.F. was supported by fellowships from the Japan Society for the Promotion of Science and the American Diabetes Association. We thank Michael Alcala for technical help, Eric Rimm for providing human samples, Fahri Saatcioglu for scientific insights and discussion, Megan Washack for editorial assistance, and Ana Paula Arruda for the graphical abstract. The technology described in this manuscript is licensed to the biopharmaceutical company UCB, Union Chimique Belge.

PY - 2013/5/7

Y1 - 2013/5/7

N2 - Proper control of hepatic glucose production is central to whole-body glucose homeostasis, and its disruption plays a major role in diabetes. Here, we demonstrate that although established as an intracellular lipid chaperone, aP2 is in fact actively secreted from adipocytes to control liver glucose metabolism. Secretion of aP2 from adipocytes is regulated by fasting- and lipolysis-related signals, and circulating aP2 levels are markedly elevated in mouse and human obesity. Recombinant aP2 stimulates glucose production and gluconeogenic activity in primary hepatocytes in vitro and in lean mice in vivo. In contrast, neutralization of secreted aP2 reduces glucose production and corrects the diabetic phenotype of obese mice. Hyperinsulinemic-euglycemic and pancreatic clamp studies upon aP2 administration or neutralization demonstrated actions of aP2 in liver. We conclude that aP2 is an adipokine linking adipocytes to hepatic glucose production and that neutralizing secreted aP2 may represent an effective therapeutic strategy against diabetes.

AB - Proper control of hepatic glucose production is central to whole-body glucose homeostasis, and its disruption plays a major role in diabetes. Here, we demonstrate that although established as an intracellular lipid chaperone, aP2 is in fact actively secreted from adipocytes to control liver glucose metabolism. Secretion of aP2 from adipocytes is regulated by fasting- and lipolysis-related signals, and circulating aP2 levels are markedly elevated in mouse and human obesity. Recombinant aP2 stimulates glucose production and gluconeogenic activity in primary hepatocytes in vitro and in lean mice in vivo. In contrast, neutralization of secreted aP2 reduces glucose production and corrects the diabetic phenotype of obese mice. Hyperinsulinemic-euglycemic and pancreatic clamp studies upon aP2 administration or neutralization demonstrated actions of aP2 in liver. We conclude that aP2 is an adipokine linking adipocytes to hepatic glucose production and that neutralizing secreted aP2 may represent an effective therapeutic strategy against diabetes.

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VL - 17

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JO - Cell metabolism

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Adipocyte lipid chaperone aP2 Is a secreted adipokine regulating hepatic glucose production

Abstract

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