Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis

William L. Holland; Jonathan Y. Xia; Joshua A. Johnson; Kai Sun; Mackenzie J. Pearson; Ankit X. Sharma; Ezekiel Quittner-Strom; Trevor S. Tippetts; Ruth Gordillo; Philipp E. Scherer

doi:10.1016/j.molmet.2017.01.002

Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis

William L. Holland, Jonathan Y. Xia, Joshua A. Johnson, Kai Sun, Mackenzie J. Pearson, Ankit X. Sharma, Ezekiel Quittner-Strom, Trevor S. Tippetts, Ruth Gordillo, Philipp E. Scherer

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

119 Scopus citations

Abstract

Objective Adiponectin and the signaling induced by its cognate receptors, AdipoR1 and AdipoR2, have garnered attention for their ability to promote insulin sensitivity and oppose steatosis. Activation of these receptors promotes the deacylation of ceramide, a lipid metabolite that appears to play a causal role in impairing insulin signaling. Methods Here, we have developed transgenic mice that overexpress AdipoR1 or AdipoR2 under the inducible control of a tetracycline response element. These represent the first inducible genetic models that acutely manipulate adiponectin receptor signaling in adult mouse tissues, which allows us to directly assess AdipoR signaling on glucose and lipid metabolism. Results Overexpression of either adiponectin receptor isoform in the adipocyte or hepatocyte is sufficient to enhance ceramidase activity, whole body glucose metabolism, and hepatic insulin sensitivity, while opposing hepatic steatosis. Importantly, metabolic improvements fail to occur in an adiponectin knockout background. When challenged with a leptin-deficient genetic model of type 2 diabetes, AdipoR2 expression in adipose or liver is sufficient to reverse hyperglycemia and glucose intolerance. Conclusion These observations reveal that adiponectin is critical for AdipoR-induced ceramidase activation which enhances hepatic glucose and lipid metabolism via rapidly acting “cross-talk” between liver and adipose tissue sphingolipids.

Original language	English (US)
Pages (from-to)	267-275
Number of pages	9
Journal	Molecular Metabolism
Volume	6
Issue number	3
DOIs	https://doi.org/10.1016/j.molmet.2017.01.002
State	Published - Mar 1 2017

Keywords

Insulin resistance
NAFLD
Sphingolipid

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1016/j.molmet.2017.01.002

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Holland, W. L., Xia, J. Y., Johnson, J. A., Sun, K., Pearson, M. J., Sharma, A. X., Quittner-Strom, E., Tippetts, T. S., Gordillo, R., & Scherer, P. E. (2017). Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis. Molecular Metabolism, 6(3), 267-275. https://doi.org/10.1016/j.molmet.2017.01.002

Holland, WL, Xia, JY, Johnson, JA, Sun, K, Pearson, MJ, Sharma, AX, Quittner-Strom, E, Tippetts, TS, Gordillo, R & Scherer, PE 2017, 'Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis', Molecular Metabolism, vol. 6, no. 3, pp. 267-275. https://doi.org/10.1016/j.molmet.2017.01.002

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title = "Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis",

abstract = "Objective Adiponectin and the signaling induced by its cognate receptors, AdipoR1 and AdipoR2, have garnered attention for their ability to promote insulin sensitivity and oppose steatosis. Activation of these receptors promotes the deacylation of ceramide, a lipid metabolite that appears to play a causal role in impairing insulin signaling. Methods Here, we have developed transgenic mice that overexpress AdipoR1 or AdipoR2 under the inducible control of a tetracycline response element. These represent the first inducible genetic models that acutely manipulate adiponectin receptor signaling in adult mouse tissues, which allows us to directly assess AdipoR signaling on glucose and lipid metabolism. Results Overexpression of either adiponectin receptor isoform in the adipocyte or hepatocyte is sufficient to enhance ceramidase activity, whole body glucose metabolism, and hepatic insulin sensitivity, while opposing hepatic steatosis. Importantly, metabolic improvements fail to occur in an adiponectin knockout background. When challenged with a leptin-deficient genetic model of type 2 diabetes, AdipoR2 expression in adipose or liver is sufficient to reverse hyperglycemia and glucose intolerance. Conclusion These observations reveal that adiponectin is critical for AdipoR-induced ceramidase activation which enhances hepatic glucose and lipid metabolism via rapidly acting “cross-talk” between liver and adipose tissue sphingolipids.",

keywords = "Insulin resistance, NAFLD, Sphingolipid",

author = "Holland, {William L.} and Xia, {Jonathan Y.} and Johnson, {Joshua A.} and Kai Sun and Pearson, {Mackenzie J.} and Sharma, {Ankit X.} and Ezekiel Quittner-Strom and Tippetts, {Trevor S.} and Ruth Gordillo and Scherer, {Philipp E.}",

note = "Funding Information: We thank Dr. Bob Hammer and the Transgenic Core Facility at UTSW for the generation of the transgenic lines, John Shelton and the Histology Core for assistance with histology and the UTSW Metabolic Core Unit for help in phenotyping. We acknowledge support from the National Institutes of Health (grants R01-DK55758 , R01-DK99110 and P01-DK88761 to PES). WLH is supported by a R00-DK094973 and JDRF Award 5-CDA-2014-185-A-N. JYX is supported by a NIH fellowship F30-DK100095 . JAJ is supported by NIH fellowship F30-DK108534 . MJP is supported by a fellowship from the NW NARCH and NIH T32-GM008203 . Funding Information: We thank Dr. Bob Hammer and the Transgenic Core Facility at UTSW for the generation of the transgenic lines, John Shelton and the Histology Core for assistance with histology and the UTSW Metabolic Core Unit for help in phenotyping. We acknowledge support from the National Institutes of Health (grants R01-DK55758, R01-DK99110 and P01-DK88761 to PES). WLH is supported by a R00-DK094973 and JDRF Award 5-CDA-2014-185-A-N. JYX is supported by a NIH fellowship F30-DK100095. JAJ is supported by NIH fellowship F30-DK108534. MJP is supported by a fellowship from the NW NARCH and NIH T32-GM008203. Publisher Copyright: {\textcopyright} 2017",

year = "2017",

month = mar,

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doi = "10.1016/j.molmet.2017.01.002",

language = "English (US)",

volume = "6",

pages = "267--275",

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T1 - Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis

AU - Holland, William L.

AU - Xia, Jonathan Y.

AU - Johnson, Joshua A.

AU - Sun, Kai

AU - Pearson, Mackenzie J.

AU - Sharma, Ankit X.

AU - Quittner-Strom, Ezekiel

AU - Tippetts, Trevor S.

AU - Gordillo, Ruth

AU - Scherer, Philipp E.

N1 - Funding Information: We thank Dr. Bob Hammer and the Transgenic Core Facility at UTSW for the generation of the transgenic lines, John Shelton and the Histology Core for assistance with histology and the UTSW Metabolic Core Unit for help in phenotyping. We acknowledge support from the National Institutes of Health (grants R01-DK55758 , R01-DK99110 and P01-DK88761 to PES). WLH is supported by a R00-DK094973 and JDRF Award 5-CDA-2014-185-A-N. JYX is supported by a NIH fellowship F30-DK100095 . JAJ is supported by NIH fellowship F30-DK108534 . MJP is supported by a fellowship from the NW NARCH and NIH T32-GM008203 . Funding Information: We thank Dr. Bob Hammer and the Transgenic Core Facility at UTSW for the generation of the transgenic lines, John Shelton and the Histology Core for assistance with histology and the UTSW Metabolic Core Unit for help in phenotyping. We acknowledge support from the National Institutes of Health (grants R01-DK55758, R01-DK99110 and P01-DK88761 to PES). WLH is supported by a R00-DK094973 and JDRF Award 5-CDA-2014-185-A-N. JYX is supported by a NIH fellowship F30-DK100095. JAJ is supported by NIH fellowship F30-DK108534. MJP is supported by a fellowship from the NW NARCH and NIH T32-GM008203. Publisher Copyright: © 2017

PY - 2017/3/1

Y1 - 2017/3/1

N2 - Objective Adiponectin and the signaling induced by its cognate receptors, AdipoR1 and AdipoR2, have garnered attention for their ability to promote insulin sensitivity and oppose steatosis. Activation of these receptors promotes the deacylation of ceramide, a lipid metabolite that appears to play a causal role in impairing insulin signaling. Methods Here, we have developed transgenic mice that overexpress AdipoR1 or AdipoR2 under the inducible control of a tetracycline response element. These represent the first inducible genetic models that acutely manipulate adiponectin receptor signaling in adult mouse tissues, which allows us to directly assess AdipoR signaling on glucose and lipid metabolism. Results Overexpression of either adiponectin receptor isoform in the adipocyte or hepatocyte is sufficient to enhance ceramidase activity, whole body glucose metabolism, and hepatic insulin sensitivity, while opposing hepatic steatosis. Importantly, metabolic improvements fail to occur in an adiponectin knockout background. When challenged with a leptin-deficient genetic model of type 2 diabetes, AdipoR2 expression in adipose or liver is sufficient to reverse hyperglycemia and glucose intolerance. Conclusion These observations reveal that adiponectin is critical for AdipoR-induced ceramidase activation which enhances hepatic glucose and lipid metabolism via rapidly acting “cross-talk” between liver and adipose tissue sphingolipids.

AB - Objective Adiponectin and the signaling induced by its cognate receptors, AdipoR1 and AdipoR2, have garnered attention for their ability to promote insulin sensitivity and oppose steatosis. Activation of these receptors promotes the deacylation of ceramide, a lipid metabolite that appears to play a causal role in impairing insulin signaling. Methods Here, we have developed transgenic mice that overexpress AdipoR1 or AdipoR2 under the inducible control of a tetracycline response element. These represent the first inducible genetic models that acutely manipulate adiponectin receptor signaling in adult mouse tissues, which allows us to directly assess AdipoR signaling on glucose and lipid metabolism. Results Overexpression of either adiponectin receptor isoform in the adipocyte or hepatocyte is sufficient to enhance ceramidase activity, whole body glucose metabolism, and hepatic insulin sensitivity, while opposing hepatic steatosis. Importantly, metabolic improvements fail to occur in an adiponectin knockout background. When challenged with a leptin-deficient genetic model of type 2 diabetes, AdipoR2 expression in adipose or liver is sufficient to reverse hyperglycemia and glucose intolerance. Conclusion These observations reveal that adiponectin is critical for AdipoR-induced ceramidase activation which enhances hepatic glucose and lipid metabolism via rapidly acting “cross-talk” between liver and adipose tissue sphingolipids.

KW - Insulin resistance

KW - NAFLD

KW - Sphingolipid

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ER -

Inducible overexpression of adiponectin receptors highlight the roles of adiponectin-induced ceramidase signaling in lipid and glucose homeostasis

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