Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration

Jiyoon Ryu; Jason T. Hadley; Zhi Li; Feng Dong; Huan Xu; Xiaoban Xin; Ye Zhang; Cang Chen; Senlin Li; Xiaoning Guo; Jared L. Zhao; Robin J. Leach; Muhammad A. Abdul-Ghani; Ralph A. Defronzo; Amrita Kamat; Feng Liu; Lily Q. Dong

doi:10.2337/DB20-1073

Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration

Jiyoon Ryu, Jason T. Hadley, Zhi Li, Feng Dong, Huan Xu, Xiaoban Xin, Ye Zhang, Cang Chen, Senlin Li, Xiaoning Guo, Jared L. Zhao, Robin J. Leach, Muhammad A. Abdul-Ghani, Ralph A. Defronzo, Amrita Kamat, Feng Liu, Lily Q. Dong

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11 Citas (Scopus)

Resumen

Adiponectin is an adipokine that exerts insulin-sensitiz-ing and anti-inflammatory roles in insulin target tissues including liver. While the insulin-sensitizing function of adiponectin has been extensively investigated, the pre-cise mechanism by which adiponectin alleviates diet-in-duced hepatic inflammation remains elusive. Here, we report that hepatocyte-specific knockout (KO) of the adaptor protein APPL2 enhanced adiponectin sensitivity and prevented mice from developing high-fat diet–in-duced inflammation, insulin resistance, and glucose intolerance, although it caused fatty liver. The improved anti-inflammatory and insulin-sensitizing effects in the APPL2 hepatocyte–specific KO mice were largely re-versed by knocking out adiponectin. Mechanistically, hepatocyte APPL2 deficiency enhances adiponectin signaling in the liver, which blocks TNF-α–stimulated MCP-1 expression via inhibiting the mTORC1 signaling pathway, leading to reduced macrophage infiltration and thus reduced inflammation in the liver. With results taken together, our study uncovers a mechanism under-lying the anti-inflammatory role of adiponectin in the liver and reveals the hepatic APPL2–mTORC1–MCP-1 axis as a potential target for treating overnutrition-induced inflammation in the liver.

Idioma original	English (US)
Páginas (desde-hasta)	1303-1316
Número de páginas	14
Publicación	Diabetes
Volumen	70
N.º	6
DOI	https://doi.org/10.2337/DB20-1073
Estado	Published - jun 2021

ASJC Scopus subject areas

Internal Medicine
Endocrinology, Diabetes and Metabolism

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10.2337/DB20-1073

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Ryu, J., Hadley, J. T., Li, Z., Dong, F., Xu, H., Xin, X., Zhang, Y., Chen, C., Li, S., Guo, X., Zhao, J. L., Leach, R. J., Abdul-Ghani, M. A., Defronzo, R. A., Kamat, A., Liu, F., & Dong, L. Q. (2021). Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration. Diabetes, 70(6), 1303-1316. https://doi.org/10.2337/DB20-1073

Ryu, J, Hadley, JT, Li, Z, Dong, F, Xu, H, Xin, X, Zhang, Y, Chen, C, Li, S, Guo, X, Zhao, JL, Leach, RJ , Abdul-Ghani, MA , Defronzo, RA , Kamat, A, Liu, F & Dong, LQ 2021, 'Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration', Diabetes, vol. 70, n.º 6, pp. 1303-1316. https://doi.org/10.2337/DB20-1073

@article{77935d74656341719740c9549a88f635,

title = "Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration",

abstract = "Adiponectin is an adipokine that exerts insulin-sensitiz-ing and anti-inflammatory roles in insulin target tissues including liver. While the insulin-sensitizing function of adiponectin has been extensively investigated, the pre-cise mechanism by which adiponectin alleviates diet-in-duced hepatic inflammation remains elusive. Here, we report that hepatocyte-specific knockout (KO) of the adaptor protein APPL2 enhanced adiponectin sensitivity and prevented mice from developing high-fat diet–in-duced inflammation, insulin resistance, and glucose intolerance, although it caused fatty liver. The improved anti-inflammatory and insulin-sensitizing effects in the APPL2 hepatocyte–specific KO mice were largely re-versed by knocking out adiponectin. Mechanistically, hepatocyte APPL2 deficiency enhances adiponectin signaling in the liver, which blocks TNF-α–stimulated MCP-1 expression via inhibiting the mTORC1 signaling pathway, leading to reduced macrophage infiltration and thus reduced inflammation in the liver. With results taken together, our study uncovers a mechanism under-lying the anti-inflammatory role of adiponectin in the liver and reveals the hepatic APPL2–mTORC1–MCP-1 axis as a potential target for treating overnutrition-induced inflammation in the liver.",

author = "Jiyoon Ryu and Hadley, {Jason T.} and Zhi Li and Feng Dong and Huan Xu and Xiaoban Xin and Ye Zhang and Cang Chen and Senlin Li and Xiaoning Guo and Zhao, {Jared L.} and Leach, {Robin J.} and Abdul-Ghani, {Muhammad A.} and Defronzo, {Ralph A.} and Amrita Kamat and Feng Liu and Dong, {Lily Q.}",

note = "Funding Information: Acknowledgments. The authors are thankful for technical support by University of Texas Health Science Center at San Antonio (UTHSCSA) Biobank-ing and Genome Analysis Core. Funding. This work was supported in part by American Diabetes Association Basic Science Award (grant 7-13-BS-043 to L.Q.D.), National Institutes of Health R01 grants (DK102965 to L.Q.D. and DK114479 to F.L.), DOM Clinical and Innovative Therapeutic Award Pilot Program (grant G1100-22100 to J.R.), a Biomedical Research grant from the Semp Russ Foundation of the San Antonio Area Foundation (grant 161926 to J.R.), and T32 Biology of Aging and Age-Related Diseases Training Grant (T32-AG021890-17 to J.T.H.). Duality of Interest. No potential conflicts of interest relevant to this article were reported. Author Contributions. L.Q.D. supervised the project, contributed to discussion, and reviewed and edited the manuscript. F.L. contributed to discussion and reviewed and edited the manuscript. J.R. performed experiments, conducted data analysis, and wrote the manuscript. J.T.H. performed experiments and edited the manuscript. Z.L., F.D., H.X., X.X., Y.Z., C.C., X.G., and J.L.Z. performed experiments. S.L., R.J.L., M.A.A.-G., A.K., and R.A.D. contributed to discussion. L.Q.D. is the guarantor of this work and, as such, had full access to all the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis. Prior Presentation. Parts of this study were presented in abstract form at the 78th Scientific Sessions of the American Diabetes Association, Orlando, FL, 22–26 June 2018. Publisher Copyright: {\textcopyright} 2021, American Diabetes Association Inc.. All rights reserved.",

year = "2021",

month = jun,

doi = "10.2337/DB20-1073",

language = "English (US)",

volume = "70",

pages = "1303--1316",

journal = "Diabetes",

issn = "0012-1797",

publisher = "American Diabetes Association Inc.",

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TY - JOUR

T1 - Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration

AU - Ryu, Jiyoon

AU - Hadley, Jason T.

AU - Li, Zhi

AU - Dong, Feng

AU - Xu, Huan

AU - Xin, Xiaoban

AU - Zhang, Ye

AU - Chen, Cang

AU - Li, Senlin

AU - Guo, Xiaoning

AU - Zhao, Jared L.

AU - Leach, Robin J.

AU - Abdul-Ghani, Muhammad A.

AU - Defronzo, Ralph A.

AU - Kamat, Amrita

AU - Liu, Feng

AU - Dong, Lily Q.

N1 - Funding Information: Acknowledgments. The authors are thankful for technical support by University of Texas Health Science Center at San Antonio (UTHSCSA) Biobank-ing and Genome Analysis Core. Funding. This work was supported in part by American Diabetes Association Basic Science Award (grant 7-13-BS-043 to L.Q.D.), National Institutes of Health R01 grants (DK102965 to L.Q.D. and DK114479 to F.L.), DOM Clinical and Innovative Therapeutic Award Pilot Program (grant G1100-22100 to J.R.), a Biomedical Research grant from the Semp Russ Foundation of the San Antonio Area Foundation (grant 161926 to J.R.), and T32 Biology of Aging and Age-Related Diseases Training Grant (T32-AG021890-17 to J.T.H.). Duality of Interest. No potential conflicts of interest relevant to this article were reported. Author Contributions. L.Q.D. supervised the project, contributed to discussion, and reviewed and edited the manuscript. F.L. contributed to discussion and reviewed and edited the manuscript. J.R. performed experiments, conducted data analysis, and wrote the manuscript. J.T.H. performed experiments and edited the manuscript. Z.L., F.D., H.X., X.X., Y.Z., C.C., X.G., and J.L.Z. performed experiments. S.L., R.J.L., M.A.A.-G., A.K., and R.A.D. contributed to discussion. L.Q.D. is the guarantor of this work and, as such, had full access to all the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis. Prior Presentation. Parts of this study were presented in abstract form at the 78th Scientific Sessions of the American Diabetes Association, Orlando, FL, 22–26 June 2018. Publisher Copyright: © 2021, American Diabetes Association Inc.. All rights reserved.

PY - 2021/6

Y1 - 2021/6

N2 - Adiponectin is an adipokine that exerts insulin-sensitiz-ing and anti-inflammatory roles in insulin target tissues including liver. While the insulin-sensitizing function of adiponectin has been extensively investigated, the pre-cise mechanism by which adiponectin alleviates diet-in-duced hepatic inflammation remains elusive. Here, we report that hepatocyte-specific knockout (KO) of the adaptor protein APPL2 enhanced adiponectin sensitivity and prevented mice from developing high-fat diet–in-duced inflammation, insulin resistance, and glucose intolerance, although it caused fatty liver. The improved anti-inflammatory and insulin-sensitizing effects in the APPL2 hepatocyte–specific KO mice were largely re-versed by knocking out adiponectin. Mechanistically, hepatocyte APPL2 deficiency enhances adiponectin signaling in the liver, which blocks TNF-α–stimulated MCP-1 expression via inhibiting the mTORC1 signaling pathway, leading to reduced macrophage infiltration and thus reduced inflammation in the liver. With results taken together, our study uncovers a mechanism under-lying the anti-inflammatory role of adiponectin in the liver and reveals the hepatic APPL2–mTORC1–MCP-1 axis as a potential target for treating overnutrition-induced inflammation in the liver.

AB - Adiponectin is an adipokine that exerts insulin-sensitiz-ing and anti-inflammatory roles in insulin target tissues including liver. While the insulin-sensitizing function of adiponectin has been extensively investigated, the pre-cise mechanism by which adiponectin alleviates diet-in-duced hepatic inflammation remains elusive. Here, we report that hepatocyte-specific knockout (KO) of the adaptor protein APPL2 enhanced adiponectin sensitivity and prevented mice from developing high-fat diet–in-duced inflammation, insulin resistance, and glucose intolerance, although it caused fatty liver. The improved anti-inflammatory and insulin-sensitizing effects in the APPL2 hepatocyte–specific KO mice were largely re-versed by knocking out adiponectin. Mechanistically, hepatocyte APPL2 deficiency enhances adiponectin signaling in the liver, which blocks TNF-α–stimulated MCP-1 expression via inhibiting the mTORC1 signaling pathway, leading to reduced macrophage infiltration and thus reduced inflammation in the liver. With results taken together, our study uncovers a mechanism under-lying the anti-inflammatory role of adiponectin in the liver and reveals the hepatic APPL2–mTORC1–MCP-1 axis as a potential target for treating overnutrition-induced inflammation in the liver.

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Adiponectin Alleviates Diet-Induced Inflammation in the Liver by Suppressing MCP-1 Expression and Macrophage Infiltration

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