Suppressing adipocyte inflammation promotes insulin resistance in mice

Suppressing adipocyte inflammation promotes insulin resistance in mice

Objective: Obesity-induced insulin resistance is closely associated with chronic subclinical inflammation in white adipose tissue. However, the mechanistic involvement of adipocyte-derived inflammation under these disease conditions remains unclear. Our aim was to investigate the relative inflammati...

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Main Authors: Qingzhang Zhu, Yu A. An, Min Kim, Zhuzhen Zhang, Shangang Zhao, Yi Zhu, Ingrid Wernstedt Asterholm, Christine M. Kusminski, Philipp E. Scherer
Format: Article
Language:English
Published: Elsevier 2020-09-01
Series:Molecular Metabolism
Subjects:
Adipocyte
Inflammation
Insulin resistance
Online Access:http://www.sciencedirect.com/science/article/pii/S2212877820300843
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spelling doaj-d5b9d8aa59174aca9e2b2fdb196f1b152020-11-25T03:29:10ZengElsevierMolecular Metabolism2212-87782020-09-0139101010Suppressing adipocyte inflammation promotes insulin resistance in miceQingzhang Zhu0Yu A. An1Min Kim2Zhuzhen Zhang3Shangang Zhao4Yi Zhu5Ingrid Wernstedt Asterholm6Christine M. Kusminski7Philipp E. Scherer8Touchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USATouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USADepartment of Biological Sciences, School of Life Sciences, Ulsan National Institute of Science and Technology, Ulsan, South KoreaTouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USATouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USATouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USADepartment of Physiology/Metabolic Physiology, Institute of Neuroscience and Physiology, Sahlgrenska Academy at University of Gothenburg, Gothenburg, SwedenTouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USATouchstone Diabetes Center, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USA; Corresponding author.Objective: Obesity-induced insulin resistance is closely associated with chronic subclinical inflammation in white adipose tissue. However, the mechanistic involvement of adipocyte-derived inflammation under these disease conditions remains unclear. Our aim was to investigate the relative inflammation-related contributions of adipocytes and macrophages to insulin sensitivity. Methods: RIDα/β is an adenoviral protein complex that inhibits several inflammatory pathways, including TLR4, TNFα, and IL1β signaling. We generated novel mouse models with adipocyte-specific and macrophage-specific doxycycline (dox)-inducible RIDα/β-transgenic mice (RIDad and RIDmac mice, respectively). Results: RIDα/β induction significantly reduced LPS-stimulated inflammatory markers, such as Tnf, Il1b, and Saa3 in adipose tissues. Surprisingly, RIDad mice had elevated levels of postprandial glucose and insulin and exhibited glucose intolerance and insulin resistance, even under chow-fed conditions. Moreover, the RIDad mice displayed further insulin resistance under obesogenic (high-fat diet, HFD) conditions despite reduced weight gain. In addition, under pre-existing obese and inflamed conditions on an HFD, subsequent induction of RIDα/β in RIDad mice reduced body weight gain, further exacerbating glucose tolerance, enhancing insulin resistance and fatty liver, and reducing adiponectin levels. This occurred despite effective suppression of the inflammatory pathways (including TNFα and IL1β). In contrast, RIDmac mice, upon HFD feeding, displayed similar weight gain, comparable adiponectin levels, and insulin sensitivity, suggesting that the inflammatory properties of macrophages did not exert a negative impact on metabolic readouts. RIDα/β expression and the ensuing suppression of inflammation in adipocytes enhanced adipose tissue fibrosis and reduced vascularization. Conclusion: Our novel findings further corroborate our previous observations suggesting that suppressing adipocyte inflammation impairs adipose tissue function and promotes insulin resistance, despite beneficial effects on weight gain.http://www.sciencedirect.com/science/article/pii/S2212877820300843AdipocyteInflammationInsulin resistance
collection DOAJ
language English
format Article
sources DOAJ
author Qingzhang Zhu
Yu A. An
Min Kim
Zhuzhen Zhang
Shangang Zhao
Yi Zhu
Ingrid Wernstedt Asterholm
Christine M. Kusminski
Philipp E. Scherer
spellingShingle Qingzhang Zhu
Yu A. An
Min Kim
Zhuzhen Zhang
Shangang Zhao
Yi Zhu
Ingrid Wernstedt Asterholm
Christine M. Kusminski
Philipp E. Scherer
Suppressing adipocyte inflammation promotes insulin resistance in mice
Molecular Metabolism
Adipocyte
Inflammation
Insulin resistance
author_facet Qingzhang Zhu
Yu A. An
Min Kim
Zhuzhen Zhang
Shangang Zhao
Yi Zhu
Ingrid Wernstedt Asterholm
Christine M. Kusminski
Philipp E. Scherer
author_sort Qingzhang Zhu
title Suppressing adipocyte inflammation promotes insulin resistance in mice
title_short Suppressing adipocyte inflammation promotes insulin resistance in mice
title_full Suppressing adipocyte inflammation promotes insulin resistance in mice
title_fullStr Suppressing adipocyte inflammation promotes insulin resistance in mice
title_full_unstemmed Suppressing adipocyte inflammation promotes insulin resistance in mice
title_sort suppressing adipocyte inflammation promotes insulin resistance in mice
publisher Elsevier
series Molecular Metabolism
issn 2212-8778
publishDate 2020-09-01
description Objective: Obesity-induced insulin resistance is closely associated with chronic subclinical inflammation in white adipose tissue. However, the mechanistic involvement of adipocyte-derived inflammation under these disease conditions remains unclear. Our aim was to investigate the relative inflammation-related contributions of adipocytes and macrophages to insulin sensitivity. Methods: RIDα/β is an adenoviral protein complex that inhibits several inflammatory pathways, including TLR4, TNFα, and IL1β signaling. We generated novel mouse models with adipocyte-specific and macrophage-specific doxycycline (dox)-inducible RIDα/β-transgenic mice (RIDad and RIDmac mice, respectively). Results: RIDα/β induction significantly reduced LPS-stimulated inflammatory markers, such as Tnf, Il1b, and Saa3 in adipose tissues. Surprisingly, RIDad mice had elevated levels of postprandial glucose and insulin and exhibited glucose intolerance and insulin resistance, even under chow-fed conditions. Moreover, the RIDad mice displayed further insulin resistance under obesogenic (high-fat diet, HFD) conditions despite reduced weight gain. In addition, under pre-existing obese and inflamed conditions on an HFD, subsequent induction of RIDα/β in RIDad mice reduced body weight gain, further exacerbating glucose tolerance, enhancing insulin resistance and fatty liver, and reducing adiponectin levels. This occurred despite effective suppression of the inflammatory pathways (including TNFα and IL1β). In contrast, RIDmac mice, upon HFD feeding, displayed similar weight gain, comparable adiponectin levels, and insulin sensitivity, suggesting that the inflammatory properties of macrophages did not exert a negative impact on metabolic readouts. RIDα/β expression and the ensuing suppression of inflammation in adipocytes enhanced adipose tissue fibrosis and reduced vascularization. Conclusion: Our novel findings further corroborate our previous observations suggesting that suppressing adipocyte inflammation impairs adipose tissue function and promotes insulin resistance, despite beneficial effects on weight gain.
topic Adipocyte
Inflammation
Insulin resistance
url http://www.sciencedirect.com/science/article/pii/S2212877820300843
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