Your search keyword '"Bandyopadhyay, Gautam"' showing total 19 results

1. Adipose tissue macrophages secrete small extracellular vesicles that mediate rosiglitazone-induced insulin sensitization.

Author

Rohm TV, Castellani Gomes Dos Reis F, Isaac R, Murphy C, Cunha E Rocha K, Bandyopadhyay G, Gao H, Libster AM, Zapata RC, Lee YS, Ying W, Miciano C, Wang A, and Olefsky JM

Subjects

Animals, Mice, Male, Humans, MicroRNAs genetics, MicroRNAs metabolism, Obesity metabolism, Insulin metabolism, Adipocytes metabolism, Adipocytes drug effects, Mice, Inbred C57BL, Rosiglitazone pharmacology, Extracellular Vesicles metabolism, Extracellular Vesicles drug effects, Insulin Resistance, Macrophages metabolism, Macrophages drug effects, Adipose Tissue metabolism, Adipose Tissue drug effects

Abstract

The obesity epidemic continues to worsen worldwide, driving metabolic and chronic inflammatory diseases. Thiazolidinediones, such as rosiglitazone (Rosi), are PPARγ agonists that promote 'M2-like' adipose tissue macrophage (ATM) polarization and cause insulin sensitization. As ATM-derived small extracellular vesicles (ATM-sEVs) from lean mice are known to increase insulin sensitivity, we assessed the metabolic effects of ATM-sEVs from Rosi-treated obese male mice (Rosi-ATM-sEVs). Here we show that Rosi leads to improved glucose and insulin tolerance, transcriptional repolarization of ATMs and increased sEV secretion. Administration of Rosi-ATM-sEVs rescues obesity-induced glucose intolerance and insulin sensitivity in vivo without the known thiazolidinedione-induced adverse effects of weight gain or haemodilution. Rosi-ATM-sEVs directly increase insulin sensitivity in adipocytes, myotubes and primary mouse and human hepatocytes. Additionally, we demonstrate that the miRNAs within Rosi-ATM-sEVs, primarily miR-690, are responsible for these beneficial metabolic effects. Thus, using ATM-sEVs with specific miRNAs may provide a therapeutic path to induce insulin sensitization., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

2. Immunosuppression of Macrophages Underlies the Cardioprotective Effects of CST (Catestatin).

Author

Ying W, Tang K, Avolio E, Schilling JM, Pasqua T, Liu MA, Cheng H, Gao H, Zhang J, Mahata S, Ko MS, Bandyopadhyay G, Das S, Roth DM, Sahoo D, Webster NJG, Sheikh F, Ghosh G, Patel HH, Ghosh P, van den Bogaart G, and Mahata SK

Subjects

Animals, Cardiotonic Agents therapeutic use, Chromogranin A metabolism, Chromogranin A pharmacology, Chromogranin A therapeutic use, Hypertension metabolism, Hypertension pathology, Hypertrophy, Left Ventricular metabolism, Hypertrophy, Left Ventricular pathology, Immunosuppression Therapy, Macrophages metabolism, Macrophages pathology, Male, Mice, Mice, Knockout, Peptide Fragments therapeutic use, Cardiotonic Agents pharmacology, Chromogranin A genetics, Hypertension drug therapy, Hypertrophy, Left Ventricular genetics, Macrophages drug effects, Peptide Fragments pharmacology

Abstract

[Figure: see text].

Published

2021

3. MiR-690, an exosomal-derived miRNA from M2-polarized macrophages, improves insulin sensitivity in obese mice.

Author

Ying W, Gao H, Dos Reis FCG, Bandyopadhyay G, Ofrecio JM, Luo Z, Ji Y, Jin Z, Ly C, and Olefsky JM

Subjects

Adipocytes cytology, Adipocytes metabolism, Animals, Antagomirs metabolism, DEAD-box RNA Helicases deficiency, DEAD-box RNA Helicases genetics, Diet, High-Fat, Hepatocytes cytology, Hepatocytes metabolism, Insulin metabolism, Insulin Resistance, Macrophages cytology, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Obese, MicroRNAs antagonists & inhibitors, MicroRNAs genetics, Muscle Fibers, Skeletal cytology, Muscle Fibers, Skeletal metabolism, Obesity metabolism, Obesity pathology, Phosphotransferases (Alcohol Group Acceptor) antagonists & inhibitors, Phosphotransferases (Alcohol Group Acceptor) genetics, Phosphotransferases (Alcohol Group Acceptor) metabolism, RNA Interference, RNA, Small Interfering metabolism, Ribonuclease III deficiency, Ribonuclease III genetics, Exosomes metabolism, Macrophages metabolism, MicroRNAs metabolism

Abstract

Insulin resistance is a major pathophysiologic defect in type 2 diabetes and obesity, while anti-inflammatory M2-like macrophages are important in maintaining normal metabolic homeostasis. Here, we show that M2 polarized bone marrow-derived macrophages (BMDMs) secrete miRNA-containing exosomes (Exos), which improve glucose tolerance and insulin sensitivity when given to obese mice. Depletion of their miRNA cargo blocks the ability of M2 BMDM Exos to enhance insulin sensitivity. We found that miR-690 is highly expressed in M2 BMDM Exos and functions as an insulin sensitizer both in vivo and in vitro. Expressing an miR-690 mimic in miRNA-depleted BMDMs generates Exos that recapitulate the effects of M2 BMDM Exos on metabolic phenotypes. Nadk is a bona fide target mRNA of miR-690, and Nadk plays a role in modulating macrophage inflammation and insulin signaling. Taken together, these data suggest miR-690 could be a new therapeutic insulin-sensitizing agent for metabolic disease., Competing Interests: Declaration of interests W.Y. and J.M. Olefsky are co-inventors on a provisional patent covering the use of miR-690 as an insulin sensitizer. Outside of this there are no competing interests for any of the authors., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

4. Catestatin Inhibits Obesity-Induced Macrophage Infiltration and Inflammation in the Liver and Suppresses Hepatic Glucose Production, Leading to Improved Insulin Sensitivity.

Author

Ying W, Mahata S, Bandyopadhyay GK, Zhou Z, Wollam J, Vu J, Mayoral R, Chi NW, Webster NJG, Corti A, and Mahata SK

Subjects

Animals, Chromogranin A genetics, Gene Expression Regulation drug effects, Gene Expression Regulation immunology, Glucagon pharmacology, Gluconeogenesis drug effects, Gluconeogenesis genetics, Hormones pharmacology, Inflammation immunology, Insulin metabolism, Kupffer Cells immunology, Lipid Metabolism drug effects, Liver immunology, Liver metabolism, Macrophages immunology, Male, Mice, Mice, Knockout, Obesity immunology, Peptide Fragments genetics, Chromogranin A pharmacology, Glucose metabolism, Insulin Resistance, Kupffer Cells drug effects, Liver drug effects, Macrophages drug effects, Obesity metabolism, Peptide Fragments pharmacology

Abstract

The activation of Kupffer cells (KCs) and monocyte-derived recruited macrophages (McMΦs) in the liver contributes to obesity-induced insulin resistance and type 2 diabetes. Mice with diet-induced obesity (DIO mice) treated with chromogranin A peptide catestatin (CST) showed several positive results. These included decreased hepatic/plasma lipids and plasma insulin, diminished expression of gluconeogenic genes, attenuated expression of proinflammatory genes, increased expression of anti-inflammatory genes in McMΦs, and inhibition of the infiltration of McMΦs resulting in improvement of insulin sensitivity. Systemic CST knockout (CST-KO) mice on normal chow diet (NCD) ate more food, gained weight, and displayed elevated blood glucose and insulin levels. Supplementation of CST normalized glucose and insulin levels. To verify that the CST deficiency caused macrophages to be very proinflammatory in CST-KO NCD mice and produced glucose intolerance, we tested the effects of (sorted with FACS) F4/80 + Ly6C - cells (representing KCs) and F4/80 - Ly6C + cells (representing McMΦs) on hepatic glucose production (HGP). Both basal HGP and glucagon-induced HGP were markedly increased in hepatocytes cocultured with KCs and McMΦs from NCD-fed CST-KO mice, and the effect was abrogated upon pretreatment of CST-KO macrophages with CST. Thus, we provide a novel mechanism of HGP suppression through CST-mediated inhibition of macrophage infiltration and function., (© 2018 by the American Diabetes Association.)

Published

2018

5. Adipose Tissue Macrophage-Derived Exosomal miRNAs Can Modulate In Vivo and In Vitro Insulin Sensitivity.

Author

Ying W, Riopel M, Bandyopadhyay G, Dong Y, Birmingham A, Seo JB, Ofrecio JM, Wollam J, Hernandez-Carretero A, Fu W, Li P, and Olefsky JM

Subjects

Adipocytes metabolism, Animals, Cells, Cultured, Glucose metabolism, Hepatocytes metabolism, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Muscle Cells metabolism, Muscle, Skeletal metabolism, Signal Transduction, Adipose Tissue cytology, Insulin Resistance, Macrophages metabolism, MicroRNAs metabolism

Abstract

MiRNAs are regulatory molecules that can be packaged into exosomes and secreted from cells. Here, we show that adipose tissue macrophages (ATMs) in obese mice secrete miRNA-containing exosomes (Exos), which cause glucose intolerance and insulin resistance when administered to lean mice. Conversely, ATM Exos obtained from lean mice improve glucose tolerance and insulin sensitivity when administered to obese recipients. miR-155 is one of the miRNAs overexpressed in obese ATM Exos, and earlier studies have shown that PPARγ is a miR-155 target. Our results show that miR-155KO animals are insulin sensitive and glucose tolerant compared to controls. Furthermore, transplantation of WT bone marrow into miR-155KO mice mitigated this phenotype. Taken together, these studies show that ATMs secrete exosomes containing miRNA cargo. These miRNAs can be transferred to insulin target cell types through mechanisms of paracrine or endocrine regulation with robust effects on cellular insulin action, in vivo insulin sensitivity, and overall glucose homeostasis., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

6. Characterization of distinct subpopulations of hepatic macrophages in HFD/obese mice.

Author

Morinaga H, Mayoral R, Heinrichsdorff J, Osborn O, Franck N, Hah N, Walenta E, Bandyopadhyay G, Pessentheiner AR, Chi TJ, Chung H, Bogner-Strauss JG, Evans RM, Olefsky JM, and Oh DY

Subjects

Animals, Diet, High-Fat adverse effects, Fatty Liver metabolism, Fatty Liver pathology, Interleukin-6 metabolism, Kupffer Cells metabolism, Kupffer Cells pathology, Liver pathology, Macrophages pathology, Male, Mice, Mice, Obese, Obesity etiology, Obesity pathology, Receptors, CCR2 metabolism, Tumor Necrosis Factor-alpha metabolism, Gluconeogenesis physiology, Liver metabolism, Macrophages metabolism, Obesity metabolism

Abstract

The current dogma is that obesity-associated hepatic inflammation is due to increased Kupffer cell (KC) activation. However, recruited hepatic macrophages (RHMs) were recently shown to represent a sizable liver macrophage population in the context of obesity. Therefore, we assessed whether KCs and RHMs, or both, represent the major liver inflammatory cell type in obesity. We used a combination of in vivo macrophage tracking methodologies and adoptive transfer techniques in which KCs and RHMs are differentially labeled with fluorescent markers. With these approaches, the inflammatory phenotype of these distinct macrophage populations was determined under lean and obese conditions. In vivo macrophage tracking revealed an approximately sixfold higher number of RHMs in obese mice than in lean mice, whereas the number of KCs was comparable. In addition, RHMs comprised smaller size and immature, monocyte-derived cells compared with KCs. Furthermore, RHMs from obese mice were more inflamed and expressed higher levels of tumor necrosis factor-α and interleukin-6 than RHMs from lean mice. A comparison of the MCP-1/C-C chemokine receptor type 2 (CCR2) chemokine system between the two cell types showed that the ligand (MCP-1) is more highly expressed in KCs than in RHMs, whereas CCR2 expression is approximately fivefold greater in RHMs. We conclude that KCs can participate in obesity-induced inflammation by causing the recruitment of RHMs, which are distinct from KCs and are not precursors to KCs. These RHMs then enhance the severity of obesity-induced inflammation and hepatic insulin resistance., (© 2015 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.)

Published

2015

7. LTB4 promotes insulin resistance in obese mice by acting on macrophages, hepatocytes and myocytes.

Author

Li P, Oh DY, Bandyopadhyay G, Lagakos WS, Talukdar S, Osborn O, Johnson A, Chung H, Maris M, Ofrecio JM, Taguchi S, Lu M, and Olefsky JM

Subjects

Animals, Blood Glucose metabolism, Diet, High-Fat, Fatty Liver immunology, Fatty Liver metabolism, Hepatocytes metabolism, Inflammation immunology, Insulin metabolism, Insulin Receptor Substrate Proteins metabolism, Mice, Mice, Obese, Muscle Fibers, Skeletal metabolism, Obesity metabolism, Phosphorylation, Proto-Oncogene Proteins c-akt metabolism, Receptors, Leukotriene B4 antagonists & inhibitors, Receptors, Leukotriene B4 genetics, Signal Transduction, Hepatocytes immunology, Insulin Resistance immunology, Leukotriene B4 immunology, Macrophages immunology, Muscle Fibers, Skeletal immunology, Obesity immunology, Receptors, Leukotriene B4 immunology

Abstract

Insulin resistance results from several pathophysiologic mechanisms, including chronic tissue inflammation and defective insulin signaling. We found that liver, muscle and adipose tissue exhibit higher levels of the chemotactic eicosanoid LTB4 in obese high-fat diet (HFD)-fed mice. Inhibition of the LTB4 receptor Ltb4r1, through either genetic or pharmacologic loss of function, led to an anti-inflammatory phenotype with protection from insulin resistance and hepatic steatosis. In vitro treatment with LTB4 directly enhanced macrophage chemotaxis, stimulated inflammatory pathways, reduced insulin-stimulated glucose uptake in L6 myocytes, and impaired insulin-mediated suppression of hepatic glucose output in primary mouse hepatocytes. This was accompanied by lower insulin-stimulated Akt phosphorylation and higher Irs-1/2 serine phosphorylation, and all of these events were dependent on Gαi and Jnk1, two downstream mediators of Ltb4r1 signaling. These observations elucidate a novel role of the LTB4-Ltb4r1 signaling pathway in hepatocyte and myocyte insulin resistance, and they show that in vivo inhibition of Ltb4r1 leads to robust insulin-sensitizing effects.

Published

2015

8. NCoR repression of LXRs restricts macrophage biosynthesis of insulin-sensitizing omega 3 fatty acids.

Author

Li P, Spann NJ, Kaikkonen MU, Lu M, Oh DY, Fox JN, Bandyopadhyay G, Talukdar S, Xu J, Lagakos WS, Patsouris D, Armando A, Quehenberger O, Dennis EA, Watkins SM, Auwerx J, Glass CK, and Olefsky JM

Subjects

Animals, Liver X Receptors, Mice, Mice, Inbred C57BL, Mice, Knockout, Nuclear Receptor Co-Repressor 1 genetics, Fatty Acids, Omega-3 metabolism, Insulin Resistance, Macrophages metabolism, Nuclear Receptor Co-Repressor 1 metabolism, Orphan Nuclear Receptors genetics

Abstract

Macrophage-mediated inflammation is a major contributor to obesity-associated insulin resistance. The corepressor NCoR interacts with inflammatory pathway genes in macrophages, suggesting that its removal would result in increased activity of inflammatory responses. Surprisingly, we find that macrophage-specific deletion of NCoR instead results in an anti-inflammatory phenotype along with robust systemic insulin sensitization in obese mice. We present evidence that derepression of LXRs contributes to this paradoxical anti-inflammatory phenotype by causing increased expression of genes that direct biosynthesis of palmitoleic acid and ω3 fatty acids. Remarkably, the increased ω3 fatty acid levels primarily inhibit NF-κB-dependent inflammatory responses by uncoupling NF-κB binding and enhancer/promoter histone acetylation from subsequent steps required for proinflammatory gene activation. This provides a mechanism for the in vivo anti-inflammatory insulin-sensitive phenotype observed in mice with macrophage-specific deletion of NCoR. Therapeutic methods to harness this mechanism could lead to a new approach to insulin-sensitizing therapies., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

9. SIRT1 inhibits inflammatory pathways in macrophages and modulates insulin sensitivity.

Author

Yoshizaki T, Schenk S, Imamura T, Babendure JL, Sonoda N, Bae EJ, Oh DY, Lu M, Milne JC, Westphal C, Bandyopadhyay G, and Olefsky JM

Subjects

Animals, Cells, Cultured, Gene Expression, Male, Mice, Rats, Rats, Zucker, Signal Transduction, Inflammation metabolism, Insulin metabolism, Insulin Resistance genetics, Macrophage Activation genetics, Macrophages metabolism, Sirtuin 1 metabolism

Abstract

Chronic inflammation is an important etiology underlying obesity-related disorders such as insulin resistance and type 2 diabetes, and recent findings indicate that the macrophage can be the initiating cell type responsible for this chronic inflammatory state. The mammalian silent information regulator 2 homolog SIRT1 modulates several physiological processes important for life span, and a potential role of SIRT1 in the regulation of insulin sensitivity has been shown. However, with respect to inflammation, the role of SIRT1 in regulating the proinflammatory pathway within macrophages is poorly understood. Here, we show that knockdown of SIRT1 in the mouse macrophage RAW264.7 cell line and in intraperitoneal macrophages broadly activates the JNK and IKK inflammatory pathways and increases LPS-stimulated TNFalpha secretion. Moreover, gene expression profiles reveal that SIRT1 knockdown leads to an increase in inflammatory gene expression. We also demonstrate that SIRT1 activators inhibit LPS-stimulated inflammatory pathways, as well as secretion of TNFalpha, in a SIRT1-dependent manner in RAW264.7 cells and in primary intraperitoneal macrophages. Treatment of Zucker fatty rats with a SIRT1 activator leads to greatly improved glucose tolerance, reduced hyperinsulinemia, and enhanced systemic insulin sensitivity during glucose clamp studies. These in vivo insulin-sensitizing effects were accompanied by a reduction in tissue inflammation markers and a decrease in the adipose tissue macrophage proinflammatory state, fully consistent with the in vitro effects of SIRT1 in macrophages. In conclusion, these results define a novel role for SIRT1 as an important regulator of macrophage inflammatory responses in the context of insulin resistance and raise the possibility that targeting of SIRT1 might be a useful strategy for treating the inflammatory component of metabolic diseases.

Published

2010

10. Hepatocyte-derived exosomes from early onset obese mice promote insulin sensitivity through miR-3075

Author

Ji, Yudong, Luo, Zhenlong, Gao, Hong, Dos Reis, Felipe Castellani Gomes, Bandyopadhyay, Gautam, Jin, Zhongmou, Manda, Kameswari Ananthakrishnan, Isaac, Roi, Yang, Meixiang, Fu, Wenxian, Ying, Wei, and Olefsky, Jerrold M

Subjects

Medical Biochemistry and Metabolomics, Medical Physiology, Biomedical and Clinical Sciences, Nutrition and Dietetics, Nutrition, Biotechnology, Obesity, Genetics, Diabetes, Aetiology, 2.1 Biological and endogenous factors, Oral and gastrointestinal, Cardiovascular, Metabolic and endocrine, Adipocytes, Animals, Diet, High-Fat, Exosomes, Hepatocytes, Insulin Resistance, Macrophages, Mice, Muscle Cells, RNA, Small Interfering, Medical biochemistry and metabolomics, Medical physiology, Nutrition and dietetics

Abstract

In chronic obesity, hepatocytes become insulin resistant and exert important effects on systemic metabolism. Here we show that in early onset obesity (4 weeks high-fat diet), hepatocytes secrete exosomes that enhance insulin sensitivity both in vitro and in vivo. These beneficial effects were due to exosomal microRNA miR-3075, which is enriched in these hepatocyte exosomes. FA2H is a direct target of miR-3075 and small interfering RNA depletion of FA2H in adipocytes, myocytes and primary hepatocytes leads to increased insulin sensitivity. In chronic obesity (16-18 weeks of a high-fat diet), hepatocyte exosomes promote a state of insulin resistance. These chronic obese hepatocyte exosomes do not directly cause impaired insulin signalling in vitro but do promote proinflammatory activation of macrophages. Taken together, these studies show that in early onset obesity, hepatocytes produce exosomes that express high levels of the insulin-sensitizing miR-3075. In chronic obesity, this compensatory effect is lost and hepatocyte-derived exosomes from chronic obese mice promote insulin resistance.

Published

2021

11. TAZ Is a Negative Regulator of PPARγ Activity in Adipocytes and TAZ Deletion Improves Insulin Sensitivity and Glucose Tolerance

Author

El Ouarrat, Dalila, Isaac, Roi, Lee, Yun Sok, Oh, Da Young, Wollam, Joshua, Lackey, Denise, Riopel, Matthew, Bandyopadhyay, Gautam, Seo, Jong Bae, Sampath-Kumar, Revathy, and Olefsky, Jerrold M

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Diabetes, Obesity, Nutrition, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Adaptor Proteins, Signal Transducing, Adipocytes, Adipogenesis, Animals, Cell Line, Diet, High-Fat, Extracellular Signal-Regulated MAP Kinases, Glucose, Glucose Tolerance Test, Humans, Immunohistochemistry, Inflammation, Insulin Resistance, Macrophages, Male, Mice, Mice, Knockout, Mice, Obese, PPAR gamma, Phosphorylation, Trans-Activators, Hippo pathway, TAZ, adipocyte, glucose tolerance, insulin sensitivity, obesity, transcriptional co-activator with PDZ-binding motif, Medical Biochemistry and Metabolomics, Endocrinology & Metabolism, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Insulin resistance is a major factor in obesity-linked type 2 diabetes. PPARγ is a master regulator of adipogenesis, and small molecule agonists, termed thiazolidinediones, are potent therapeutic insulin sensitizers. Here, we studied the role of transcriptional co-activator with PDZ-binding motif (TAZ) as a transcriptional co-repressor of PPARγ. We found that adipocyte-specific TAZ knockout (TAZ AKO) mice demonstrate a constitutively active PPARγ state. Obese TAZ AKO mice show improved glucose tolerance and insulin sensitivity compared to littermate controls. PPARγ response genes are upregulated in adipose tissue from TAZ AKO mice and adipose tissue inflammation was also decreased. In vitro and in vivo mechanistic studies revealed that the TAZ-PPARγ interaction is partially dependent on ERK-mediated Ser112 PPARγ phosphorylation. As adipocyte PPARγ Ser112 phosphorylation is increased in obesity, repression of PPARγ activity by TAZ could contribute to insulin resistance. These results identify TAZ as a new factor in the development of obesity-induced insulin resistance.

Published

2020

12. Adipose tissue B2 cells promote insulin resistance through leukotriene LTB4/LTB4R1 signaling

Author

Ying, Wei, Wollam, Joshua, Ofrecio, Jachelle M, Bandyopadhyay, Gautam, Ouarrat, Dalila El, Lee, Yun Sok, Oh, Da Young, Li, Pingping, Osborn, Olivia, and Olefsky, Jerrold M

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Obesity, Diabetes, Nutrition, 2.1 Biological and endogenous factors, Aetiology, Cancer, Metabolic and endocrine, Adipose Tissue, Animals, B-Lymphocyte Subsets, Dietary Fats, Insulin Resistance, Leukotriene B4, Macrophages, Mice, Mice, Knockout, Receptors, Leukotriene B4, Signal Transduction, T-Lymphocytes, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Tissue inflammation is a key component of obesity-induced insulin resistance, with a variety of immune cell types accumulating in adipose tissue. Here, we have demonstrated increased numbers of B2 lymphocytes in obese adipose tissue and have shown that high-fat diet-induced (HFD-induced) insulin resistance is mitigated in B cell-deficient (Bnull) mice. Adoptive transfer of adipose tissue B2 cells (ATB2) from wild-type HFD donor mice into HFD Bnull recipients completely restored the effect of HFD to induce insulin resistance. Recruitment and activation of ATB2 cells was mediated by signaling through the chemokine leukotriene B4 (LTB4) and its receptor LTB4R1. Furthermore, the adverse effects of ATB2 cells on glucose homeostasis were partially dependent upon T cells and macrophages. These results demonstrate the importance of ATB2 cells in obesity-induced insulin resistance and suggest that inhibition of the LTB4/LTB4R1 axis might be a useful approach for developing insulin-sensitizing therapeutics.

Published

2017

13. Catestatin Inhibits Obesity-Induced Macrophage Infiltration and Inflammation in the Liver and Suppresses Hepatic Glucose Production, Leading to Improved Insulin Sensitivity.

Author

Wei Ying, Mahata, Sumana, Bandyopadhyay, Gautam K., Zhenqi Zhou, Wollam, Joshua, Vu, Jessica, Mayoral, Rafael, Nai-Wen Chi, Webster, Nicholas J. G., Corti, Angelo, Mahata, Sushil K., Ying, Wei, Zhou, Zhenqi, and Chi, Nai-Wen

Subjects

MACROPHAGES, INFLAMMATION prevention, LIVER diseases, INSULIN resistance, OBESITY, KUPFFER cells, GLUCOSE metabolism, ANIMAL experimentation, COMPARATIVE studies, GENES, GENETIC disorders, GLUCAGON, HORMONES, INFLAMMATION, INSULIN, LIPID metabolism disorders, LIVER, RESEARCH methodology, MEDICAL cooperation, METABOLISM, MICE, PEPTIDES, PROTEIN precursors, RESEARCH, EVALUATION research

Abstract

The activation of Kupffer cells (KCs) and monocyte-derived recruited macrophages (McMΦs) in the liver contributes to obesity-induced insulin resistance and type 2 diabetes. Mice with diet-induced obesity (DIO mice) treated with chromogranin A peptide catestatin (CST) showed several positive results. These included decreased hepatic/plasma lipids and plasma insulin, diminished expression of gluconeogenic genes, attenuated expression of proinflammatory genes, increased expression of anti-inflammatory genes in McMΦs, and inhibition of the infiltration of McMΦs resulting in improvement of insulin sensitivity. Systemic CST knockout (CST-KO) mice on normal chow diet (NCD) ate more food, gained weight, and displayed elevated blood glucose and insulin levels. Supplementation of CST normalized glucose and insulin levels. To verify that the CST deficiency caused macrophages to be very proinflammatory in CST-KO NCD mice and produced glucose intolerance, we tested the effects of (sorted with FACS) F4/80+Ly6C- cells (representing KCs) and F4/80-Ly6C+ cells (representing McMΦs) on hepatic glucose production (HGP). Both basal HGP and glucagon-induced HGP were markedly increased in hepatocytes cocultured with KCs and McMΦs from NCD-fed CST-KO mice, and the effect was abrogated upon pretreatment of CST-KO macrophages with CST. Thus, we provide a novel mechanism of HGP suppression through CST-mediated inhibition of macrophage infiltration and function. [ABSTRACT FROM AUTHOR]

Published

2018

14. Pancreastatin-Dependent Inflammatory Signaling Mediates Obesity-Induced Insulin Resistance.

Author

Bandyopadhyay, Gautam K., Minh Lu, Avolio, Ennio, Siddiqui, Jawed A., Gayen, Jiaur R., Wollam, Joshua, Vu, Christine U., Nai-Wen Chi, O'Connor, Daniel T., and Mahata, Sushil K.

Subjects

*CHROMOGRANINS, *LABORATORY mice, *OBESITY, *MACROPHAGES, *CYTOKINES, *GENES, *BCL genes

Abstract

Chromogranin A knockout (Chga-KO) mice exhibit enhanced insulin sensitivity despite obesity. Here, we probed the role of the chromogranin A-derived peptide pancreastatin (PST: CHGA273-301) by investigating the effect of diet-induced obesity (DIO) on insulin sensitivity of these mice. We found that on a high-fat diet (HFD), Chga-KO mice (KO-DIO) remain more insulin sensitive than wild-type DIO (WT-DIO) mice. Concomitant with this phenotype is enhanced Akt and AMPK signaling in muscle and white adipose tissue (WAT) as well as increased FoxO1 phosphorylation and expression of mature Srebp-1c in liver and downregulation of the hepatic gluconeogenic genes, Pepck and G6pase. KO-DIO mice also exhibited downregulation of cytokines and proinflammatory genes and upregulation of anti-inflammatory genes in WAT, and peritoneal macrophages from KO mice displayed similarly reduced proinflammatory gene expression. The insulin-sensitive, anti-inflammatory phenotype of KO-DIO mice is masked by supplementing PST. Conversely, a PST variant peptide PSTv1 (PST-NΔ3: CHGA276-301), lacking PST activity, simulated the KO phenotype by sensitizing WT-DIO mice to insulin. In summary, the reduced inflammation due to PST deficiency prevented the development of insulin resistance in KO-DIO mice. Thus, obesity manifests insulin resistance only in the presence of PST, and in its absence obesity is dissociated from insulin resistance. [ABSTRACT FROM AUTHOR]

Published

2015

15. Neutrophils mediate insulin resistance in mice fed a high-fat diet through secreted elastase.

Author

Talukdar, Saswata, Oh, Da Young, Bandyopadhyay, Gautam, Li, Dongmei, Xu, Jianfeng, McNelis, Joanne, Lu, Min, Li, Pingping, Yan, Qingyun, Zhu, Yimin, Ofrecio, Jachelle, Lin, Michael, Brenner, Martin B, and Olefsky, Jerrold M

Subjects

NEUTROPHILS, INSULIN resistance, HIGH-fat diet, ELASTASES, ADIPOSE tissues, MACROPHAGES, EOSINOPHILS, LABORATORY mice

Abstract

Chronic low-grade adipose tissue and liver inflammation is a major cause of systemic insulin resistance and is a key component of the low degree of insulin sensitivity that exists in obesity and type 2 diabetes. Immune cells, such as macrophages, T cells, B cells, mast cells and eosinophils, have all been implicated as having a role in this process. Neutrophils are typically the first immune cells to respond to inflammation and can exacerbate the chronic inflammatory state by helping to recruit macrophages and by interacting with antigen-presenting cells. Neutrophils secrete several proteases, one of which is neutrophil elastase, which can promote inflammatory responses in several disease models. Here we show that treatment of hepatocytes with neutrophil elastase causes cellular insulin resistance and that deletion of neutrophil elastase in high-fat-diet-induced obese (DIO) mice leads to less tissue inflammation that is associated with lower adipose tissue neutrophil and macrophage content. These changes are accompanied by improved glucose tolerance and increased insulin sensitivity. Taken together, we show that neutrophils can be added to the extensive repertoire of immune cells that participate in inflammation-induced metabolic disease. [ABSTRACT FROM AUTHOR]

Published

2012

16. NCoR Repression of LXRs Restricts Macrophage Biosynthesis of Insulin-Sensitizing Omega 3 Fatty Acids

Author

Li Pingping, Spann Nathanael J., Kaikkonen Minna U., Lu Min, Oh Da Young, Fox Jesse N., Bandyopadhyay Gautam, Talukdar Saswata, Xu Jianfeng, Lagakos William S., Patsouris David, Armando Aaron, Quehenberger Oswald, Dennis Edward A., Watkins Steven M., Auwerx Johan, Glass Christopher K., and Olefsky Jerrold M.

Subjects

medicine.medical_treatment, Knockout, Biology, Inbred C57BL, Medical and Health Sciences, General Biochemistry, Genetics and Molecular Biology, Article, Proinflammatory cytokine, 03 medical and health sciences, Mice, 0302 clinical medicine, Insulin resistance, Fatty Acids, Omega-3, Complementary and Integrative Health, medicine, Genetics, Animals, Nuclear Receptor Co-Repressor 1, 2.1 Biological and endogenous factors, Obesity, Aetiology, Liver X receptor, Derepression, Metabolic and endocrine, 030304 developmental biology, Liver X Receptors, Nutrition, chemistry.chemical_classification, Regulation of gene expression, Mice, Knockout, Omega-3, 0303 health sciences, Biochemistry, Genetics and Molecular Biology(all), Insulin, Macrophages, Fatty Acids, Fatty acid, Biological Sciences, medicine.disease, Orphan Nuclear Receptors, Cell biology, Mice, Inbred C57BL, Biochemistry, chemistry, Insulin Resistance, Corepressor, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Summary Macrophage mediated inflammation is a major contributor to obesity associated insulin resistance. The corepressor NCoR interacts with inflammatory pathway genes in macrophages suggesting that its removal would result in increased activity of inflammatory responses. Surprisingly we find that macrophage specific deletion of NCoR instead results in an anti inflammatory phenotype along with robust systemic insulin sensitization in obese mice. We present evidence that derepression of LXRs contributes to this paradoxical anti inflammatory phenotype by causing increased expression of genes that direct biosynthesis of palmitoleic acid and ?3 fatty acids. Remarkably the increased ?3 fatty acid levels primarily inhibit NF ?B dependent inflammatory responses by uncoupling NF ?B binding and enhancer/promoter histone acetylation from subsequent steps required for proinflammatory gene activation. This provides a mechanism for the in vivo anti inflammatory insulin sensitive phenotype observed in mice with macrophage specific deletion of NCoR. Therapeutic methods to harness this mechanism could lead to a new approach to insulin sensitizing therapies. © 2013 Elsevier Inc.

17. Adipose tissue B2 cells promote insulin resistance through leukotriene LTB4/LTB4R1 signaling.

Author

Wei Ying, Wollam, Joshua, Ofrecio, Jachelle M., Bandyopadhyay, Gautam, Ouarrat, Dalila El, Yun Sok Lee, Da Young Oh, Pingping Li, Osborn, Olivia, Olefsky, Jerrold M., Ying, Wei, El Ouarrat, Dalila, Lee, Yun Sok, Oh, Da Young, and Li, Pingping

Subjects

*ADIPOSE tissues, *INSULIN resistance, *LEUKOTRIENES, *CELLULAR signal transduction, *CELLULAR immunity, *MACROPHAGES, *ANIMALS, *B cells, *CELL receptors, *FAT content of food, *MICE, *OBESITY, *T cells

Abstract

Tissue inflammation is a key component of obesity-induced insulin resistance, with a variety of immune cell types accumulating in adipose tissue. Here, we have demonstrated increased numbers of B2 lymphocytes in obese adipose tissue and have shown that high-fat diet-induced (HFD-induced) insulin resistance is mitigated in B cell-deficient (Bnull) mice. Adoptive transfer of adipose tissue B2 cells (ATB2) from wild-type HFD donor mice into HFD Bnull recipients completely restored the effect of HFD to induce insulin resistance. Recruitment and activation of ATB2 cells was mediated by signaling through the chemokine leukotriene B4 (LTB4) and its receptor LTB4R1. Furthermore, the adverse effects of ATB2 cells on glucose homeostasis were partially dependent upon T cells and macrophages. These results demonstrate the importance of ATB2 cells in obesity-induced insulin resistance and suggest that inhibition of the LTB4/LTB4R1 axis might be a useful approach for developing insulin-sensitizing therapeutics. [ABSTRACT FROM AUTHOR]

Published

2017

18. Catestatin as a key attenuator of cardiac inflammation in hypertension: Role of macrophage immunosuppression.

Author

Pasqua, Teresa, Ying, Wei, Tang, Kechun, Avolio, Ennio, Schilling, Jan M., Liu, Matthew A., Cheng, Hongqiang, Gao, Hong, Zhang, Jing, Mahata, Sumana, Ko, Myung S., Bandyopadhyay, Gautam, Das, Soumita, Roth, David M., Sahoo, Debashis, Webster, Nicholas J.G., Sheikh, Farah, Ghosh, Gourisankar, Patel, Hemal H., and Ghosh, Pradipta

Subjects

*IMMUNOSUPPRESSION, *HYPERTENSION, *INFLAMMATION, *MACROPHAGES

Published

2022

19. Catestatin Inhibits Obesity-Induced Macrophage Infiltration and Inflammation in the Liver and Suppresses Hepatic Glucose Production Leading to Improved Insulin Sensitivity

Author

Nai-Wen Chi, Wei Ying, Zhenqi Zhou, Nicholas J. G. Webster, Gautam Bandyopadhyay, Sumana Mahata, Joshua Wollam, Angelo Corti, Sushil K. Mahata, Rafael Mayoral, Jessica Vu, Ying, Wei, Mahata, Sumana, Bandyopadhyay, Gautam K., Zhou, Zhenqi, Wollam, Joshua, Vu, Jessica, Mayoral, Rafael, Chi, Nai-Wen, Webster, Nicholas J. G., Corti, Angelo, and Mahata, Sushil K.

Subjects

0301 basic medicine, Male, Macrophage, medicine.medical_treatment, Endocrinology, Diabetes and Metabolism, Type 2 diabetes, Cardiovascular, Medical and Health Sciences, Oral and gastrointestinal, Mice, 0302 clinical medicine, Peptide Fragment, 2.1 Biological and endogenous factors, Insulin, Aetiology, Mice, Knockout, biology, Chemistry, Liver Disease, Diabetes, Chromogranin A, medicine.anatomical_structure, Liver, 030220 oncology & carcinogenesis, Kupffer Cell, medicine.symptom, Infiltration (medical), Gluconeogenesi, medicine.medical_specialty, Kupffer Cells, Knockout, Inflammation, Carbohydrate metabolism, 03 medical and health sciences, Endocrinology & Metabolism, Insulin resistance, Internal medicine, medicine, Internal Medicine, Animals, Obesity, Metabolic and endocrine, Nutrition, Animal, Monocyte, Macrophages, Gluconeogenesis, medicine.disease, Glucagon, Lipid Metabolism, Hormone, Hormones, Peptide Fragments, 030104 developmental biology, Endocrinology, Glucose, Metabolism, Gene Expression Regulation, biology.protein, Insulin Resistance, Digestive Diseases, human activities

Abstract

The activation of Kupffer cells (KCs) and monocyte-derived recruited macrophages (McMΦs) in the liver contributes to obesity-induced insulin resistance and type 2 diabetes. Mice with diet-induced obesity (DIO mice) treated with chromogranin A peptide catestatin (CST) showed several positive results. These included decreased hepatic/plasma lipids and plasma insulin, diminished expression of gluconeogenic genes, attenuated expression of proinflammatory genes, increased expression of anti-inflammatory genes in McMΦs, and inhibition of the infiltration of McMΦs resulting in improvement of insulin sensitivity. Systemic CST knockout (CST-KO) mice on normal chow diet (NCD) ate more food, gained weight, and displayed elevated blood glucose and insulin levels. Supplementation of CST normalized glucose and insulin levels. To verify that the CST deficiency caused macrophages to be very proinflammatory in CST-KO NCD mice and produced glucose intolerance, we tested the effects of (sorted with FACS) F4/80+Ly6C− cells (representing KCs) and F4/80−Ly6C+ cells (representing McMΦs) on hepatic glucose production (HGP). Both basal HGP and glucagon-induced HGP were markedly increased in hepatocytes cocultured with KCs and McMΦs from NCD-fed CST-KO mice, and the effect was abrogated upon pretreatment of CST-KO macrophages with CST. Thus, we provide a novel mechanism of HGP suppression through CST-mediated inhibition of macrophage infiltration and function.

Published

2018