Your search keyword '"Shangang Zhao"' showing total 66 results

1. AAV-delivered muscone-induced transgene system for treating chronic diseases in mice via inhalation

Author

Xin Wu, Yuanhuan Yu, Meiyan Wang, Di Dai, Jianli Yin, Wenjing Liu, Deqiang Kong, Shasha Tang, Meiyao Meng, Tian Gao, Yuanjin Zhang, Yang Zhou, Ningzi Guan, Shangang Zhao, and Haifeng Ye

Subjects

Science

Abstract

Abstract Gene therapies provide treatment options for many diseases, but the safe and long-term control of therapeutic transgene expression remains a primary issue for clinical applications. Here, we develop a muscone-induced transgene system packaged into adeno-associated virus (AAV) vectors (AAVMUSE) based on a G protein-coupled murine olfactory receptor (MOR215-1) and a synthetic cAMP-responsive promoter (PCRE). Upon exposure to the trigger, muscone binds to MOR215-1 and activates the cAMP signaling pathway to initiate transgene expression. AAVMUSE enables remote, muscone dose- and exposure-time-dependent control of luciferase expression in the livers or lungs of mice for at least 20 weeks. Moreover, we apply this AAVMUSE to treat two chronic inflammatory diseases: nonalcoholic fatty liver disease (NAFLD) and allergic asthma, showing that inhalation of muscone—after only one injection of AAVMUSE—can achieve long-term controllable expression of therapeutic proteins (ΔhFGF21 or ΔmIL-4). Our odorant-molecule-controlled system can advance gene-based precision therapies for human diseases.

Published

2024

2. Qa-SNARE syntaxin 18 mediates lipid droplet fusion with SNAP23 and SEC22B

Author

Yuhui Fu, Binbin Ding, Xiaoxia Liu, Shangang Zhao, Fang Chen, Linsen Li, Yi Zhu, Jingxuan Zhao, Zhen Yuan, Yafeng Shen, Chaofeng Yang, Mengle Shao, She Chen, Perry E. Bickel, and Qing Zhong

Subjects

Cytology, QH573-671

Abstract

Abstract Lipid droplets (LDs) are dynamic lipid storage organelles that can sense and respond to changes in systemic energy balance. The size and number of LDs are controlled by complex and delicate mechanisms, among which, whether and which SNARE proteins mediate LD fusion, and the mechanisms governing this process remain poorly understood. Here we identified a SNARE complex, syntaxin 18 (STX18)–SNAP23–SEC22B, that is recruited to LDs to mediate LD fusion. STX18 targets LDs with its transmembrane domain spanning the phospholipid monolayer twice. STX18–SNAP23–SEC22B complex drives LD fusion in adiposome lipid mixing and content mixing in vitro assays. CIDEC/FSP27 directly binds STX18, SEC22B, and SNAP23, and promotes the lipid mixing of SNAREs-reconstituted adiposomes by promoting LD clustering. Knockdown of STX18 in mouse liver via AAV resulted in smaller liver and reduced LD size under high-fat diet conditions. All these results demonstrate a critical role of the SNARE complex STX18–SNAP23–SEC22B in LD fusion.

Published

2023

3. Protective roles of adiponectin and molecular signatures of HNF4α and PPARα as downstream targets of adiponectin in pancreatic β cells

Author

Toshiharu Onodera, Dae-Seok Kim, Risheng Ye, May-Yun Wang, Shiuhwei Chen, Bianca C. Field, Leon Straub, Xue-Nan Sun, Chao Li, Charlotte Lee, Megan Paredes, Clair Crewe, Shangang Zhao, Christine M. Kusminski, Ruth Gordillo, and Philipp E. Scherer

Subjects

Adiponectin, PPARα, HNF4α, β cell, Internal medicine, RC31-1245

Abstract

The disease progression of the metabolic syndrome is associated with prolonged hyperlipidemia and insulin resistance, eventually giving rise to impaired insulin secretion, often concomitant with hypoadiponectinemia. As an adipose tissue derived hormone, adiponectin is beneficial for insulin secretion and β cell health and differentiation. However, the down-stream pathway of adiponectin in the pancreatic islets has not been studied extensively. Here, along with the overall reduction of endocrine pancreatic function in islets from adiponectin KO mice, we examine PPARα and HNF4α as additional down-regulated transcription factors during a prolonged metabolic challenge. To elucidate the function of β cell-specific PPARα and HNF4α expression, we developed doxycycline inducible pancreatic β cell-specific PPARα (β-PPARα) and HNF4α (β-HNF4α) overexpression mice. β-PPARα mice exhibited improved protection from lipotoxicity, but elevated β-oxidative damage in the islets, and also displayed lowered phospholipid levels and impaired glucose-stimulated insulin secretion. β-HNF4α mice showed a more severe phenotype when compared to β-PPARα mice, characterized by lower body weight, small islet mass and impaired insulin secretion. RNA-sequencing of the islets of these models highlights overlapping yet unique roles of β-PPARα and β-HNF4α. Given that β-HNF4α potently induces PPARα expression, we define a novel adiponectin-HNF4α-PPARα cascade. We further analyzed downstream genes consistently regulated by this axis. Among them, the islet amyloid polypeptide (IAPP) gene is an important target and accumulates in adiponectin KO mice. We propose a new mechanism of IAPP aggregation in type 2 diabetes through reduced adiponectin action.

Published

2023

4. Activating Connexin43 gap junctions primes adipose tissue for therapeutic intervention

Author

Yi Zhu, Na Li, Mingyang Huang, Xi Chen, Yu A. An, Jianping Li, Shangang Zhao, Jan-Bernd Funcke, Jianhong Cao, Zhenyan He, Qingzhang Zhu, Zhuzhen Zhang, Zhao V. Wang, Lin Xu, Kevin W. Williams, Chien Li, Kevin Grove, and Philipp E. Scherer

Subjects

GJA1, Adipose tissue, Gap junction, Connexin43, FGF21, β3-Adrenergic receptor agonist, Therapeutics. Pharmacology, RM1-950

Abstract

Adipose tissue is a promising target for treating obesity and metabolic diseases. However, pharmacological agents usually fail to effectively engage adipocytes due to their extraordinarily large size and insufficient vascularization, especially in obese subjects. We have previously shown that during cold exposure, connexin43 (Cx43) gap junctions are induced and activated to connect neighboring adipocytes to share limited sympathetic neuronal input amongst multiple cells. We reason the same mechanism may be leveraged to improve the efficacy of various pharmacological agents that target adipose tissue. Using an adipose tissue-specific Cx43 overexpression mouse model, we demonstrate effectiveness in connecting adipocytes to augment metabolic efficacy of the β3-adrenergic receptor agonist Mirabegron and FGF21. Additionally, combing those molecules with the Cx43 gap junction channel activator danegaptide shows a similar enhanced efficacy. In light of these findings, we propose a model in which connecting adipocytes via Cx43 gap junction channels primes adipose tissue to pharmacological agents designed to engage it. Thus, Cx43 gap junction activators hold great potential for combination with additional agents targeting adipose tissue.

Published

2022

5. Adipose tissue hyaluronan production improves systemic glucose homeostasis and primes adipocytes for CL 316,243-stimulated lipolysis

Author

Yi Zhu, Na Li, Mingyang Huang, Mason Bartels, Sophie Dogné, Shangang Zhao, Xi Chen, Clair Crewe, Leon Straub, Lavanya Vishvanath, Zhuzhen Zhang, Mengle Shao, Yongjie Yang, Christy M. Gliniak, Ruth Gordillo, Gordon I. Smith, William L. Holland, Rana K. Gupta, Bingning Dong, Nathalie Caron, Yong Xu, Yucel Akgul, Samuel Klein, and Philipp E. Scherer

Subjects

Science

Abstract

Hyaluronan is a naturally occurring linear polysaccharide that together with collagens, enzymes, and glycoproteins forms the extracellular matrix. Here the authors show that adipose tissue overproduction of Hyaluronan reduces fat accumulation in mice fed high-fat diet and improves systemic glucose homeostasis.

Published

2021

6. Dimethyl Sulfoxide Inhibits Bile Acid Synthesis in Healthy Mice but Does Not Protect Mice from Bile-Acid-Induced Liver Damage

Author

Xi Chen, Huiqiao Li, Yu’e Liu, Jing Qi, Bingning Dong, Shixia Huang, Shangang Zhao, and Yi Zhu

Subjects

dimethyl sulfoxide (DMSO), bile acid, liver damage, nonalcoholic steatohepatitis (NASH), Biology (General), QH301-705.5

Abstract

Bile acids serve a vital function in lipid digestion and absorption; however, their accumulation can precipitate liver damage. In our study, we probed the effects of dimethyl sulfoxide (DMSO) on bile acid synthesis and the ensuing liver damage in mice induced by bile acids. Our findings indicate that DMSO efficaciously curbs bile acid synthesis by inhibiting key enzymes involved in the biosynthetic pathway, both in cultured primary hepatocytes and in vivo. Contrarily, we observed that DMSO treatment did not confer protection against bile-acid-induced liver damage in two distinct mouse models: one induced by a 0.1% DDC diet, leading to bile duct obstruction, and another induced by a CDA-HFD, resulting in non-alcoholic steatohepatitis (NASH). Histopathological and biochemical analyses unveiled a comparable extent of liver injury and fibrosis levels in DMSO-treated mice, characterized by similar levels of increase in Col1a1 and Acta2 expression and equivalent total liver collagen levels. These results suggest that, while DMSO can promptly inhibit bile acid synthesis in healthy mice, compensatory mechanisms might rapidly override this effect, negating any protective impact against bile-acid-induced liver damage in mice. Through these findings, our study underscores the need to reconsider treating DMSO as a mere inert solvent and prompts further exploration to identify more effective therapeutic strategies for the prevention and treatment of bile-acid-associated liver diseases.

Published

2023

7. Response to Kunos et al. and Lotersztajn and Mallat

Author

Simeng Wang, Qingzhang Zhu, Guosheng Liang, Tania Franks, Magalie Boucher, Kendra K. Bence, Mingjian Lu, Carlos M. Castorena, Shangang Zhao, Joel K. Elmquist, Philipp E. Scherer, and Jay D. Horton

Subjects

Metabolism, Medicine

Published

2022

8. Adiponectin preserves metabolic fitness during aging

Author

Na Li, Shangang Zhao, Zhuzhen Zhang, Yi Zhu, Christy M Gliniak, Lavanya Vishvanath, Yu A An, May-yun Wang, Yingfeng Deng, Qingzhang Zhu, Bo Shan, Amber Sherwood, Toshiharu Onodera, Orhan K Oz, Ruth Gordillo, Rana K Gupta, Ming Liu, Tamas L Horvath, Vishwa Deep Dixit, and Philipp E Scherer

Subjects

Adiponectin, longevity, healthspan, metabolism, fat tissue, Medicine, Science, Biology (General), QH301-705.5

Abstract

Adiponectin is essential for the regulation of tissue substrate utilization and systemic insulin sensitivity. Clinical studies have suggested a positive association of circulating adiponectin with healthspan and lifespan. However, the direct effects of adiponectin on promoting healthspan and lifespan remain unexplored. Here, we are using an adiponectin null mouse and a transgenic adiponectin overexpression model. We directly assessed the effects of circulating adiponectin on the aging process and found that adiponectin null mice display exacerbated age-related glucose and lipid metabolism disorders. Moreover, adiponectin null mice have a significantly shortened lifespan on both chow and high-fat diet. In contrast, a transgenic mouse model with elevated circulating adiponectin levels has a dramatically improved systemic insulin sensitivity, reduced age-related tissue inflammation and fibrosis, and a prolonged healthspan and median lifespan. These results support a role of adiponectin as an essential regulator for healthspan and lifespan.

Published

2021

9. Adipose ABHD6 regulates tolerance to cold and thermogenic programs

Author

Pegah Poursharifi, Camille Attané, Yves Mugabo, Anfal Al-Mass, Anindya Ghosh, Clémence Schmitt, Shangang Zhao, Julian Guida, Roxane Lussier, Heidi Erb, Isabelle Chenier, Marie-Line Peyot, Erik Joly, Christophe Noll, André C. Carpentier, S.R. Murthy Madiraju, and Marc Prentki

Subjects

Metabolism, Medicine

Abstract

Enhanced energy expenditure in brown (BAT) and white adipose tissues (WAT) can be therapeutic against metabolic diseases. We examined the thermogenic role of adipose α/β-hydrolase domain 6 (ABHD6), which hydrolyzes monoacylglycerol (MAG), by employing adipose-specific ABHD6-KO mice. Control and KO mice showed similar phenotypes at room temperature and thermoneutral conditions. However, KO mice were resistant to hypothermia, which can be accounted for by the simultaneously increased lipolysis and lipogenesis of the thermogenic glycerolipid/free fatty acid (GL/FFA) cycle in visceral fat, despite unaltered uncoupling protein 1 expression. Upon cold stress, nuclear 2-MAG levels increased in visceral WAT of the KO mice. Evidence is provided that 2-MAG causes activation of PPARα in white adipocytes, leading to elevated expression and activity of GL/FFA cycle enzymes. In the ABHD6-ablated BAT, glucose and oxidative metabolism were elevated upon cold induction, without changes in GL/FFA cycle and lipid turnover. Moreover, response to in vivo β3-adrenergic stimulation was comparable between KO and control mice. Our data reveal a MAG/PPARα/GL/FFA cycling metabolic signaling network in visceral adipose tissue, which contributes to cold tolerance, and that adipose ABHD6 is a negative modulator of adaptive thermogenesis.

Published

2020

10. Suppressing adipocyte inflammation promotes insulin resistance in mice

Author

Qingzhang Zhu, Yu A. An, Min Kim, Zhuzhen Zhang, Shangang Zhao, Yi Zhu, Ingrid Wernstedt Asterholm, Christine M. Kusminski, and Philipp E. Scherer

Subjects

Adipocyte, Inflammation, Insulin resistance, Internal medicine, RC31-1245

Abstract

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.

Published

2020

11. Partial leptin deficiency confers resistance to diet-induced obesity in mice

Author

Shangang Zhao, Na Li, Yi Zhu, Leon Straub, Zhuzhen Zhang, May-Yun Wang, Qingzhang Zhu, Christine M. Kusminski, Joel K. Elmquist, and Philipp E. Scherer

Subjects

Leptin, Partial leptin deficiency, Leptin resistance, Adipose tissue inflammation, Fatty liver, Liver fibrosis, Internal medicine, RC31-1245

Abstract

Objective: Hyperleptinemia per se is sufficient to promote leptin resistance in the obese state. Leptin sensitivity can be restored by reducing circulating leptin levels within a physiologically healthy range and is a viable antiobesity and antidiabetic strategy. However, a previous study suggests that partial leptin deficiency favors diet-induced obesity and related metabolic disorders in mice, arguing that a lower leptin level may indeed promote diet-induced obesity and its associated metabolic disorders. Here, we aim to elucidate what the impact of partial leptin deficiency is on fat mass and insulin sensitivity. Methods: We used two different mouse models of partial leptin deficiency: an adipocyte-specific congenital heterozygous leptin knockout mouse line (LepHZ) and the well-established whole body heterozygous leptin knockout mouse (OBHZ). The metabolic studies of OBHZ and LepHZ mice were performed both on normal carbohydrate-rich chow diet and on a high-fat diet (HFD). Male and female mice were included in the study to account for sex-specific differences. Body weight, food intake, glucose tolerance, and insulin tolerance were tested. Histology of adipose tissue and liver tissue allowed insights into adipose tissue inflammation and hepatic triglyceride content. Immunohistochemistry was paired with RT-PCR analysis for expression levels of inflammatory markers. Results: Both OBHZ and LepHZ mice displayed reduced circulating leptin levels on the chow diet and HFD. On chow diet, male OBHZ and LepHZ mice showed elevated fat mass and body weight, while their glucose tolerance and insulin sensitivity remained unchanged. However, the inability in partially leptin-deficient mice to fully induce circulating leptin during the development of diet-induced obesity results in reduced food intake and leaner mice with lower body weight compared to their littermate controls. Importantly, a strong reduction of adipose tissue inflammation is observed along with improvements in insulin sensitivity and enhanced glucose tolerance. Additionally, partial leptin deficiency protects the mice from fatty liver and liver fibrosis. Chronically HFD-fed OBHZ and LepHZ mice remain more sensitive to exogenous leptin injection, as reflected by their reduced food intake upon an acute leptin treatment. Conclusion: In response to HFD feeding, the inability to upregulate leptin levels due to partial leptin deficiency protects mice from diet-induced obesity and metabolic dysregulation. Thus, in an obesogenic environment, maintaining lower leptin levels is highly beneficial for both obesity and diabetes management. Chronic leptin reduction represents a viable preventive strategy whose efficacy awaits clinical testing.

Published

2020

12. α/β-Hydrolase Domain 6 Deletion Induces Adipose Browning and Prevents Obesity and Type 2 Diabetes

Author

Shangang Zhao, Yves Mugabo, Gwynne Ballentine, Camille Attane, Jose Iglesias, Pegah Poursharifi, Dongwei Zhang, Thuy Anne Nguyen, Heidi Erb, Raphael Prentki, Marie-Line Peyot, Erik Joly, Stephanie Tobin, Stephanie Fulton, J. Mark Brown, S.R. Murthy Madiraju, and Marc Prentki

Subjects

Biology (General), QH301-705.5

Abstract

Suppression of α/β-domain hydrolase-6 (ABHD6), a monoacylglycerol (MAG) hydrolase, promotes glucose-stimulated insulin secretion by pancreatic β cells. We report here that high-fat-diet-fed ABHD6-KO mice show modestly reduced food intake, decreased body weight gain and glycemia, improved glucose tolerance and insulin sensitivity, and enhanced locomotor activity. ABHD6-KO mice also show increased energy expenditure, cold-induced thermogenesis, brown adipose UCP1 expression, fatty acid oxidation, and white adipose browning. Adipose browning and cold-induced thermogenesis are replicated by the ABHD6 inhibitor WWL70 and by antisense oligonucleotides targeting ABHD6. Our evidence suggests that one mechanism by which the lipolysis derived 1-MAG signals intrinsic and cell-autonomous adipose browning is via PPARα and PPARγ activation, and that ABHD6 regulates adipose browning by controlling signal competent 1-MAG levels. Thus, ABHD6 regulates energy homeostasis, brown adipose function, and white adipose browning and is a potential therapeutic target for obesity and type 2 diabetes.

Published

2016

13. Simplified assays of lipolysis enzymes for drug discovery and specificity assessment of known inhibitors

Author

Jose Iglesias, Julien Lamontagne, Heidi Erb, Sari Gezzar, Shangang Zhao, Erik Joly, Vouy Linh Truong, Kathryn Skorey, Sheldon Crane, S.R.Murthy Madiraju, and Marc Prentki

Subjects

adipose triglyceride lipase, alpha/beta hydrolase domain 6, hormone sensitive lipase, diacylglycerol lipase, monoacylglycerol lipase, fatty acid amide hydrolase, Biochemistry, QD415-436

Abstract

Lipids are used as cellular building blocks and condensed energy stores and also act as signaling molecules. The glycerolipid/ fatty acid cycle, encompassing lipolysis and lipogenesis, generates many lipid signals. Reliable procedures are not available for measuring activities of several lipolytic enzymes for the purposes of drug screening, and this resulted in questionable selectivity of various known lipase inhibitors. We now describe simple assays for lipolytic enzymes, including adipose triglyceride lipase (ATGL), hormone sensitive lipase (HSL), sn-1-diacylglycerol lipase (DAGL), monoacylglycerol lipase, α/β-hydrolase domain 6, and carboxylesterase 1 (CES1) using recombinant human and mouse enzymes either in cell extracts or using purified enzymes. We observed that many of the reported inhibitors lack specificity. Thus, Cay10499 (HSL inhibitor) and RHC20867 (DAGL inhibitor) also inhibit other lipases. Marked differences in the inhibitor sensitivities of human ATGL and HSL compared with the corresponding mouse enzymes was noticed. Thus, ATGListatin inhibited mouse ATGL but not human ATGL, and the HSL inhibitors WWL11 and Compound 13f were effective against mouse enzyme but much less potent against human enzyme. Many of these lipase inhibitors also inhibited human CES1. Results describe reliable assays for measuring lipase activities that are amenable for drug screening and also caution about the specificity of the many earlier described lipase inhibitors.

Published

2016

14. α/β-Hydrolase domain-6 and saturated long chain monoacylglycerol regulate insulin secretion promoted by both fuel and non-fuel stimuli

Author

Shangang Zhao, Pegah Poursharifi, Yves Mugabo, Emily J. Levens, Kevin Vivot, Camille Attane, Jose Iglesias, Marie-line Peyot, Erik Joly, S.R. Murthy Madiraju, and Marc Prentki

Subjects

α/β-Hydrolase domain-6, Monoacylglycerol, Insulin secretion, Pancreatic islets, Cytosolic Ca2+, Internal medicine, RC31-1245

Abstract

Objective: α/β-Hydrolase domain-6 (ABHD6) is a newly identified monoacylglycerol (MAG) lipase. We recently reported that it negatively regulates glucose stimulated insulin secretion (GSIS) in the β cells by hydrolyzing lipolysis-derived MAG that acts as a metabolic coupling factor and signaling molecule via exocytotic regulator Munc13-1. Whether ABHD6 and MAG play a role in response to all classes of insulin secretagogues, in particular various fuel and non-fuel stimuli, is unknown. Methods: Insulin secretion in response to various classes of secretagogues, exogenous MAG and pharmacological agents was measured in islets of mice deficient in ABHD6 specifically in the β cell (BKO). Islet perifusion experiments and determinations of glucose and fatty acid metabolism, cytosolic Ca2+ and MAG species levels were carried out. Results: Deletion of ABHD6 potentiated insulin secretion in response to the fuels glutamine plus leucine and α-ketoisocaproate and to the non-fuel stimuli glucagon-like peptide 1, carbamylcholine and elevated KCl. Fatty acids amplified GSIS in control and BKO mice to the same extent. Exogenous 1-MAG amplified insulin secretion in response to fuel and non-fuel stimuli. MAG hydrolysis activity was greatly reduced in BKO islets without changes in total diacylglycerol and triacylglycerol lipase activity. ABHD6 deletion induced insulin secretion independently from KATP channels and did not alter the glucose induced rise in intracellular Ca2+. Perifusion studies showed elevated insulin secretion during second phase of GSIS in BKO islets that was not due to altered cytosolic Ca2+ signaling or because of changes in glucose and fatty acid metabolism. Glucose increased islet saturated long chain 1-MAG species and ABHD6 deletion caused accumulation of these 1-MAG species at both low and elevated glucose. Conclusion: ABHD6 regulates insulin secretion in response to fuel stimuli at large and some non-fuel stimuli by controlling long chain saturated 1-MAG levels that synergize with other signaling pathways for secretion.

Published

2015

15. Crosstalk between adipose tissue and the heart: An update

Author

Chao Li, Xue-Nan Sun, Shangang Zhao, and Philipp E. Scherer

Subjects

Internal Medicine

Abstract

It is important to understand how different human organs coordinate and interact with each other. Since obesity and cardiac disease frequently coincide, the crosstalk between adipose tissues and heart has drawn attention. We appreciate that specific peptides/proteins, lipids, nucleic acids, and even organelles shuttle between the adipose tissues and heart. These bioactive components can profoundly affect the metabolism of cells in distal organs, including heart. Importantly, this process can be dysregulated under pathophysiological conditions. This also opens the door to efforts targeting these mediators as potential therapeutic strategies to treat patients who manifest diabetes and cardiovascular disease. Here, we summarize the recent progress toward a better understanding of how the adipose tissues and heart interact with each other.

Published

2022

16. Dermal adipocytes contribute to the metabolic regulation of dermal fibroblasts

Author

Na Li, Christine M. Kusminski, Christy M. Gliniak, Ilja L. Kruglikov, Philipp E. Scherer, May-Yun Wang, Zhuzhen Zhang, Zhenzhen Zi, Qingzhang Zhu, and Shangang Zhao

Subjects

Male, 0301 basic medicine, Adipose Tissue, White, Lipolysis, Population, Gene Expression, Dermatology, Diet, High-Fat, Biochemistry, Collagen Type I, Extracellular matrix, Mice, 030207 dermatology & venereal diseases, 03 medical and health sciences, chemistry.chemical_compound, Paracrine signalling, 0302 clinical medicine, Dermis, Adipocyte, Paracrine Communication, Adipocytes, medicine, Animals, education, Autocrine signalling, Molecular Biology, Skin, education.field_of_study, Cumulus Cells, integumentary system, Fatty Acids, Fibroblasts, Extracellular Matrix, Cell biology, Collagen Type I, alpha 1 Chain, Crosstalk (biology), Collagen Type III, 030104 developmental biology, medicine.anatomical_structure, Cellular Microenvironment, chemistry, Female, Collagen, Reticular Dermis

Abstract

Dermal fibroblasts are an essential population of skin cells. They are not only responsible for synthesis and remodelling of the extracellular matrix of the dermis, but also communicate with other skin cells via autocrine and paracrine interactions. Skin-associated dermal adipocytes reside below the reticular dermis. Strong lipolysis is observed during the regression of dermal adipocytes. However, the nature of the local intercellular crosstalk in which lipids released by dermal adipocytes affecting the metabolism of adjacent skin fibroblasts has not yet been examined. With the use of a series of novel mouse models that allow us to manipulate adipocytes, we demonstrate that dermal adipocytes can modulate the structure of the dermis through regulating extracellular matrix production in dermal fibroblasts. Fatty acids released by dermal adipocytes are involved in this process. Our observations offer new in vivo insights into the role of dermal adipocyte-derived lipids in influencing metabolism of adjacent local cells in the skin through a paracrine effect in the microenvironment of the dermal adipocyte.

Published

2020

17. Activating Connexin43 gap junctions primes adipose tissue for therapeutic intervention

Author

Yi Zhu, Na Li, Mingyang Huang, Xi Chen, Yu A. An, Jianping Li, Shangang Zhao, Jan-Bernd Funcke, Jianhong Cao, Zhenyan He, Qingzhang Zhu, Zhuzhen Zhang, Zhao V. Wang, Lin Xu, Kevin W. Williams, Chien Li, Kevin Grove, and Philipp E. Scherer

Subjects

General Pharmacology, Toxicology and Pharmaceutics

Abstract

Adipose tissue is a promising target for treating obesity and metabolic diseases. However, pharmacological agents usually fail to effectively engage adipocytes due to their extraordinarily large size and insufficient vascularization, especially in obese subjects. We have previously shown that during cold exposure, connexin43 (Cx43) gap junctions are induced and activated to connect neighboring adipocytes to share limited sympathetic neuronal input amongst multiple cells. We reason the same mechanism may be leveraged to improve the efficacy of various pharmacological agents that target adipose tissue. Using an adipose tissue-specific Cx43 overexpression mouse model, we demonstrate effectiveness in connecting adipocytes to augment metabolic efficacy of the

Published

2021

18. Cannabinoid receptor 1 signaling in hepatocytes and stellate cells does not contribute to NAFLD

Author

Kendra K. Bence, Philipp E. Scherer, Mingjian Lu, Qingzhang Zhu, Shangang Zhao, Guosheng Liang, Jay D. Horton, Simeng Wang, Magalie Boucher, Tania Franks, Carlos M. Castorena, and Joel K. Elmquist

Subjects

Liver Cirrhosis, medicine.medical_specialty, medicine.medical_treatment, Diet, High-Fat, Mice, Receptor, Cannabinoid, CB1, Fibrosis, Non-alcoholic Fatty Liver Disease, Internal medicine, Nonalcoholic fatty liver disease, Hepatic Stellate Cells, Medicine, Animals, Obesity, Receptor, Letter to the Editor, business.industry, General Medicine, medicine.disease, Endocannabinoid system, Mice, Inbred C57BL, Insulin signaling, Endocrinology, medicine.anatomical_structure, Metabolism, Hepatocyte, Hepatic stellate cell, Hepatocytes, Cannabinoid, Metabolic syndrome, business, Signal Transduction

Abstract

The endocannabinoid system regulates appetite and energy expenditure and inhibitors of the cannabinoid receptor-1 (CB-1) induce weight loss with improvement in components of the metabolic syndrome. While CB-1 blockage in brain is responsible for weight loss, many of the metabolic benefits associated with CB-1 blockade have been attributed to inhibition of CB-1 signaling in the periphery. As a result, there has been interest in developing a peripherally restricted CB-1 inhibitor for the treatment of nonalcoholic fatty liver disease (NAFLD) that would lack the unwanted centrally mediated side effects. Here, we produced mice that lacked CB-1 receptors in hepatocytes or stellate cells to determine if CB-1 signaling contributes to the development of NAFLD or liver fibrosis. Deletion of CB-1 receptors in hepatocytes did not alter the development of NAFLD in mice fed a high sucrose high fat diet or high fat diet (HFD). Similarly, deletion of CB-1 deletion specifically in stellate cells also did not prevent the development of NAFLD in mice fed the HFD nor did it protect mice for carbon tetrachloride (CCl4)-induced fibrosis. Combined, these studies do not support a direct role for hepatocyte or stellate cell CB-1 signaling in the development of NAFLD or liver fibrosis.

Published

2021

19. PKM1 Exerts Critical Roles in Cardiac Remodeling Under Pressure Overload in the Heart

Author

Craig R. Malloy, Xiang Luo, Charles D. Smart, Jun Lin, Lin Tan, Yu An, Philipp E. Scherer, Qinfeng Li, Chongshan Dai, Luke I. Szweda, Guihao Chen, Thomas G. Gillette, Guangyu Zhang, Meihui Wang, Yingfeng Deng, Shangang Zhao, Guosheng Fu, Gaurav Sharma, Yingchao Gong, Jason W. Locasale, Chao Li, Zhao V. Wang, Shawn M. Davidson, Waleed M. Elhelaly, Philip L. Lorenzi, Abdallah Elnwasany, Matthew G. Vander Heiden, Juan Liu, and Shuang Jie Lv

Subjects

0301 basic medicine, medicine.medical_specialty, Glucose utilization, Thyroid Hormones, Cell Respiration, Gene Expression, 030204 cardiovascular system & hematology, Models, Biological, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Physiology (medical), Internal medicine, medicine, Animals, Humans, Glycolysis, Myocytes, Cardiac, Hemodynamic stress, Pressure overload, Heart Failure, Mice, Knockout, Ventricular Remodeling, business.industry, Membrane Proteins, medicine.disease, Pyruvate dehydrogenase complex, Mitochondria, Enzyme Activation, Disease Models, Animal, 030104 developmental biology, Glucose, Heart failure, Heart Function Tests, Cardiology, Disease Progression, Disease Susceptibility, Cardiology and Cardiovascular Medicine, business, Carrier Proteins, Pyruvate kinase, Biomarkers

Abstract

Background: Metabolic remodeling precedes most alterations during cardiac hypertrophic growth under hemodynamic stress. The elevation of glucose utilization has been recognized as a hallmark of metabolic remodeling. However, its role in cardiac hypertrophic growth and heart failure in response to pressure overload remains to be fully illustrated. Here, we aimed to dissect the role of cardiac PKM1 (pyruvate kinase muscle isozyme 1) in glucose metabolic regulation and cardiac response under pressure overload. Methods: Cardiac-specific deletion of PKM1 was achieved by crossing the floxed PKM1 mouse model with the cardiomyocyte-specific Cre transgenic mouse. PKM1 transgenic mice were generated under the control of tetracycline response elements, and cardiac-specific overexpression of PKM1 was induced by doxycycline administration in adult mice. Pressure overload was triggered by transverse aortic constriction. Primary neonatal rat ventricular myocytes were used to dissect molecular mechanisms. Moreover, metabolomics and nuclear magnetic resonance spectroscopy analyses were conducted to determine cardiac metabolic flux in response to pressure overload. Results: We found that PKM1 expression is reduced in failing human and mouse hearts. It is important to note that cardiomyocyte-specific deletion of PKM1 exacerbates cardiac dysfunction and fibrosis in response to pressure overload. Inducible overexpression of PKM1 in cardiomyocytes protects the heart against transverse aortic constriction–induced cardiomyopathy and heart failure. At the mechanistic level, PKM1 is required for the augmentation of glycolytic flux, mitochondrial respiration, and ATP production under pressure overload. Furthermore, deficiency of PKM1 causes a defect in cardiomyocyte growth and a decrease in pyruvate dehydrogenase complex activity at both in vitro and in vivo levels. Conclusions: These findings suggest that PKM1 plays an essential role in maintaining a homeostatic response in the heart under hemodynamic stress.

Published

2021

20. Author response: Adiponectin preserves metabolic fitness during aging

Author

Ruth Gordillo, Yi Zhu, May-Yun Wang, Christy M. Gliniak, Orhan K. Öz, Tamas L. Horvath, Amber Sherwood, Philipp E. Scherer, Yingfeng Deng, Toshiharu Onodera, Shangang Zhao, Qingzhang Zhu, Bo Shan, Vishwa Deep Dixit, Yu An, Na Li, Rana K. Gupta, Zhuzhen Zhang, Ming Liu, and Lavanya Vishvanath

Subjects

medicine.medical_specialty, Endocrinology, Adiponectin, business.industry, Internal medicine, medicine, business

Published

2021

21. Glucagon blockade restores functional β-cell mass in type 1 diabetic mice and enhances function of human islets

Author

May Yun Wang, Greg Poffenberger, Philipp E. Scherer, William L. Holland, Reshing Ye, Ruth E. Gimeno, Yiyi Zhang, Kyle W. Sloop, Derek C. Leonard, S. Kay McCorkle, Alexander M. Efanov, Roger H Unger, Yi Zhu, Alison Von Deylen, Alvin C. Powers, E. Danielle Dean, Shiuhwei Chen, Kamrul H. Chowdhury, Shangang Zhao, Zhuzhen Zhang, Xinxin Yu, Young Chul Lee, Ezekiel B. Quittner-Strom, Na Li, and Amnon Schlegel

Subjects

Blood Glucose, Medical Sciences, medicine.medical_treatment, Islets of Langerhans Transplantation, Gene Expression, Nod, chemistry.chemical_compound, Mice, Mice, Inbred NOD, Insulin-Secreting Cells, Receptors, Glucagon, Glucose homeostasis, Multidisciplinary, geography.geographical_feature_category, islet, diabetes, C-Peptide, C-peptide, Antibodies, Monoclonal, Organ Size, Biological Sciences, Islet, Treatment Outcome, hormones, hormone substitutes, and hormone antagonists, medicine.medical_specialty, insulin, Glucagon, Diabetes Mellitus, Experimental, Islets of Langerhans, Diabetes mellitus, Internal medicine, medicine, Animals, Humans, Hypoglycemic Agents, Cell Lineage, geography, business.industry, Insulin, medicine.disease, Endocrinology, Diabetes Mellitus, Type 1, chemistry, Glucagon-Secreting Cells, regeneration, Cell Transdifferentiation, business, Glucagon receptor

Abstract

Significance Both type 1 and type 2 diabetes are associated with reduced β-cell mass or function, resulting from decreased proliferation and increased apoptosis. Understanding the signals governing β-cell survival and regeneration is critical for developing strategies to maintain healthy populations of these cells in individuals. Both forms of diabetes are associated with hyperglucagonemia and an increased plasma glucagon:insulin ratio. Glucagon excess contributes to metabolic dysregulation of the diabetic state and glucagon receptor antagonism is a potential target area for the treatment and prevention of diabetes. Our studies presented here suggest that blockade of glucagon signaling lowers glycemia in mouse models of type 1 diabetes while enhancing formation of functional β-cell mass and production of insulin-positive cells from α-cell precursors., We evaluated the potential for a monoclonal antibody antagonist of the glucagon receptor (Ab-4) to maintain glucose homeostasis in type 1 diabetic rodents. We noted durable and sustained improvements in glycemia which persist long after treatment withdrawal. Ab-4 promoted β-cell survival and enhanced the recovery of insulin+ islet mass with concomitant increases in circulating insulin and C peptide. In PANIC-ATTAC mice, an inducible model of β-cell apoptosis which allows for robust assessment of β-cell regeneration following caspase-8–induced diabetes, Ab-4 drove a 6.7-fold increase in β-cell mass. Lineage tracing suggests that this restoration of functional insulin-producing cells was at least partially driven by α-cell-to-β-cell conversion. Following hyperglycemic onset in nonobese diabetic (NOD) mice, Ab-4 treatment promoted improvements in C-peptide levels and insulin+ islet mass was dramatically increased. Lastly, diabetic mice receiving human islet xenografts showed stable improvements in glycemic control and increased human insulin secretion.

Published

2021

22. Adiponectin Preserves Metabolic Fitness During Aging

Author

Yi Zhu, Christy M. Gliniak, Yingfeng Deng, Shangang Zhao, Ming Liu, Ruth Gordillo, Lavanya Vishvanath, Orhan K. Öz, Philipp E. Scherer, Rana K. Gupta, Vishwa Deep Dixit, Tamas L. Horvath, Na Li, Qingzhang Zhu, Yu An, May-Yun Wang, Toshiharu Onodera, and Zhuzhen Zhang

Subjects

Null mice, Genetically modified mouse, medicine.medical_specialty, Lipid Metabolism Disorder, Adiponectin, business.industry, Transgene, Regulator, nutritional and metabolic diseases, Insulin sensitivity, medicine.disease, Endocrinology, Fibrosis, Internal medicine, Medicine, business, hormones, hormone substitutes, and hormone antagonists

Abstract

Adiponectin is essential for the regulation of tissue substrate utilization and systemic insulin sensitivity. Clinical studies have suggested a positive association of circulating adiponectin with healthspan and lifespan. However, the direct effects of adiponectin on promoting healthspan and lifespan remain unexplored. Here, we are using an adiponectin null mouse and a transgenic adiponectin overexpression model. We directly assessed the effects of circulating adiponectin on the aging process and found that adiponectin null mice display exacerbated age-related glucose and lipid metabolism disorders. Moreover, adiponectin null mice have a significantly shortened lifespan on both chow and high-fat diet (HFD). In contrast, a transgenic mouse model with elevated circulating adiponectin levels has a dramatically improved systemic insulin sensitivity, reduced age-related tissue inflammation and fibrosis, and a prolonged healthspan and median lifespan. These results support a role of adiponectin as an essential regulator for healthspan and lifespan.

Published

2021

23. Adiponectin, Leptin and Cardiovascular Disorders

Author

Shangang Zhao, Philipp E. Scherer, and Christine M. Kusminski

Subjects

0301 basic medicine, Leptin, medicine.medical_specialty, Physiology, Adipose tissue, Bariatric Surgery, 030204 cardiovascular system & hematology, Cardiovascular System, Article, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Endocrine system, Animals, Humans, Obesity, Adiponectin, business.industry, digestive, oral, and skin physiology, nutritional and metabolic diseases, Cardiovascular Agents, medicine.disease, 030104 developmental biology, Endocrinology, Adipose Tissue, Cardiovascular Diseases, Leptin signaling, Anti-Obesity Agents, Cardiology and Cardiovascular Medicine, business, Cardiovascular outcomes, hormones, hormone substitutes, and hormone antagonists, Metabolism, Inborn Errors, Signal Transduction

Abstract

The landmark discoveries of leptin and adiponectin firmly established adipose tissue as a sophisticated and highly active endocrine organ, opening a new era of investigating adipose-mediated tissue crosstalk. Both obesity-associated hyperleptinemia and hypoadiponectinemia are important biomarkers to predict cardiovascular outcomes, suggesting a crucial role for adiponectin and leptin in obesity-associated cardiovascular disorders. Normal physiological levels of adiponectin and leptin are indeed essential to maintain proper cardiovascular function. Insufficient adiponectin and leptin signaling results in cardiovascular dysfunction. However, a paradox of high levels of both leptin and adiponectin is emerging in the pathogenesis of cardiovascular disorders. Here, we (1) summarize the recent progress in the field of adiponectin and leptin and its association with cardiovascular disorders, (2) further discuss the underlying mechanisms for this new paradox of leptin and adiponectin action, and (3) explore the possible application of partial leptin reduction, in addition to increasing the adiponectin/leptin ratio as a means to prevent or reverse cardiovascular disorders.

Published

2021

24. Adiponectin preserves metabolic fitness during aging

Author

Yu An, Christy M. Gliniak, Yi Zhu, May-Yun Wang, Amber Sherwood, Yingfeng Deng, Tamas L. Horvath, Orhan K. Öz, Philipp E. Scherer, Shangang Zhao, Bo Shan, Rana K. Gupta, Toshiharu Onodera, Qingzhang Zhu, Ming Liu, Lavanya Vishvanath, Ruth Gordillo, Na Li, Zhuzhen Zhang, and Vishwa Deep Dixit

Subjects

0301 basic medicine, Male, Aging, Lipid Metabolism Disorder, Mouse, Regulator, Adipose tissue, healthspan, Mice, 0302 clinical medicine, Fibrosis, Homeostasis, Biology (General), General Neuroscience, General Medicine, 030220 oncology & carcinogenesis, Medicine, Female, Adiponectin, hormones, hormone substitutes, and hormone antagonists, Research Article, Genetically modified mouse, medicine.medical_specialty, QH301-705.5, Science, Transgene, Longevity, Mice, Transgenic, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Internal medicine, medicine, Animals, General Immunology and Microbiology, business.industry, nutritional and metabolic diseases, Metabolism, Cell Biology, medicine.disease, Lipid Metabolism, 030104 developmental biology, Endocrinology, Glucose, fat tissue, Insulin Resistance, business, metabolism

Abstract

Adiponectin is essential for the regulation of tissue substrate utilization and systemic insulin sensitivity. Clinical studies have suggested a positive association of circulating adiponectin with healthspan and lifespan. However, the direct effects of adiponectin on promoting healthspan and lifespan remain unexplored. Here, we are using an adiponectin null mouse and a transgenic adiponectin overexpression model. We directly assessed the effects of circulating adiponectin on the aging process and found that adiponectin null mice display exacerbated age-related glucose and lipid metabolism disorders. Moreover, adiponectin null mice have a significantly shortened lifespan on both chow and high-fat diet. In contrast, a transgenic mouse model with elevated circulating adiponectin levels has a dramatically improved systemic insulin sensitivity, reduced age-related tissue inflammation and fibrosis, and a prolonged healthspan and median lifespan. These results support a role of adiponectin as an essential regulator for healthspan and lifespan.

Published

2020

25. Adipocyte iron levels impinge on a fat-gut crosstalk to regulate intestinal lipid absorption and mediate protection from obesity

Author

Yingfeng Deng, Zhuzhen Zhang, Shangang Zhao, Qingzhang Zhu, May-Yun Wang, Laurent Gautron, Yi Zhu, Zhenzhen Zi, Philipp E. Scherer, Shiuhwei Chen, Jan-Bernd Funcke, Prithvi Raj, Clair Crewe, Christine M. Kusminski, Charlotte E. Lee, Luke J. Engelking, Alexandra L. Ghaben, Ruth Gordillo, Na Li, Leon G. Straub, and Yu An

Subjects

0301 basic medicine, medicine.medical_specialty, Diabetes risk, Physiology, Enterocyte, Iron, Adipose tissue, Transferrin receptor, White adipose tissue, Diet, High-Fat, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Adipocyte, Internal medicine, medicine, Adipocytes, Animals, Obesity, Molecular Biology, Intestinal lipid absorption, Cell Biology, Lipid Metabolism, Lipids, Vesicular transport protein, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, Adipose Tissue, 030217 neurology & neurosurgery

Abstract

Iron overload is positively associated with diabetes risk. However, the role of iron in adipose tissue remains incompletely understood. Here, we report that transferrin-receptor-1-mediated iron uptake is differentially required for distinct subtypes of adipocytes. Notably, adipocyte-specific transferrin receptor 1 deficiency substantially protects mice from high-fat-diet-induced metabolic disorders. Mechanistically, low cellular iron levels have a positive impact on the health of the white adipose tissue and can restrict lipid absorption from the intestine through modulation of vesicular transport in enterocytes following high-fat diet feeding. Specific reduction of adipocyte iron by AAV-mediated overexpression of the iron exporter Ferroportin1 in adult mice effectively mimics these protective effects. In summary, our studies highlight an important role of adipocyte iron in the maintenance of systemic metabolism through an adipocyte-enterocyte axis, offering an additional level of control over caloric influx into the system after feeding by regulating intestinal lipid absorption.

Published

2020

26. Hepatic GALE Regulates Whole-Body Glucose Homeostasis by Modulating Tff3 Expression

Author

Chao Xing, Shangang Zhao, Fang Zhang, Mengle Shao, Ruth Gordillo, Olga Zagnitko, Hua V. Lin, Yang Li, Ping Xu, Philipp E. Scherer, Yi Zhu, Bei B. Zhang, Yingfeng Deng, Alexandra L. Ghaben, Huachuan Cao, Rana K. Gupta, and David Scott

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Mice, Transgenic, Carbohydrate metabolism, Biology, Endoplasmic Reticulum, Gene Expression Regulation, Enzymologic, 03 medical and health sciences, chemistry.chemical_compound, Mice, UDPglucose 4-Epimerase, Internal medicine, Internal Medicine, medicine, Glucose homeostasis, Animals, Homeostasis, Endoplasmic reticulum, Leloir pathway, carbohydrates (lipids), 030104 developmental biology, Endocrinology, Metabolism, Glucose, Gluconeogenesis, chemistry, Liver, Galactose, Unfolded protein response, Trefoil Factor-3

Abstract

Transcripts of key enzymes in the Leloir pathway of galactose metabolism in mouse livers are significantly increased after chronic high-fat/high-sucrose feeding. UDP-galactose-4-epimerase (GALE) is the last enzyme in this pathway that converts UDP-galactose to UDP-glucose and was previously identified as a downstream target of the endoplasmic reticulum (ER) stress effector spliced X-box binding protein 1, suggesting an interesting cross talk between galactose and glucose metabolism in the context of hepatic ER stress and whole-body metabolic fitness. However, its specific role in glucose metabolism is not established. Using an inducible and tissue-specific mouse model, we report that hepatic overexpression of Gale increases gluconeogenesis from pyruvate and impairs glucose tolerance. Conversely, genetic reduction of Gale in liver improves glucose tolerance. Transcriptional profiling identifies trefoil factor 3 (Tff3) as one of the downstream targets of GALE. Restoration of Tff3 expression corrects glucose intolerance in Gale-overexpressing mice. These studies reveal a new link between hepatic GALE activity and whole-body glucose homeostasis via regulation of hepatic Tff3 expression.

Published

2017

27. Partial leptin deficiency confers resistance to diet-induced obesity in mice

Author

Qingzhang Zhu, Na Li, Christine M. Kusminski, Yi Zhu, Shangang Zhao, Leon G. Straub, Joel K. Elmquist, May-Yun Wang, Zhuzhen Zhang, and Philipp E. Scherer

Subjects

0301 basic medicine, Leptin, Male, Adipose tissue, Mice, Obese, Mice, 0302 clinical medicine, Insulin, Adipose tissue inflammation, Mice, Knockout, Leptin Deficiency, Fatty liver, digestive, oral, and skin physiology, Adipose Tissue, Liver, Knockout mouse, Body Composition, Female, Original Article, Partial leptin deficiency, medicine.symptom, hormones, hormone substitutes, and hormone antagonists, medicine.medical_specialty, lcsh:Internal medicine, Adipose Tissue, White, Leptin resistance, Liver fibrosis, 030209 endocrinology & metabolism, Inflammation, Diet, High-Fat, 03 medical and health sciences, Downregulation and upregulation, Metabolic Diseases, Internal medicine, medicine, Animals, Obesity, lcsh:RC31-1245, Molecular Biology, business.industry, Body Weight, Cell Biology, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Insulin Resistance, business

Abstract

Objective Hyperleptinemia per se is sufficient to promote leptin resistance in the obese state. Leptin sensitivity can be restored by reducing circulating leptin levels within a physiologically healthy range and is a viable antiobesity and antidiabetic strategy. However, a previous study suggests that partial leptin deficiency favors diet-induced obesity and related metabolic disorders in mice, arguing that a lower leptin level may indeed promote diet-induced obesity and its associated metabolic disorders. Here, we aim to elucidate what the impact of partial leptin deficiency is on fat mass and insulin sensitivity. Methods We used two different mouse models of partial leptin deficiency: an adipocyte-specific congenital heterozygous leptin knockout mouse line (LepHZ) and the well-established whole body heterozygous leptin knockout mouse (OBHZ). The metabolic studies of OBHZ and LepHZ mice were performed both on normal carbohydrate-rich chow diet and on a high-fat diet (HFD). Male and female mice were included in the study to account for sex-specific differences. Body weight, food intake, glucose tolerance, and insulin tolerance were tested. Histology of adipose tissue and liver tissue allowed insights into adipose tissue inflammation and hepatic triglyceride content. Immunohistochemistry was paired with RT-PCR analysis for expression levels of inflammatory markers. Results Both OBHZ and LepHZ mice displayed reduced circulating leptin levels on the chow diet and HFD. On chow diet, male OBHZ and LepHZ mice showed elevated fat mass and body weight, while their glucose tolerance and insulin sensitivity remained unchanged. However, the inability in partially leptin-deficient mice to fully induce circulating leptin during the development of diet-induced obesity results in reduced food intake and leaner mice with lower body weight compared to their littermate controls. Importantly, a strong reduction of adipose tissue inflammation is observed along with improvements in insulin sensitivity and enhanced glucose tolerance. Additionally, partial leptin deficiency protects the mice from fatty liver and liver fibrosis. Chronically HFD-fed OBHZ and LepHZ mice remain more sensitive to exogenous leptin injection, as reflected by their reduced food intake upon an acute leptin treatment. Conclusion In response to HFD feeding, the inability to upregulate leptin levels due to partial leptin deficiency protects mice from diet-induced obesity and metabolic dysregulation. Thus, in an obesogenic environment, maintaining lower leptin levels is highly beneficial for both obesity and diabetes management. Chronic leptin reduction represents a viable preventive strategy whose efficacy awaits clinical testing., Highlights • Partial leptin deficiency protects from diet-induced obesity. • Reduced leptin protects from diet-induced obesity independent of sex. • Reduction of circulating leptin levels inhibits HFD-induced adipose tissue inflammation. • Partial leptin deficiency confers resistance to HFD-induced liver fibrosis. • Partial leptin deficiency enhances leptin sensitivity.

Published

2020

28. Dermal adipose tissue has high plasticity and undergoes reversible dedifferentiation in mice

Author

Chelsea Hepler, Yingfeng Deng, Ashwani Kumar, Laurent Gautron, Qingzhang Zhu, May-Yun Wang, Chao Xing, Clair Crewe, Yu An, Qiong A. Wang, Philipp E. Scherer, Lavanya Vishvanath, Toshiharu Onodera, Christine M. Kusminski, Na Li, Zhenzhen Zi, Alexandra L. Ghaben, Mengle Shao, Shangang Zhao, Yi Zhu, Rana K. Gupta, Ilja L. Kruglikov, Nolwenn Joffin, Zhuzhen Zhang, and Ruth Gordillo

Subjects

0301 basic medicine, Male, Adipocytes, White, Cell Plasticity, Adipose tissue, White adipose tissue, Cell Separation, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Molecular level, Lineage tracing, Animals, White Adipocytes, Myofibroblasts, Skin, Wound Healing, integumentary system, Gene Expression Profiling, Cell Differentiation, General Medicine, Cell Dedifferentiation, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, 030220 oncology & carcinogenesis, Wound healing, Hair Follicle, Homeostasis, Research Article

Abstract

Dermal adipose tissue (also known as dermal white adipose tissue and herein referred to as dWAT) has been the focus of much discussion in recent years. However, dWAT remains poorly characterized. The fate of the mature dermal adipocytes and the origin of the rapidly reappearing dermal adipocytes at different stages remain unclear. Here, we isolated dermal adipocytes and characterized dermal fat at the cellular and molecular level. Together with dWAT's dynamic responses to external stimuli, we established that dermal adipocytes are a distinct class of white adipocytes with high plasticity. By combining pulse-chase lineage tracing and single-cell RNA sequencing, we observed that mature dermal adipocytes undergo dedifferentiation and redifferentiation under physiological and pathophysiological conditions. Upon various challenges, the dedifferentiated cells proliferate and redifferentiate into adipocytes. In addition, manipulation of dWAT highlighted an important role for mature dermal adipocytes for hair cycling and wound healing. Altogether, these observations unravel a surprising plasticity of dermal adipocytes and provide an explanation for the dynamic changes in dWAT mass that occur under physiological and pathophysiological conditions, and highlight the important contributions of dWAT toward maintaining skin homeostasis.

Published

2019

29. Leptin: Less Is More

Author

Shangang Zhao, Joel K. Elmquist, Philipp E. Scherer, and Christine M. Kusminski

Subjects

0301 basic medicine, Leptin, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Context (language use), Type 2 diabetes, Bioinformatics, 03 medical and health sciences, Mice, 0302 clinical medicine, Internal Medicine, medicine, Animals, Humans, Leptin resistance, Obesity, Leptin Deficiency, Extramural, business.industry, digestive, oral, and skin physiology, medicine.disease, Biological Evolution, 030104 developmental biology, Perspectives in Diabetes, Lipodystrophy, business, hormones, hormone substitutes, and hormone antagonists

Abstract

The successful use of leptin for the treatment of individuals with lipodystrophy and leptin deficiency is well established. However, pharmacological approaches of leptin therapy for the treatment of diet-induced obesity have been ineffective. There is ample room for a better understanding of the much famed “leptin resistance” phenomenon. Our recent data in this area prompt us to call for a conceptual shift. This shift entails a model in which a reduction of bioactive leptin levels in the context of obesity triggers a high degree of leptin sensitization and improved leptin action, both centrally and peripherally. Put another way, hyperleptinemia per se causes leptin resistance and associated metabolic disorders. In this perspective, we briefly discuss the underlying conceptual steps that led us to explore partial leptin reduction as a viable therapeutic avenue. We hope this discussion will contribute to potential future applications of partial leptin reduction therapy for the treatment of obesity and type 2 diabetes.

Published

2019

30. Pathologic HIF1α signaling drives adipose progenitor dysfunction in obesity

Author

Shangang Zhao, Douglas W. Strand, Bo Shan, Chelsea Hepler, Gervaise H. Henry, Yibo Wu, Lavanya Vishvanath, Qianbin Zhang, Rana K. Gupta, Yu An, and Mengle Shao

Subjects

Adipose Tissue, White, Adipose tissue, White adipose tissue, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Precursor cell, Adipocyte, Genetics, Progenitor cell, 030304 developmental biology, 0303 health sciences, Adipogenesis, biology, Cell Differentiation, Cell Biology, Adipose Tissue, chemistry, biology.protein, Cancer research, Molecular Medicine, Phosphorylation, Energy Metabolism, 030217 neurology & neurosurgery, Platelet-derived growth factor receptor

Abstract

Adipose precursor cells (APCs) exhibits regional variation in response to obesity, for unclear reasons. Here, we reveal that HIFα-induced PDGFRβ signaling within murine white adipose tissue (WAT) PDGFRβ+ cells drives inhibitory serine 112 (S112) phosphorylation of PPARγ, the master regulator of adipogenesis. Levels of PPARγ S112 phosphorylation in WAT PDGFRb+ cells are depot-dependent, with levels of PPARγ phosphorylation in PDGFRβ+ cells inversely correlating with their capacity for adipogenesis upon high fat diet feeding. HIFα suppression in PDGFRβ+ progenitors promotes subcutaneous and intra-abdominal adipogenesis, healthy WAT remodeling, and improved metabolic health in obesity. These metabolic benefits are mimicked by treatment of obese mice with the PDGFR antagonist, Imatinib, which promotes adipocyte hyperplasia and glucose tolerance in a progenitor cell PPARγ-dependent manner. Our studies unveil a mechanism underlying depot-specific responses of APCs to high-fat feeding, and highlight the potential for APCs to be targeted pharmacologically to improve metabolic health in obesity.

Published

2021

31. Connexin 43 Mediates White Adipose Tissue Beiging by Facilitating the Propagation of Sympathetic Neuronal Signals

Author

Mengle Shao, David C. Spray, Yong Gao, William L. Holland, Joshua A. Johnson, Wei Huang, Kevin W. Williams, Matthew D. Lynes, Caroline Tao, Philipp E. Scherer, Lei Cao, Herbert B. Tanowitz, Yu-Hua Tseng, Rana K. Gupta, Ting Yao, Hua V. Lin, Tiemin Liu, Yi Zhu, Shangang Zhao, Joel K. Elmquist, Aaron M. Cypess, and Olga T. Gupta

Subjects

0301 basic medicine, medicine.medical_specialty, Sympathetic nervous system, Sympathetic Nervous System, Physiology, Adipose Tissue, White, Population, Adipose tissue, Connexin, White adipose tissue, Biology, Models, Biological, 03 medical and health sciences, Adipose Tissue, Brown, Internal medicine, medicine, Animals, Promoter Regions, Genetic, education, Molecular Biology, Uncoupling Protein 1, Neurons, Denervation, education.field_of_study, Gap junction, Gap Junctions, food and beverages, Cell Biology, Adipose Tissue, Beige, Adaptation, Physiological, Thermogenin, Cell biology, Cold Temperature, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Connexin 43, Glycyrrhetinic Acid, Gene Deletion, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

"Beige" adipocytes reside in white adipose tissue (WAT) and dissipate energy as heat. Several studies have shown that cold temperature can activate pro-opiomelanocortin-expressing (POMC) neurons and increase sympathetic neuronal tone to regulate WAT beiging. WAT, however, is traditionally known to be sparsely innervated. Details regarding the neuronal innervation and, more importantly, the propagation of the signal within the population of "beige" adipocytes are sparse. Here, we demonstrate that beige adipocytes display an increased cell-to-cell coupling via connexin 43 (Cx43) gap junction channels. Blocking of Cx43 channels by 18α-glycyrrhetinic acid decreases POMC-activation-induced adipose tissue beiging. Adipocyte-specific deletion of Cx43 reduces WAT beiging to a level similar to that observed in denervated fat pads. In contrast, overexpression of Cx43 is sufficient to promote beiging even with mild cold stimuli. These data reveal the importance of cell-to-cell communication, effective in cold-induced WAT beiging, for the propagation of limited neuronal inputs in adipose tissue.

Published

2016

32. FoxO1 Deacetylation Decreases Fatty Acid Oxidation in β-Cells and Sustains Insulin Secretion in Diabetes

Author

Shangang Zhao, Jason Fan, Alexander S. Banks, Ja Young Kim-Muller, Domenico Accili, Young Jung R. Kim, and Marc Prentki

Subjects

0301 basic medicine, endocrine system, medicine.medical_treatment, 030209 endocrinology & metabolism, FOXO1, Mitochondrion, Biology, Biochemistry, Diabetes Mellitus, Experimental, Mice, 03 medical and health sciences, 0302 clinical medicine, Insulin-Secreting Cells, Insulin Secretion, medicine, Animals, Insulin, Molecular Biology, Beta oxidation, geography, geography.geographical_feature_category, Forkhead Box Protein O1, Fatty Acids, Wild type, Acetylation, Forkhead Transcription Factors, Molecular Bases of Disease, Lipid metabolism, Cell Biology, Lipid Metabolism, Islet, Mitochondria, 030104 developmental biology, Mutation, Oxidation-Reduction, Ex vivo

Abstract

Pancreatic β-cell dysfunction contributes to onset and progression of type 2 diabetes. In this state β-cells become metabolically inflexible, losing the ability to select between carbohydrates and lipids as substrates for mitochondrial oxidation. These changes lead to β-cell dedifferentiation. We have proposed that FoxO proteins are activated through deacetylation-dependent nuclear translocation to forestall the progression of these abnormalities. However, how deacetylated FoxO exert their actions remains unclear. To address this question, we analyzed islet function in mice homozygous for knock-in alleles encoding deacetylated FoxO1 (6KR). Islets expressing 6KR mutant FoxO1 have enhanced insulin secretion in vivo and ex vivo and decreased fatty acid oxidation ex vivo. Remarkably, the gene expression signature associated with FoxO1 deacetylation differs from wild type by only ∼2% of the >4000 genes regulated in response to re-feeding. But this narrow swath includes key genes required for β-cell identity, lipid metabolism, and mitochondrial fatty acid and solute transport. The data support the notion that deacetylated FoxO1 protects β-cell function by limiting mitochondrial lipid utilization and raise the possibility that inhibition of fatty acid oxidation in β-cells is beneficial to diabetes treatment.

Published

2016

33. Diabetes-Hepatic GALE Regulates Whole-Body Glucose Homeostasis by Modulating Tff3 Expression.pdf

Author

Zhu, Yi, Shangang Zhao, Yingfeng Deng, Gordillo, Ruth, Ghaben, Alexandra, Mengle Shao, Zhang, Fang, Xu, Ping, Li, Yang, Huachuan Cao, Zagnitko, Olga, Scott, David, Gupta, Rana, Xing, Chao, Zhang, Bei, Lin, Hua, and Scherer, Philipp E.

Subjects

carbohydrates (lipids), FOS: Clinical medicine, 110107 Metabolic Medicine

Abstract

Transcripts of key enzymes in the Leloir pathway ofgalactose metabolism in mouse livers are significantly increasedafter chronic high-fat/high-sucrose feeding. UDPgalactose-4-epimerase (GALE) is the last enzyme in thispathway that converts UDP-galactose to UDP-glucoseand was previously identified as a downstream target ofthe endoplasmic reticulum(ER) stress effector spliced X-boxbinding protein 1, suggesting an interesting cross talkbetween galactose and glucose metabolism in the contextof hepatic ER stress and whole-body metabolic fitness.However, its specific role in glucose metabolism is notestablished. Using an inducible and tissue-specific mousemodel, we report that hepatic overexpression of Gale increasesgluconeogenesis from pyruvate and impairs glucosetolerance. Conversely, genetic reduction of Gale inliver improves glucose tolerance. Transcriptional profilingidentifies trefoil factor 3 (Tff3) as one of the downstreamtargets of GALE. Restoration of Tff3 expression correctsglucose intolerance in Gale-overexpressing mice. Thesestudies reveal a new link between hepatic GALE activityand whole-body glucose homeostasis via regulation ofhepatic Tff3 expression

Published

2019

34. TLR4-Induced Local Adipose Inflammation Critically Regulates Glucose Homeostasis

Author

Philipp E. Scherer and Shangang Zhao

Subjects

0301 basic medicine, medicine.medical_specialty, 030102 biochemistry & molecular biology, business.industry, Endocrinology, Diabetes and Metabolism, Adipose tissue, Inflammation, Systemic inflammation, medicine.disease, 03 medical and health sciences, chemistry.chemical_compound, Insulin resistance, Endocrinology, chemistry, Adipogenesis, Internal medicine, Adipocyte, Internal Medicine, medicine, TLR4, Glucose homeostasis, medicine.symptom, business

Abstract

Acute adipose inflammation is beneficial for adipose tissue remodeling, while chronic unsolved inflammation may lead to systemic insulin resistance. Toll-like receptor 4 (TLR4) may be an important mediator for obesity-associated chronic low grade inflammation and insulin resistance. However, up to date, we do not have a model available that allows us to study systemic consequences of adipose tissue inflammation originating selectively at the level of the adipocyte. Here, using cre-loxP and doxycycline-inducible system, we generated a new mouse model, which exclusively expresses physiological levels of TLR4 in adipocytes of adult mice in the background of an otherwise global TLR4 null mouse (“ATLR4 mice”). Upon LPS injection, ATLR4 mice show modest acute inflammation in local adipose tissue, but no inflammatory response at the systemic level. However, when exposed long-term to a HFD diet, ATLR4 mice show reduced body weight gain as well as improved glucose and insulin tolerance. This beneficial effect may - at least in part - be due to increased browning of subcutaneous white adipocytes. Under thermoneutral conditions (when we minimize the contributions of the browning effects), the ALTR4 mice show a slightly higher body weight gain, but still preserve better glucose tolerance. RNAseq data indicates the beneficial effect of ATLR4 mice may be associated with enhancing acetyl-coA synthesis pathway to promote PPARgamma acetylation and adipogenesis. Based on that, we conclude that adipose tissue inflammation originating in the adipocyte contributes only minimal, if any, effects on systemic inflammation. In contrast, TLR4-induced local inflammation signaling results in improvements in glucose homeostasis. Disclosure S. Zhao: None. P.E. Scherer: None.

Published

2018

35. Simplified assays of lipolysis enzymes for drug discovery and specificity assessment of known inhibitors

Author

Shangang Zhao, Heidi Erb, Sari Gezzar, Kathryn Skorey, Jose Antonio Iglesias, Erik Joly, Julien Lamontagne, S.R. Murthy Madiraju, Vouy Linh Truong, Marc Prentki, and Sheldon Crane

Subjects

0301 basic medicine, hormone sensitive lipase, Diacylglycerol lipase, adipose triglyceride lipase, Lipolysis, alpha/beta hydrolase domain 6, Hormone-sensitive lipase, QD415-436, Pharmacology, Biochemistry, 03 medical and health sciences, Mice, Endocrinology, diacylglycerol lipase, monoacylglycerol lipase, Drug Discovery, Methods, fatty acid amide hydrolase, Animals, Humans, Lipase, Enzyme Inhibitors, Triglycerides, chemistry.chemical_classification, Lipoprotein lipase, biology, Chemistry, Lipogenesis, Fatty Acids, Cell Biology, Sterol Esterase, Monoacylglycerol Lipases, Monoacylglycerol lipase, Lipoprotein Lipase, 030104 developmental biology, Enzyme, Adipose Tissue, Lipase inhibitors, Adipose triglyceride lipase, biology.protein, Carboxylic Ester Hydrolases

Abstract

Lipids are used as cellular building blocks and condensed energy stores and also act as signaling molecules. The glycerolipid/ fatty acid cycle, encompassing lipolysis and lipogenesis, generates many lipid signals. Reliable procedures are not available for measuring activities of several lipolytic enzymes for the purposes of drug screening, and this resulted in questionable selectivity of various known lipase inhibitors. We now describe simple assays for lipolytic enzymes, including adipose triglyceride lipase (ATGL), hormone sensitive lipase (HSL), sn-1-diacylglycerol lipase (DAGL), monoacylglycerol lipase, α/β-hydrolase domain 6, and carboxylesterase 1 (CES1) using recombinant human and mouse enzymes either in cell extracts or using purified enzymes. We observed that many of the reported inhibitors lack specificity. Thus, Cay10499 (HSL inhibitor) and RHC20867 (DAGL inhibitor) also inhibit other lipases. Marked differences in the inhibitor sensitivities of human ATGL and HSL compared with the corresponding mouse enzymes was noticed. Thus, ATGListatin inhibited mouse ATGL but not human ATGL, and the HSL inhibitors WWL11 and Compound 13f were effective against mouse enzyme but much less potent against human enzyme. Many of these lipase inhibitors also inhibited human CES1. Results describe reliable assays for measuring lipase activities that are amenable for drug screening and also caution about the specificity of the many earlier described lipase inhibitors.

Published

2016

36. Metabolic Inflexibility Impairs Insulin Secretion and Results In MODY-like Diabetes in Triple FoxO-Deficient Mice

Author

Marc Prentki, Shangang Zhao, Edward Y. Skolnik, Anthony W. Ferrante, Domenico Accili, YoungJung R. Kim, Shekhar Srivastava, Ja Young Kim-Muller, Yves Mugabo, Hye Lim Noh, and S.R. Murthy Madiraju

Subjects

Blood Glucose, medicine.medical_specialty, Calcium Channels, L-Type, Physiology, medicine.medical_treatment, FOXO1, Cell Cycle Proteins, Type 2 diabetes, Biology, Article, Mice, Internal medicine, Diabetes mellitus, Insulin-Secreting Cells, medicine, Animals, Insulin, Hepatocyte Nuclear Factor 1-alpha, Molecular Biology, Homeodomain Proteins, Mice, Knockout, Glucose tolerance test, medicine.diagnostic_test, Forkhead Box Protein O1, Gene Expression Profiling, Forkhead Box Protein O3, Forkhead Transcription Factors, Cell Biology, Glucose Tolerance Test, medicine.disease, Mitochondria, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, Hepatocyte nuclear factor 4, Diabetes Mellitus, Type 2, Hepatocyte Nuclear Factor 4, Trans-Activators, PDX1, Calcium, Energy source

Abstract

SummaryPancreatic β cell failure in type 2 diabetes is associated with functional abnormalities of insulin secretion and deficits of β cell mass. It’s unclear how one begets the other. We have shown that loss of β cell mass can be ascribed to impaired FoxO1 function in different models of diabetes. Here we show that ablation of the three FoxO genes (1, 3a, and 4) in mature β cells results in early-onset, maturity-onset diabetes of the young (MODY)-like diabetes, with abnormalities of the MODY networks Hnf4α, Hnf1α, and Pdx1. FoxO-deficient β cells are metabolically inflexible, i.e., they preferentially utilize lipids rather than carbohydrates as an energy source. This results in impaired ATP generation and reduced Ca2+-dependent insulin secretion. The present findings demonstrate a secretory defect caused by impaired FoxO activity that antedates dedifferentiation. We propose that defects in both pancreatic β cell function and mass arise through FoxO-dependent mechanisms during diabetes progression.

Published

2014

37. Partial Leptin Reduction as an Insulin Sensitization and Weight Loss Strategy

Author

Tiemin Liu, Philipp E. Scherer, Ningyan Zhang, Christine M. Kusminski, Alexandre Caron, Na Li, Hui Deng, Kai Sun, Jia Sun, Zhuzhen Zhang, Zhenyan He, Yingfeng Deng, Robbie D. Schultz, Kevin W. Williams, Angela K. Odle, Charlotte E. Lee, Gwen V. Childs, Joel K. Elmquist, Min Kim, Ruth Gordillo, Shangang Zhao, Yi Zhu, Qingzhang Zhu, Zhiqiang An, and Wei Xiong

Subjects

Leptin, 0301 basic medicine, medicine.medical_specialty, Physiology, medicine.medical_treatment, Mice, Inbred Strains, Context (language use), Article, Eating, Mice, 03 medical and health sciences, 0302 clinical medicine, Weight loss, Diabetes mellitus, Internal medicine, Weight Loss, medicine, Animals, Insulin, Obesity, Molecular Biology, business.industry, digestive, oral, and skin physiology, Cell Biology, medicine.disease, Antibodies, Neutralizing, Weight Reduction Programs, 030104 developmental biology, Endocrinology, Hypothalamus, Insulin Resistance, medicine.symptom, Energy Metabolism, business, Weight gain, hormones, hormone substitutes, and hormone antagonists, 030217 neurology & neurosurgery

Abstract

The physiological role of leptin is thought to be a driving force to reduce food intake and increase energy expenditure. However, leptin therapies in the clinic have failed to effectively treat obesity, predominantly due to a phenomenon referred to as leptin resistance. The mechanisms linking obesity and the associated leptin resistance remain largely unclear. With various mouse models and a leptin neutralizing antibody, we demonstrated that hyperleptinemia is a driving force for metabolic disorders. A partial reduction of plasma leptin levels in the context of obesity restores hypothalamic leptin sensitivity and effectively reduces weight gain and enhances insulin sensitivity. These results highlight that a partial reduction in plasma leptin levels leads to improved leptin sensitivity, while pointing to a new avenue for therapeutic interventions in the treatment of obesity and its associated comorbidities.

Published

2019

38. Metabolic fate of glucose and candidate signaling and excess-fuel detoxification pathways in pancreatic β-cells

Author

Julien Lamontagne, Yves Mugabo, Marie-Line Peyot, Erik Joly, Barbara E. Corkey, S.R. Murthy Madiraju, Anfal Al-Mass, Marc Prentki, and Shangang Zhao

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Biology, Carbohydrate metabolism, Biochemistry, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Adenosine Triphosphate, Internal medicine, Insulin-Secreting Cells, medicine, Animals, Rats, Wistar, Molecular Biology, Triglycerides, Dihydroxyacetone phosphate, chemistry.chemical_classification, Glycogen, Triglyceride, Dose-Response Relationship, Drug, Fatty Acids, Fatty acid, Lipid metabolism, Cell Biology, Metabolism, Rats, Citric acid cycle, Malonyl Coenzyme A, 030104 developmental biology, Endocrinology, Glucose, chemistry, Dihydroxyacetone Phosphate, Glycerophosphates, Cholesterol Esters, Signal Transduction

Abstract

Glucose metabolism promotes insulin secretion in β-cells via metabolic coupling factors that are incompletely defined. Moreover, chronically elevated glucose causes β-cell dysfunction, but little is known about how cells handle excess fuels to avoid toxicity. Here we sought to determine which among the candidate pathways and coupling factors best correlates with glucose-stimulated insulin secretion (GSIS), define the fate of glucose in the β-cell, and identify pathways possibly involved in excess-fuel detoxification. We exposed isolated rat islets for 1 h to increasing glucose concentrations and measured various pathways and metabolites. Glucose oxidation, oxygen consumption, and ATP production correlated well with GSIS and saturated at 16 mm glucose. However, glucose utilization, glycerol release, triglyceride and glycogen contents, free fatty acid (FFA) content and release, and cholesterol and cholesterol esters increased linearly up to 25 mm glucose. Besides being oxidized, glucose was mainly metabolized via glycerol production and release and lipid synthesis (particularly FFA, triglycerides, and cholesterol), whereas glycogen production was comparatively low. Using targeted metabolomics in INS-1(832/13) cells, we found that several metabolites correlated well with GSIS, in particular some Krebs cycle intermediates, malonyl-CoA, and lower ADP levels. Glucose dose-dependently increased the dihydroxyacetone phosphate/glycerol 3-phosphate ratio in INS-1(832/13) cells, indicating a more oxidized state of NAD in the cytosol upon glucose stimulation. Overall, the data support a role for accelerated oxidative mitochondrial metabolism, anaplerosis, and malonyl-CoA/lipid signaling in β-cell metabolic signaling and suggest that a decrease in ADP levels is important in GSIS. The results also suggest that excess-fuel detoxification pathways in β-cells possibly comprise glycerol and FFA formation and release extracellularly and the diversion of glucose carbons to triglycerides and cholesterol esters.

Published

2016

39. Rehmanniae Radix in osteoporosis: A review of traditional Chinese medicinal uses, phytochemistry, pharmacokinetics and pharmacology

Author

Baosheng Zhao, Shangang Zhao, Ruyuan Zhu, Chenyue Liu, Min Fu, Lili Wang, Jinfa Tang, Jianzhao Niu, Yu Li, Sihua Gao, Dongwei Zhang, Yubo Guo, Haixia Liu, and Rufeng Ma

Subjects

0301 basic medicine, medicine.medical_specialty, Osteoporosis, Traditional Chinese medicine, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Osteogenesis, Internal medicine, Drug Discovery, medicine, Animals, Humans, Medicine, Chinese Traditional, Adverse effect, Pharmacology, Osteoblasts, Traditional medicine, business.industry, Plant Extracts, Rehmanniae Radix, medicine.disease, Clinical trial, Rehmannia, 030104 developmental biology, Endocrinology, Knowledge resource, 030220 oncology & carcinogenesis, Secondary osteoporosis, business, Drugs, Chinese Herbal, Phytotherapy

Abstract

Ethnopharmacological relevance Emerging clinical usage and pharmacological effects have been achieved in using Rehmanniae Radix either singly or in combination with other herbs to treat skeletal diseases in traditional Chinese medicine (TCM) in the recent years. This study is aimed to provide a comprehensive review about the historical TCM interpretation of the action of Rehmanniae Radix in osteoporosis, its usage in clinical trials and osteoporotic models, its main phytochemical constituents, and its pharmacokinetics. Materials and methods Several databases included PubMed, China Knowledge Resource Integrated Database, China Science and Technology Journal Database, National Science and Technology Library and the Web of Science Database were consulted to locate the publications pertaining to Rehmanniae Radix . The initial inquiry was conducted for the presence of the following terms combinations in the abstracts: Rehmanniae Radix , Dihuang, phytochemistry, pharmacokinetics, osteoporosis, bone, osteoclast and osteoblast. About 330 research papers and reviews were consulted. Results In TCM, Rehmanniae Radix exerts the anti-osteoporotic effect via regulating the functions of kidney and liver as well as improving blood circulation. 107 clinical trials are identified that used Rehmanniae Radix in combination with other herbs to treat post-menopausal, senile and secondary osteoporosis. Most of the clinical trials are characterized by high efficacy and no obvious adverse effects. However, the efficacies of these clinical trials are limited because of small patient sample size, short treatment duration and poor clinical design. In addition, TCM herbs under the clinical study are not clear because of a lack of standardization and authentication. The pharmacokinetics data demonstrate that the ingredients of Rehmanniae Radix are widely distributed after administration, and that catalpol and ajugol as well as acetoside are supposed to be the active constituents. More than 140 individual compounds have been currently isolated from this plant and reported to show pleiotropic effects on various diseases. Rehmanniae Radix displays bone protecting features in the osteoporosis models via the delicate balance between osteoclastogenesis and osteoblastogenesis through single herb extracts and its isolated compounds. Conclusions The successful inclusion of Rehmanniae Radix in clinical trials and preclinical studies for the management of osteoporosis has attracted rising attentions for identifying potential anti-osteoporotic candidates from this plant and clinical existing TCM formulas, which will further speed up anti-osteoporosis drug discovery processes. Properly designed and well controlled prospective studies are still needed to further demonstrate bone protective actions and safe use of this herb and its ingredients

Published

2016

40. Requirements of calcium fluxes and ERK kinase activation for glucose- and interleukin-1β-induced β-cell apoptosis

Author

Bin Zhao, Qin Wang, Hongqiang Fei, and Shangang Zhao

Subjects

MAPK/ERK pathway, medicine.medical_specialty, Thapsigargin, Calcium Channels, L-Type, Calmodulin, Interleukin-1beta, Clinical Biochemistry, Apoptosis, Biology, chemistry.chemical_compound, Insulin-Secreting Cells, Internal medicine, Insulin Secretion, Calcium flux, medicine, Animals, Humans, Insulin, Calcium Signaling, Extracellular Signal-Regulated MAP Kinases, Egtazic Acid, Molecular Biology, Sulfonamides, Voltage-dependent calcium channel, Kinase, Ionomycin, Cell Biology, General Medicine, Calcium Channel Blockers, Rats, Enzyme Activation, Glucose, Endocrinology, chemistry, Mibefradil, biology.protein, Nimodipine, Signal transduction, Ion Channel Gating

Abstract

Increasing evidence indicates that beta-cell apoptosis and impaired secretory function were partly mediated by interleukin (IL)-1beta and/or high-glucose-induced beta-cell production of IL-1beta. However, the specific signal transduction pathways and molecular events involved in beta-cell dysfunction remain largely unresolved. In this study, we investigated whether Ca(2+) and extracellular signal-regulated kinase (ERK) activation plays a role for IL-1beta action in rat islets. Exposure of rat islets for 4 days to 33.3 mM glucose and 140 ng/ml IL-1beta- induced beta-cell apoptosis and impaired glucose-stimulated insulin secretion. By Western blotting with phosphospecific antibodies, glucose and IL-1beta were shown to activate ERK. Ca(2+) channel blocker nimodipine or ERK inhibitor PD98059 prevented glucose- and IL-1beta-induced ERK activation, beta-cell apoptosis, and impaired function. Furthermore, treatment with Ca(2+) ionophore ionomycin, or exposure to thapsigargin, an inhibitor of sarco(endo)plasmic reticulum Ca(2+) ATPase, all caused an amplification of IL-1beta-induced ERK activation in rat islet. On the other hand, a chelator of intracellular free Ca(2+) [bis-(o-aminophenoxy)-N,N,N',N'-tetraacetic acid-acetoxymethyl] (BAPTA/AM) and an inhibitor of calmodulin (W7) diminished IL-1beta-induced phosphorylation of ERK. Finally, islet release of IL-1beta in response to high glucose could be abrogated by nimodipine, mibefradil, or PD98059. Together, these data suggest that glucose- and IL-1beta-induced beta-cell secretory dysfunction and apoptosis are Ca(2+) influx and ERK dependent in rat islets.

Published

2008

41. Identification of a mammalian glycerol-3-phosphate phosphatase: Role in metabolism and signaling in pancreatic β-cells and hepatocytes

Author

Erik Joly, Annegrit Seifried, Yves Mugabo, Julien Lamontagne, Marc Prentki, Marie-Line Peyot, Camille Attané, Pegah Poursharifi, Antje Gohla, Sari Gezzar, Dongwei Zhang, S.R. Murthy Madiraju, Shangang Zhao, Jose Antonio Iglesias, and Anfal Al-Mass

Subjects

Glycerol, Male, 0301 basic medicine, Molecular Sequence Data, Nutritional Status, Mitochondria, Liver, Carbohydrate metabolism, Biology, Cell Line, Mitochondrial Proteins, Lactones, Mice, 03 medical and health sciences, chemistry.chemical_compound, Insulin resistance, Stress, Physiological, Insulin-Secreting Cells, Insulin Secretion, medicine, Animals, Insulin, Glycolysis, Amino Acid Sequence, Beta oxidation, Orlistat, Multidisciplinary, Sequence Homology, Amino Acid, Hydrolysis, Fatty Acids, Metabolism, Lipid Metabolism, medicine.disease, Phosphoric Monoester Hydrolases, Rats, 030104 developmental biology, PNAS Plus, Biochemistry, Gluconeogenesis, chemistry, Glycerophosphates, Hepatocytes, Carbohydrate Metabolism, RNA Interference, Glycerol 3-phosphate, Phosphoglycolate phosphatase, Signal Transduction

Abstract

Obesity, and the associated disturbed glycerolipid/fatty acid (GL/FA) cycle, contribute to insulin resistance, islet β-cell failure, and type 2 diabetes. Flux through the GL/FA cycle is regulated by the availability of glycerol-3-phosphate (Gro3P) and fatty acyl-CoA. We describe here a mammalian Gro3P phosphatase (G3PP), which was not known to exist in mammalian cells, that can directly hydrolyze Gro3P to glycerol. We identified that mammalian phosphoglycolate phosphatase, with an uncertain function, acts in fact as a G3PP. We found that G3PP, by controlling Gro3P levels, regulates glycolysis and glucose oxidation, cellular redox and ATP production, gluconeogenesis, glycerolipid synthesis, and fatty acid oxidation in pancreatic islet β-cells and hepatocytes, and that glucose stimulated insulin secretion and the response to metabolic stress, e.g., glucolipotoxicity, in β-cells. In vivo overexpression of G3PP in rat liver lowers body weight gain and hepatic glucose production from glycerol and elevates plasma HDL levels. G3PP is expressed at various levels in different tissues, and its expression varies according to the nutritional state in some tissues. As Gro3P lies at the crossroads of glucose, lipid, and energy metabolism, control of its availability by G3PP adds a key level of metabolic regulation in mammalian cells, and G3PP offers a potential target for type 2 diabetes and cardiometabolic disorders.

Published

2016

42. α/β-Hydrolase Domain 6 Deletion Induces Adipose Browning and Prevents Obesity and Type 2 Diabetes

Author

Heidi Erb, Camille Attané, Thuy Anne Nguyen, J. Mark Brown, Stephanie Tobin, Marc Prentki, Stephanie Fulton, Yves Mugabo, Dongwei Zhang, S.R. Murthy Madiraju, Marie Line Peyot, Erik Joly, Gwynne Ballentine, Shangang Zhao, Raphael Prentki, Pegah Poursharifi, and Jose Antonio Iglesias

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Adipose tissue, White adipose tissue, Biology, Motor Activity, Diet, High-Fat, General Biochemistry, Genetics and Molecular Biology, Energy homeostasis, Diglycerides, 03 medical and health sciences, Mice, Adipose Tissue, Brown, Internal medicine, 3T3-L1 Cells, medicine, Browning, Lipolysis, Animals, Humans, PPAR alpha, Obesity, lcsh:QH301-705.5, Beta oxidation, Uncoupling Protein 1, 2. Zero hunger, Mice, Knockout, Biphenyl Compounds, Thermogenesis, ABHD6, Monoacylglycerol Lipases, Mice, Inbred C57BL, PPAR gamma, 030104 developmental biology, Endocrinology, HEK293 Cells, lcsh:Biology (General), Diabetes Mellitus, Type 2, Female, Carbamates, Lipid Peroxidation, Energy Metabolism

Abstract

SummarySuppression of α/β-domain hydrolase-6 (ABHD6), a monoacylglycerol (MAG) hydrolase, promotes glucose-stimulated insulin secretion by pancreatic β cells. We report here that high-fat-diet-fed ABHD6-KO mice show modestly reduced food intake, decreased body weight gain and glycemia, improved glucose tolerance and insulin sensitivity, and enhanced locomotor activity. ABHD6-KO mice also show increased energy expenditure, cold-induced thermogenesis, brown adipose UCP1 expression, fatty acid oxidation, and white adipose browning. Adipose browning and cold-induced thermogenesis are replicated by the ABHD6 inhibitor WWL70 and by antisense oligonucleotides targeting ABHD6. Our evidence suggests that one mechanism by which the lipolysis derived 1-MAG signals intrinsic and cell-autonomous adipose browning is via PPARα and PPARγ activation, and that ABHD6 regulates adipose browning by controlling signal competent 1-MAG levels. Thus, ABHD6 regulates energy homeostasis, brown adipose function, and white adipose browning and is a potential therapeutic target for obesity and type 2 diabetes.

Published

2015

43. α/β-Hydrolase Domain-6-Accessible Monoacylglycerol Controls Glucose-Stimulated Insulin Secretion

Author

Jose Antonio Iglesias, Abdelkarim Abousalham, Viviane Delghingaro-Augusto, Matthew A. Davis, Yves Mugabo, Erik Joly, Shangang Zhao, Li Xie, Marc Prentki, Bouchra Taïb, J. Mark Brown, Herbert Y. Gaisano, Roxane Lussier, Marie Line Peyot, S.R. Murthy Madiraju, Depierre, Frédérique, Métabolisme, Enzymes et Mécanismes Moléculaires (MEM²), Institut de Chimie et Biochimie Moléculaires et Supramoléculaires (ICBMS), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut National des Sciences Appliquées de Lyon (INSA Lyon), Université de Lyon-Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-École Supérieure Chimie Physique Électronique de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL), and Université de Lyon-Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-École Supérieure Chimie Physique Électronique de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Physiology, medicine.medical_treatment, [SDV]Life Sciences [q-bio], Lactones, Mice, 0302 clinical medicine, Insulin-Secreting Cells, Insulin Secretion, Insulin, Enzyme Inhibitors, RNA, Small Interfering, Receptors, Cannabinoid, Receptor, [SDV.BBM.BC] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Cells, Cultured, Mice, Knockout, 0303 health sciences, ABHD6, [SDV] Life Sciences [q-bio], Monoglycerides, RNA Interference, Signal transduction, Protein Binding, Signal Transduction, medicine.medical_specialty, endocrine system, Lipolysis, Nerve Tissue Proteins, 030209 endocrinology & metabolism, Carbohydrate metabolism, Biology, Exocytosis, 03 medical and health sciences, Internal medicine, medicine, Animals, Humans, Rats, Wistar, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, 030304 developmental biology, Orlistat, Biphenyl Compounds, Lipid metabolism, Lipase, Cell Biology, Lipid Metabolism, Monoacylglycerol Lipases, Rats, Mice, Inbred C57BL, Monoacylglycerol lipase, Glucose, Endocrinology, Anti-Obesity Agents, Carbamates

Abstract

International audience; Glucose metabolism in pancreatic β cells stimulates insulin granule exocytosis, and this process requires generation of a lipid signal. However, the signals involved in lipid amplification of glucose-stimulated insulin secretion (GSIS) are unknown. Here we show that in β cells, glucose stimulates production of lipolysis-derived long-chain saturated monoacylglycerols, which further increase upon inhibition of the membrane-bound monoacylglycerol lipase α/β-Hydrolase Domain-6 (ABHD6). ABHD6 expression in β cells is inversely proportional to GSIS. Exogenous monoacylglycerols stimulate β cell insulin secretion and restore GSIS suppressed by the pan-lipase inhibitor orlistat. Whole-body and β-cell-specific ABHD6-KO mice exhibit enhanced GSIS, and their islets show elevated monoacylglycerol production and insulin secretion in response to glucose. Inhibition of ABHD6 in diabetic mice restores GSIS and improves glucose tolerance. Monoacylglycerol binds and activates the vesicle priming protein Munc13-1, thereby inducing insulin exocytosis. We propose saturated monoacylglycerol as a signal for GSIS and ABHD6 as a negative modulator of insulin secretion.

Published

2014

44. Glucolipotoxicity alters lipid partitioning and causes mitochondrial dysfunction, cholesterol, and ceramide deposition and reactive oxygen species production in INS832/13 ss-cells

Author

Enrique Roche, Émilie Pepin, Annie Barbeau, Marc Prentki, Erik Joly, Isabel Maestre, Robert Sladek, Shangang Zhao, Jose Antonio Iglesias, Jean Buteau, and Wissal El-Assaad

Subjects

medicine.medical_specialty, Ceramide, Palmitates, Apoptosis, Biology, Mitochondrion, Carbohydrate metabolism, Ceramides, Models, Biological, chemistry.chemical_compound, Endocrinology, Lipid oxidation, Acetyltransferases, Internal medicine, Lipid droplet, Insulin-Secreting Cells, medicine, Animals, Fatty acid synthesis, Oligonucleotide Array Sequence Analysis, chemistry.chemical_classification, Fatty acid, Lipid metabolism, Lipid Metabolism, Nucleotidyltransferases, Mitochondria, Rats, Cholesterol, Glucose, chemistry, Biochemistry, RNA Interference, Reactive Oxygen Species

Abstract

Elevated glucose and saturated fatty acids synergize in inducing apoptosis in INS832/13 cells and in human islet cells. In order to gain insight into the molecular mechanism(s) of glucolipotoxicity (Gltox), gene profiling and metabolic analyses were performed in INS832/13 cells cultured at 5 or 20 mm glucose in the absence or presence of palmitate. Expression changes were observed for transcripts involved in mitochondrial, lipid, and glucose metabolism. At 24 h after Gltox, increased expression of lipid partitioning genes suggested a promotion of fatty acid esterification and reduced lipid oxidation/detoxification, whereas changes in the expression of energy metabolism genes suggested mitochondrial dysfunction. These changes were associated with decreased glucose-induced insulin secretion, total insulin content, ATP levels, AMP-kinase activity, mitochondrial membrane potential and fat oxidation, unchanged de novo fatty acid synthesis, and increased reactive oxygen species, cholesterol, ceramide, and triglyceride levels. However, the synergy between elevated glucose and palmitate to cause ß-cell toxicity in term of apoptosis and reduced glucose-induced insulin secretion only correlated with triglyceride and ceramide depositions. Overexpression of endoplasmic reticulum glycerol-3-phosphate acyl transferase to enhance lipid esterification amplified Gltox at intermediate glucose (11 mm), whereas reducing acetyl-coenzyme A carboxylase 1 expression by small interfering RNA to shift lipid partitioning to fat oxidation reduced Gltox. The results suggest that Gltox entails alterations in lipid partitioning, sterol and ceramide accumulation, mitochondrial dysfunction, and reactive oxygen species production, all contributing to altering ß-cell function. The data also suggest that the early promotion of lipid esterification processes is instrumental in the Gltox process.

Published

2010

45. Hepatic GALE Regulates Whole-Body Glucose Homeostasis by Modulating Expression.

Author

Yi Zhu, Shangang Zhao, Yingfeng Deng, Gordillo, Ruth, Ghaben, Alexandra L., Mengle Shao, Fang Zhang, Ping Xu, Yang Li, Huachuan Cao, Zagnitko, Olga, Scott, David A., Gupta, Rana K., Chao Xing, Bei B. Zhang, Hua V. Lin, Scherer, Philipp E., Zhu, Yi, Zhao, Shangang, and Deng, Yingfeng

Subjects

*HOMEOSTASIS, *GLUCOSE metabolism, *LIVER, *LABORATORY mice, *ENZYMES, *GLUCONEOGENESIS, *MAMMALS, *ENZYME metabolism, *ANIMAL experimentation, *CYTOPLASM, *GENES, *MICE, *RESEARCH funding

Abstract

Transcripts of key enzymes in the Leloir pathway of galactose metabolism in mouse livers are significantly increased after chronic high-fat/high-sucrose feeding. UDP-galactose-4-epimerase (GALE) is the last enzyme in this pathway that converts UDP-galactose to UDP-glucose and was previously identified as a downstream target of the endoplasmic reticulum (ER) stress effector spliced X-box binding protein 1, suggesting an interesting cross talk between galactose and glucose metabolism in the context of hepatic ER stress and whole-body metabolic fitness. However, its specific role in glucose metabolism is not established. Using an inducible and tissue-specific mouse model, we report that hepatic overexpression of Gale increases gluconeogenesis from pyruvate and impairs glucose tolerance. Conversely, genetic reduction of Gale in liver improves glucose tolerance. Transcriptional profiling identifies trefoil factor 3 (Tff3) as one of the downstream targets of GALE. Restoration of Tff3 expression corrects glucose intolerance in Gale-overexpressing mice. These studies reveal a new link between hepatic GALE activity and whole-body glucose homeostasis via regulation of hepatic Tff3 expression. [ABSTRACT FROM AUTHOR]

Published

2017

46. Metabolic fate of glucose and candidate signaling and excess-fuel detoxification pathways in pancreatic β-cells.

Author

Yves Mugabo, Shangang Zhao, Lamontagne, Julien, Al-Mass, Anfal, Peyot, Marie-Line, Corkey, Barbara E., Joly, Erik, Madiraju, S. R. Murthy, and Prentki, Marc

Subjects

*GLYCOGENOLYSIS, *GLUCOSE metabolism, *METABOLIC detoxification, *PANCREATIC beta cells, *FREE fatty acids

Abstract

Glucose metabolism promotes insulin secretion in β-cells via metabolic coupling factors that are incompletely defined. Moreover, chronically elevated glucose causes β-cell dysfunction, but little is known about how cells handle excess fuels to avoid toxicity. Here we sought to determine which among the candidate pathways and coupling factors best correlates with glucosestimulated insulin secretion (GSIS), define the fate of glucose in the β-cell, and identify pathways possibly involved in excessfuel detoxification. We exposed isolated rat islets for 1 h to increasing glucose concentrations and measured various pathways and metabolites. Glucose oxidation, oxygen consumption, and ATP production correlated well with GSIS and saturated at 16 mM glucose. However, glucose utilization, glycerol release, triglyceride and glycogen contents, free fatty acid (FFA) content and release, and cholesterol and cholesterol esters increased linearly up to 25 mM glucose. Besides being oxidized, glucose was mainly metabolized via glycerol production and release and lipid synthesis (particularly FFA, triglycerides, and cholesterol), whereas glycogen production was comparatively low. Using targeted metabolomics in INS-1(832/13) cells, we found that several metabolites correlated well with GSIS, in particular some Krebs cycle intermediates, malonyl-CoA, and lower ADP levels. Glucose dose-dependently increased the dihydroxyacetone phosphate/glycerol 3-phosphate ratio in INS-1(832/13) cells, indicating a more oxidized state of NAD in the cytosol upon glucose stimulation. Overall, the data support a role for accelerated oxidative mitochondrial metabolism, anaplerosis, and malonyl-CoA/lipid signaling in β-cell metabolic signaling and suggest that a decrease in ADP levels is important in GSIS. The results also suggest that excess-fuel detoxification pathways in β-cells possibly comprise glycerol and FFA formation and release extracellularly and the diversion of glucose carbons to triglycerides and cholesterol esters. [ABSTRACT FROM AUTHOR]

Published

2017

47. A Novel Pathway of Glucodetoxification in Pancreatic β-cells

Author

I. Jose, Shangang Zhao, Marc Prentki, Yves Mugabo, Erik Joly, S. Gezzar-Dandashi, Marie-Line Peyot, and S. R. Madiraju

Subjects

Endocrinology, business.industry, Endocrinology, Diabetes and Metabolism, Internal Medicine, Cancer research, Medicine, General Medicine, business

Published

2014

48. Monoacylglycerol as a Metabolic Coupling Factor in Glucose-Stimulated Insulin Secretion

Author

Erik Joly, Marc Prentki, Yves Mugabo, S.R. Murthy Madiraju, Marie-Line Peyot, Shangang Zhao, and Jose Antonio Iglesias

Subjects

chemistry.chemical_classification, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, Fatty acid, General Medicine, ABHD6, Monoacylglycerol lipase, Glutamine, Endocrinology, chemistry, Internal medicine, Internal Medicine, medicine, Lipolysis, Secretion, business, Diacylglycerol kinase

Abstract

Insulin secretion by the pancreatic -cell in response to post-prandial increase in blood glucose levels is an essential physiological process that is governed by cellular, nutritional and pathological factors. Other fuels including amino acids like leucine and glutamine and also fatty acids contribute to further augment insulin secretion. Failure to secrete adequate amount of insulin according to the changing demands of the body by -cell is a key determinant of diabetes. The role played by the elevated Ca influx and K-ATP channels in insulin secretion is well known. Even though the precise mechanism of the lipid amplification of insulin secretion and the involved molecular signals are not clear, Glycerolipid/Free fatty acid (GL/FFA) cycle and its lipolytic segment have been recognized as essential components in the lipid amplification pathway of insulin secretion. Diacylglycerol produced by lipolysis was proposed as an important lipid amplification signal. However, hydrolysis of triglycerides and also of diacylglycerols is shown to be essential for glucose stimulated insulin secretion (GSIS), indicating a possible role for monoacylglycerol (MAG) in this process. In the present study we demonstrate that the obliterated GSIS due to lipolysis inhibition in cells can be restored by providing exogenous MAG. In the -cells MAG levels increase significantly in the presence of high glucose concentration and specific inhibition of the major MAG hydrolase, abhydrolase-6 (ABHD6), in -cells and islets with WWL70 leads to accumulation of MAG with concomitant increase in insulin secretion. Lipidomics analysis

Published

2013

49. Identification of a mammalian glycerol-3-phosphate phosphatase: Role in metabolism and signaling in pancreatic β-cells and hepatocytes.

Author

Mugabo, Yves, Shangang Zhao, Seifried, Annegrit, Gezzar, Sari, Al-Mass, Anfal, Dongwei Zhang, Lamontagne, Julien, Attane, Camille, Poursharifi, Pegah, Iglesias, José, Joly, Erik, Peyot, Marie-Line, Gohla, Antje, Murthy Madiraju, S. R., and Prentki, Marc

Subjects

GLYCERIN, LIVER cells, GLYCEROLIPIDS, TYPE 2 diabetes, GLYCOLYSIS, GLUCONEOGENESIS

Abstract

Obesity, and the associated disturbed glycerolipid/fatty acid (GL/FA) cycle, contribute to insulin resistance, islet β-cell failure, and type 2 diabetes. Flux through the GL/FA cycle is regulated by the availability of glycerol-3-phosphate (Gro3P) and fatty acyl-CoA. We describe here amammalian Gro3P phosphatase (G3PP), which was not known to exist in mammalian cells, that can directly hydrolyze Gro3P to glycerol. We identified that mammalian phosphoglycolate phosphatase, with an uncertain function, acts in fact as a G3PP. We found that G3PP, by controlling Gro3P levels, regulates glycolysis and glucose oxidation, cellular redox and ATP production, gluconeogenesis, glycerolipid synthesis, and fatty acid oxidation in pancreatic islet β-cells and hepatocytes, and that glucose stimulated insulin secretion and the response tometabolic stress, e.g., glucolipotoxicity, in β-cells. In vivo overexpression of G3PP in rat liver lowers body weight gain and hepatic glucose production from glycerol and elevates plasma HDL levels. G3PP is expressed at various levels in different tissues, and its expression varies according to the nutritional state in some tissues. As Gro3P lies at the crossroads of glucose, lipid, and energy metabolism, control of its availability by G3PP adds a key level of metabolic regulation in mammalian cells, and G3PP offers a potential target for type 2 diabetes and cardiometabolic disorders. [ABSTRACT FROM AUTHOR]

Published

2016

50. Requirements of calcium fluxes and ERK kinase activation for glucose- and interleukin-1β-induced β-cell apoptosis.

Author

Hongqiang Fei, Bin Zhao, Shangang Zhao, and Qin Wang

Abstract

Abstract  Increasing evidence indicates that β-cell apoptosis and impaired secretory function were partly mediated by interleukin (IL)-1β and/or high-glucose-induced β-cell production of IL-1β. However, the specific signal transduction pathways and molecular events involved in β-cell dysfunction remain largely unresolved. In this study, we investigated whether Ca2+ and extracellular signal-regulated kinase (ERK) activation plays a role for IL-1β action in rat islets. Exposure of rat islets for 4 days to 33.3 mM glucose and 140 ng/ml IL-1β- induced β-cell apoptosis and impaired glucose-stimulated insulin secretion. By Western blotting with phosphospecific antibodies, glucose and IL-1β were shown to activate ERK. Ca2+ channel blocker nimodipine or ERK inhibitor PD98059 prevented glucose- and IL-1β-induced ERK activation, β-cell apoptosis, and impaired function. Furthermore, treatment with Ca2+ ionophore ionomycin, or exposure to thapsigargin, an inhibitor of sarco(endo)plasmic reticulum Ca2+ ATPase, all caused an amplification of IL-1β-induced ERK activation in rat islet. On the other hand, a chelator of intracellular free Ca2+ [bis-(o-aminophenoxy)-N,N,N′,N′-tetraacetic acid-acetoxymethyl] (BAPTA/AM) and an inhibitor of calmodulin (W7) diminished IL-1β-induced phosphorylation of ERK. Finally, islet release of IL-1β in response to high glucose could be abrogated by nimodipine, mibefradil, or PD98059. Together, these data suggest that glucose- and IL-1β-induced β-cell secretory dysfunction and apoptosis are Ca2+ influx and ERK dependent in rat islets. [ABSTRACT FROM AUTHOR]

Published

2008