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1. TET3 plays a critical role in white adipose development and diet-induced remodeling.

Author

Jung, Byung Chul, You, Dongjoo, Lee, Ikjun, Li, Daofeng, Schill, Rebecca, Ma, Katherine, Pi, Anna, Song, Zehan, Mu, Wei-Chieh, Wang, Ting, MacDougald, Ormond, Banks, Alexander, and Kang, Sona

Subjects
CP: Metabolism, CP: Molecular biology, DNA demethylation, TET3, adipocyte expansion, adipocyte precursor cells, adipocytes, adipogenesis, epigenetics, Animals, Humans, Mice, Adipocytes, Adipogenesis, Adipose Tissue, Adipose Tissue, White, Cell Differentiation, Diet, Dioxygenases, Obesity, PPAR gamma
Abstract

Maintaining healthy adipose tissue is crucial for metabolic health, requiring a deeper understanding of adipocyte development and response to high-calorie diets. This study highlights the importance of TET3 during white adipose tissue (WAT) development and expansion. Selective depletion of Tet3 in adipose precursor cells (APCs) reduces adipogenesis, protects against diet-induced adipose expansion, and enhances whole-body metabolism. Transcriptomic analysis of wild-type and Tet3 knockout (KO) APCs unveiled TET3 target genes, including Pparg and several genes linked to the extracellular matrix, pivotal for adipogenesis and remodeling. DNA methylation profiling and functional studies underscore the importance of DNA demethylation in gene regulation. Remarkably, targeted DNA demethylation at the Pparg promoter restored its transcription. In conclusion, TET3 significantly governs adipogenesis and diet-induced adipose expansion by regulating key target genes in APCs.

Published
2023

2. AIFM2 Is Required for High-Intensity Aerobic Exercise in Promoting Glucose Utilization.

Author

You, Dongjoo, Lin, Frances, Yi, Danielle, Pi, Anna, Ma, Katherine, Jung, Sunhee, Park, Sang-Hee, Nguyen, Hai, Villivalam, Sneha, Sul, Hei, Kang, Sona, Jang, Cholsoon, and Jung, Byung Chul

Subjects
Animals, Glucose, Glycolysis, Mice, Microtubule-Associated Proteins, Muscle, Skeletal, NAD, NADH Dehydrogenase, Tamoxifen
Abstract

Skeletal muscle is a major regulator of glycemic control at rest, and glucose utilization increases drastically during exercise. Sustaining a high glucose utilization via glycolysis requires efficient replenishment of NAD+ in the cytosol. Apoptosis-inducing mitochondrion-associated factor 2 (AIFM2) was previously shown to be a NADH oxidoreductase domain-containing flavoprotein that promotes glycolysis for diet and cold-induced thermogenesis. Here, we find that AIFM2 is selectively and highly induced in glycolytic extensor digitorum longus (EDL) muscle during exercise. Overexpression (OE) of AIFM2 in myotubes is sufficient to elevate the NAD+-to-NADH ratio, increasing the glycolytic rate. Thus, OE of AIFM2 in skeletal muscle greatly increases exercise capacity, with increased glucose utilization. Conversely, muscle-specific Aifm2 depletion via in vivo transfection of hairpins against Aifm2 or tamoxifen-inducible haploinsufficiency of Aifm2 in muscles decreases exercise capacity and glucose utilization in mice. Moreover, muscle-specific introduction of NDE1, Saccharomyces cerevisiae external NADH dehydrogenase (NDE), ameliorates impairment in glucose utilization and exercise intolerance of the muscle-specific Aifm2 haploinsufficient mice. Together, we show a novel role for AIFM2 as a critical metabolic regulator for efficient utilization of glucose in glycolytic EDL muscles.

Published
2022

3. The glucocorticoid receptor represses, whereas C/EBPβ can enhance or repress CYP26A1 transcription.

Author

Yoo, Hong Sik, Rodriguez, Adrienne, You, Dongjoo, Lee, Rebecca A, Cockrum, Michael A, Grimes, Jack A, Wang, Jen-Chywan, Kang, Sona, and Napoli, Joseph L

Subjects
Biochemistry, Biological sciences, Molecular biology, Genetics, Metabolic and endocrine
Abstract

Retinoic acid (RA) counters insulin's metabolic actions. Insulin reduces liver RA biosynthesis by exporting FoxO1 from nuclei. RA induces its catabolism, catalyzed by CYP26A1. A CYP26A1 contribution to RA homeostasis with changes in energy status had not been investigated. We found that glucagon, cortisol, and dexamethasone decrease RA-induced CYP26A1 transcription, thereby reducing RA oxidation during fasting. Interaction between the glucocorticoid receptor and the RAR/RXR coactivation complex suppresses CYP26A1 expression, increasing RA's elimination half-life. Interaction between CCAAT-enhancer-binding protein beta (C/EBPβ) and the major allele of SNP rs2068888 enhances CYP26A1 expression; the minor allele restricts the C/EBPβ effect on CYP26A1. The major and minor alleles associate with impaired human health or reduction in blood triglycerides, respectively. Thus, regulating CYP26A1 transcription contributes to adapting RA to coordinate energy availability with metabolism. These results enhance insight into CYP26A1 effects on RA during changes in energy status and glucocorticoid receptor modification of RAR-regulated gene expression.

Published
2022

4. Epigenetic regulation of inflammatory factors in adipose tissue

Author

Jung, Byung Chul and Kang, Sona

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Genetics, Biological Sciences, Diabetes, Nutrition, Obesity, Human Genome, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Metabolic and endocrine, Adipose Tissue, Animals, Epigenesis, Genetic, Humans, Inflammation, Adipose tissue, Epigenetics, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

Obesity is a strong risk factor for insulin resistance. Chronic low-grade tissue inflammation and systemic inflammation have been proposed as major mechanisms that promote insulin resistance in obesity. Adipose tissue has been recognized as a nexus between inflammation and metabolism, but how exactly inflammatory gene expression is orchestrated during the development of obesity is not well understood. Epigenetic modifications are defined as heritable changes in gene expression and cellular function without changes to the original DNA sequence. The major epigenetic mechanisms include DNA methylation, histone modification, noncoding RNAs, nucleopositioning/remodeling and chromatin reorganization. Epigenetic mechanisms provide a critical layer of gene regulation in response to environmental changes. Accumulating evidence supports that epigenetics plays a large role in the regulation of inflammatory genes in adipocytes and adipose-resident immune cell types. This review focuses on the association between adipose tissue inflammation in obesity and major epigenetic modifications.

Published
2021

5. JMJD8 is a Novel Molecular Nexus Between Adipocyte-Intrinsic Inflammation and Insulin Resistance.

Author

You, Dongjoo, Chul Jung, Byung, Villivalam, Sneha, Lim, Hee-Woong, and Kang, Sona

Abstract

Chronic low-grade inflammation, often referred to as metainflammation, develops in response to overnutrition and is a major player in the regulation of insulin sensitivity. While many studies have investigated adipose tissue inflammation from the perspective of the immune cell compartment, little is known about how adipocytes intrinsically contribute to metainflammation and insulin resistance at the molecular level. Here, we demonstrate a novel role for Jumonji C Domain Containing Protein 8 (JMJD8) as an adipocyte-intrinsic molecular nexus between inflammation and insulin resistance. We determined that JMJD8 was highly enriched in white adipose tissue, especially in the adipocyte fraction. Adipose JMJD8 levels were dramatically increased in obesity-associated insulin resistance models. Its levels were increased by feeding and insulin, and inhibited by fasting. A JMJD8 gain of function was sufficient to drive insulin resistance, whereas loss of function improved insulin sensitivity in mouse and human adipocytes. Consistent with this, Jmjd8-ablated mice had increased whole-body and adipose insulin sensitivity and glucose tolerance on both chow and a high-fat diet, while adipocyte-specific Jmjd8-overexpressing mice displayed worsened whole-body metabolism on a high-fat diet. We found that JMJD8 affected the transcriptional regulation of inflammatory genes. In particular, it was required for LPS-mediated inflammation and insulin resistance in adipocytes. For this, JMJD8 required Interferon Regulatory Factor (IRF3) to mediate its actions in adipocytes. Together, our results demonstrate that JMJD8 acts as a novel molecular factor that drives adipocyte inflammation in conjunction with insulin sensitivity.

Published
2021

6. A necessary role of DNMT3A in endurance exercise by suppressing ALDH1L1-mediated oxidative stress.

Author

Damal Villivalam, Sneha, Ebert, Scott, Lim, Hee, Kim, Jinse, You, Dongjoo, Jung, Byung, Palacios, Hector, Tcheau, Tabitha, Adams, Christopher, and Kang, Sona

Subjects
DNA methylation, exercise, oxidative stress, Animals, Cell Line, DNA (Cytosine-5-)-Methyltransferases, DNA Methyltransferase 3A, Gene Expression Profiling, Gene Knockout Techniques, Mice, Mitochondria, Muscle, Muscle, Skeletal, Oxidative Stress, Oxidoreductases Acting on CH-NH Group Donors, Physical Endurance, Rats, Reactive Oxygen Species, Sequence Analysis, RNA
Abstract

Exercise can alter the skeletal muscle DNA methylome, yet little is known about the role of the DNA methylation machinery in exercise capacity. Here, we show that DNMT3A expression in oxidative red muscle increases greatly following a bout of endurance exercise. Muscle-specific Dnmt3a knockout mice have reduced tolerance to endurance exercise, accompanied by reduction in oxidative capacity and mitochondrial respiration. Moreover, Dnmt3a-deficient muscle overproduces reactive oxygen species (ROS), the major contributors to muscle dysfunction. Mechanistically, we show that DNMT3A suppresses the Aldh1l1 transcription by binding to its promoter region, altering its epigenetic profile. Forced expression of ALDH1L1 elevates NADPH levels, which results in overproduction of ROS by the action of NADPH oxidase complex, ultimately resulting in mitochondrial defects in myotubes. Thus, inhibition of ALDH1L1 pathway can rescue oxidative stress and mitochondrial dysfunction from Dnmt3a deficiency in myotubes. Finally, we show that in vivo knockdown of Aldh1l1 largely rescues exercise intolerance in Dnmt3a-deficient mice. Together, we establish that DNMT3A in skeletal muscle plays a pivotal role in endurance exercise by controlling intracellular oxidative stress.

Published
2021

7. The role of striated muscle Pik3r1 in glucose and protein metabolism following chronic glucocorticoid exposure.

Author

Chen, Tzu-Chieh, Kuo, Taiyi, Dandan, Mohamad, Lee, Rebecca A, Chang, Maggie, Villivalam, Sneha D, Liao, Szu-Chi, Costello, Damian, Shankaran, Mahalakshmi, Mohammed, Hussein, Kang, Sona, Hellerstein, Marc K, and Wang, Jen-Chywan

Subjects
Animals, Mice, Knockout, Mice, Muscular Atrophy, Insulin Resistance, Disease Models, Animal, Insulin, Glucose, Glucocorticoids, Signal Transduction, Male, Proto-Oncogene Proteins c-akt, Muscle, Striated, Muscle Fibers, Skeletal, Class Ia Phosphatidylinositol 3-Kinase, Pik3r1, glucocorticoid receptor, glucocorticoids, insulin resistance, protein synthesis, skeletal muscle, striated muscle, Diabetes, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Musculoskeletal, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology
Abstract

Chronic glucocorticoid exposure causes insulin resistance and muscle atrophy in skeletal muscle. We previously identified phosphoinositide-3-kinase regulatory subunit 1 (Pik3r1) as a primary target gene of skeletal muscle glucocorticoid receptors involved in the glucocorticoid-mediated suppression of insulin action. However, the in vivo functions of Pik3r1 remain unclear. Here, we generated striated muscle-specific Pik3r1 knockout (MKO) mice and treated them with a dexamethasone (DEX), a synthetic glucocorticoid. Treating wildtype (WT) mice with DEX attenuated insulin activated Akt activity in liver, epididymal white adipose tissue, and gastrocnemius (GA) muscle. This DEX effect was diminished in GA muscle of MKO mice, therefore, resulting in improved glucose and insulin tolerance in DEX-treated MKO mice. Stable isotope labeling techniques revealed that in WT mice, DEX treatment decreased protein fractional synthesis rates in GA muscle. Furthermore, histology showed that in WT mice, DEX treatment reduced GA myotube diameters. In MKO mice, myotube diameters were smaller than in WT mice, and there were more fast oxidative fibers. Importantly, DEX failed to further reduce myotube diameters. Pik3r1 knockout also decreased basal protein synthesis rate (likely caused by lower 4E-BP1 phosphorylation at Thr37/Thr46) and curbed the ability of DEX to attenuate protein synthesis rate. Finally, the ability of DEX to inhibit eIF2α phosphorylation and insulin-induced 4E-BP1 phosphorylation was reduced in MKO mice. Taken together, these results demonstrate the role of Pik3r1 in glucocorticoid-mediated effects on glucose and protein metabolism in skeletal muscle.

Published
2021

8. TET1 is a beige adipocyte-selective epigenetic suppressor of thermogenesis.

Author

Damal Villivalam, Sneha, You, Dongjoo, Kim, Jinse, Lim, Hee Woong, Xiao, Han, Zushin, Pete-James H, Oguri, Yasuo, Amin, Pouya, and Kang, Sona

Abstract

It has been suggested that beige fat thermogenesis is tightly controlled by epigenetic regulators that sense environmental cues such as temperature. Here, we report that subcutaneous adipose expression of the DNA demethylase TET1 is suppressed by cold and other stimulators of beige adipocyte thermogenesis. TET1 acts as an autonomous repressor of key thermogenic genes, including Ucp1 and Ppargc1a, in beige adipocytes. Adipose-selective Tet1 knockout mice generated by using Fabp4-Cre improves cold tolerance and increases energy expenditure and protects against diet-induced obesity and insulin resistance. Moreover, the suppressive role of TET1 in the thermogenic gene regulation of beige adipocytes is largely DNA demethylase-independent. Rather, TET1 coordinates with HDAC1 to mediate the epigenetic changes to suppress thermogenic gene transcription. Taken together, TET1 is a potent beige-selective epigenetic breaker of the thermogenic gene program. Our findings may lead to a therapeutic strategy to increase energy expenditure in obesity and related metabolic disorders.

Published
2020

9. The role of DNA methylation in thermogenic adipose biology

Author

Xiao, Han and Kang, Sona

Subjects
Biochemistry and Cell Biology, Biological Sciences, Obesity, Diabetes, Nutrition, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Adipose Tissue, Beige, Adipose Tissue, Brown, Animals, DNA Methylation, Epigenesis, Genetic, Gene Expression Regulation, Gene Regulatory Networks, Humans, Thermogenesis, Epigenetics, DNA methylation, brown adipocytes, beige adipocytes, obesity, type 2 diabetes, Medical Biochemistry and Metabolomics, Developmental Biology, Biochemistry and cell biology
Abstract

The two types of thermogenic fat cells, beige and brown adipocytes, play a significant role in regulating energy homeostasis. Their development and thermogenesis are tightly regulated by dynamic epigenetic mechanisms, which could potentially be targeted to treat metabolic disorders such as obesity. However, we are just beginning to catalog and understand these dynamic changes. In this review, we will discuss the current understanding of the role of DNA (de)methylation events in beige and brown adipose biology in order to highlight the holes in our knowledge and to point the way forward for future studies.

Published
2019

10. Functional Implications of DNA Methylation in Adipose Biology

Author

Ma, Xiang and Kang, Sona

Subjects
Biomedical and Clinical Sciences, Diabetes, Biotechnology, Nutrition, Human Genome, Obesity, Genetics, 1.1 Normal biological development and functioning, Aetiology, Underpinning research, 2.1 Biological and endogenous factors, Metabolic and endocrine, Cardiovascular, Adipose Tissue, Adiposity, Animals, DNA Methylation, Epigenesis, Genetic, Humans, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences
Abstract

The twin epidemics of obesity and type 2 diabetes (T2D) are a serious health, social, and economic issue. The dysregulation of adipose tissue biology is central to the development of these two metabolic disorders, as adipose tissue plays a pivotal role in regulating whole-body metabolism and energy homeostasis (1). Accumulating evidence indicates that multiple aspects of adipose biology are regulated, in part, by epigenetic mechanisms. The precise and comprehensive understanding of the epigenetic control of adipose tissue biology is crucial to identifying novel therapeutic interventions that target epigenetic issues. Here, we review the recent findings on DNA methylation events and machinery in regulating the developmental processes and metabolic function of adipocytes. We highlight the following points: 1) DNA methylation is a key epigenetic regulator of adipose development and gene regulation, 2) emerging evidence suggests that DNA methylation is involved in the transgenerational passage of obesity and other metabolic disorders, 3) DNA methylation is involved in regulating the altered transcriptional landscape of dysfunctional adipose tissue, 4) genome-wide studies reveal specific DNA methylation events that associate with obesity and T2D, and 5) the enzymatic effectors of DNA methylation have physiological functions in adipose development and metabolic function.

Published
2019

11. TET2 facilitates PPARγ agonist–mediated gene regulation and insulin sensitization in adipocytes

Author

Bian, Fuyun, Ma, Xiang, Villivalam, Sneha Damal, You, Dongjoo, Choy, Lauren Raquel, Paladugu, Anushka, Fung, Sarah, and Kang, Sona

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Obesity, Human Genome, Nutrition, Biotechnology, Genetics, Diabetes, Aetiology, Underpinning research, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Metabolic and endocrine, 3T3-L1 Cells, Adipocytes, Animals, DNA Methylation, DNA-Binding Proteins, Diet, High-Fat, Dioxygenases, Epigenesis, Genetic, Gene Expression Regulation, Glucose, Insulin Resistance, Mice, Mice, Inbred C57BL, PPAR gamma, Polymerase Chain Reaction, Proto-Oncogene Proteins, Signal Transduction, Insulin sensitivity, Epigenetics, DNA demethylation, TET proteins, Endocrinology & Metabolism, Clinical sciences
Abstract

Emerging evidence indicates that epigenetic mechanisms like DNA methylation directly contribute to metabolic regulation. For example, we previously demonstrated that de novo DNA methyltransferase Dnmt3a plays a causal role in the development of adipocyte insulin resistance. Recent studies suggest that DNA demethylation plays an important role in the developmental process of adipocytes. However, little is known about whether DNA demethylase ten-eleven translocation (TET) proteins regulate the metabolic functions of adipocytes.MethodsThe expression of Tet genes was assessed in the fractionated adipocytes of chow- and high fat diet-fed C57/Bl6 mice using qPCR and western blotting. The effect of Tet2 gain- or loss-of-function in fully mature 3T3-L1 adipocytes in the presence/absence of Rosiglitazone (Rosi) and TNF-α on insulin sensitivity was using the insulin-stimulated glucose uptake and insulin signaling assays. Gene expression and DNA methylation analyses of PPARγ target genes was performed in the same setting. In addition, PPARγ reporter assays, co-immunoprecipitation assays, PPARγ ChIP-PCR analyses were performed.ResultsWe found that adipose expression of TET2, alone among its family members, was significantly reduced in diet-induced insulin resistance. TET2 gain-of-function was sufficient to promote insulin sensitivity while loss-of-function was necessary to facilitate insulin sensitization in response to the PPARγ agonist Rosiglitazone (Rosi) in cultured adipocytes. Consistent with this, TET2 was required for Rosi-dependent gene activation of certain PPARγ targets accompanied by changes in DNA demethylation at the promoter regions. Furthermore, TET2 was necessary to sustain PPARγ binding to target loci upon activation with Rosi via physical interaction with PPARγ.ConclusionsOur data demonstrate that TET2 works as an epigenetic regulator of Rosi-mediated insulin sensitization and transcriptional regulation in adipocytes.

Published
2018

13. Dnmt3a is an epigenetic mediator of adipose insulin resistance.

Author

You, Dongjoo, Nilsson, Emma, Tenen, Danielle E, Lyubetskaya, Anna, Lo, James C, Jiang, Rencong, Deng, Jasmine, Dawes, Brian A, Vaag, Allan, Ling, Charlotte, Rosen, Evan D, and Kang, Sona

Subjects
Cells, Cultured, Adipocytes, Animals, Mice, Knockout, Humans, Mice, Insulin Resistance, Gene Expression Profiling, Epigenesis, Genetic, DNA (Cytosine-5-)-Methyltransferases, adipocyte, cell biology, epigenetic, insulin resistance, mouse, Cells, Cultured, Knockout, Epigenesis, Genetic, Genetics, Nutrition, Obesity, Diabetes, 2.1 Biological and endogenous factors, Metabolic and Endocrine, Biochemistry and Cell Biology
Abstract

Insulin resistance results from an intricate interaction between genetic make-up and environment, and thus may be orchestrated by epigenetic mechanisms like DNA methylation. Here, we demonstrate that DNA methyltransferase 3a (Dnmt3a) is both necessary and sufficient to mediate insulin resistance in cultured mouse and human adipocytes. Furthermore, adipose-specific Dnmt3a knock-out mice are protected from diet-induced insulin resistance and glucose intolerance without accompanying changes in adiposity. Unbiased gene profiling studies revealed Fgf21 as a key negatively regulated Dnmt3a target gene in adipocytes with concordant changes in DNA methylation at the Fgf21 promoter region. Consistent with this, Fgf21 can rescue Dnmt3a-mediated insulin resistance, and DNA methylation at the FGF21 locus was elevated in human subjects with diabetes and correlated negatively with expression of FGF21 in human adipose tissue. Taken together, our data demonstrate that adipose Dnmt3a is a novel epigenetic mediator of insulin resistance in vitro and in vivo.

Published
2017

14. Exploration of Underlying Mechanism of Anti-adipogenic Activity of Sulfuretin.

Author

Lamichhane, Ramakanta, Kim, Se-Gun, Kang, Sona, Lee, Kyung-Hee, Pandeya, Prakash Raj, and Jung, Hyun-Ju

Subjects
Adipose Tissue, 3T3-L1 Cells, Adipocytes, Animals, Mice, Rhus, Obesity, Benzofurans, Flavonoids, DNA-Binding Proteins, CCAAT-Enhancer-Binding Proteins, PPAR gamma, Transcription Factors, Anti-Obesity Agents, Plant Extracts, Phytotherapy, Gene Expression, Adipogenesis, beta Catenin, Sterol Regulatory Element Binding Protein 1, adipogenic transcription factor, anti-adipogenesis, oil-red-O, sulfuretin, Pharmacology and Pharmaceutical Sciences, Medicinal and Biomolecular Chemistry, Plant Biology, Pharmacology & Pharmacy
Abstract

Sulfuretin is a natural flavonoid found in the plant Rhus verniciflua STOKES. The plant has been traditionally used as medicinal agent for antiviral, cathartic, diaphoretic, anti-rheumatic and sedative activities in East Asia. In this study we isolated and identified sulfuretin from R. verniciflua and investigated its anti-adipogenic activity against 3T3-L1 preadipocytes cells. We evaluated the effects of sulfuretin on the adipogenic transcription factors like peroxisome proliferator-activated receptor γ (PPARγ), CCAAT/enhancer-binding protein α (C/EBPα), fatty acid synthase (FAS), Fabp4, adiponectin and zinc fingerprint protein (Zfp) 521 by gene expression (real-time QPCR) and Western blot analysis. Sulfuretin treatment at Day 0 and 2 showed significant reduction of lipid production in 3T3-L1 cells in concentration dependent manner. Gene expression analysis (real-time PCR) revealed that sulfuretin inhibited the both major adipogenic factors (C/EBPα, C/EBPβ and PPARγ) and minor adipogenic factors (sterol regulatory element-binding protein (SREBP1c), adiponectin, FAS, Fabp4, Zfp423, and Ebf1). Western blot analysis showed the increased expression of β-catenin and suppression of PPARγ after sulfuretin treatment. Overall, sulfuretin is a natural flavonoid having potent anti-adipogenic activity through the suppression of major adipogenic factors C/EBPα, C/EBPβ and PPARγ, which initiate adipogenesis.

Published
2017

17. IRF3 promotes adipose inflammation and insulin resistance and represses browning

Author

Kumari, Manju, Wang, Xun, Lantier, Louise, Lyubetskaya, Anna, Eguchi, Jun, Kang, Sona, Tenen, Danielle, Roh, Hyun Cheol, Kong, Xingxing, Kazak, Lawrence, Ahmad, Rasheed, and Rosen, Evan D.

Subjects
Adipose tissues -- Growth -- Genetic aspects, Cellular signal transduction -- Genetic aspects -- Health aspects, Transcription factors -- Properties, Company growth, Health care industry
Abstract

The chronic inflammatory state that accompanies obesity is a major contributor to insulin resistance and other dysfunctional adaptations in adipose tissue. Cellular and secreted factors promote the inflammatory milieu of obesity, but the transcriptional pathways that drive these processes are not well described. Although the canonical inflammatory transcription factor NF-κB is considered to be the major driver of adipocyte inflammation, members of the interferon regulatory factor (IRF) family may also play a role in this process. Here, we determined that IRF3 expression is upregulated in the adipocytes of obese mice and humans. Signaling through TLR3 and TLR4, which lie upstream of IRF3, induced insulin resistance in murine adipocytes, while IRF3 knockdown prevented insulin resistance. Furthermore, improved insulin sensitivity in IRF3-deficient mice was associated with reductions in intra-adipose and systemic inflammation in the high fat-fed state, enhanced browning of subcutaneous fat, and increased adipose expression of GLUT4. Taken together, the data indicate that IRF3 is a major transcriptional regulator of adipose inflammation and is involved in maintaining systemic glucose and energy homeostasis., Introduction One of the major concepts emerging from the last 2 decades of metabolism research is the notion of 'metainflammation,' the state of chronic low-grade inflammation that develops during periods [...]

Published
2016
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20. AIFM2 Is Required for High-Intensity Aerobic Exercise in Promoting Glucose Utilization.

Author

Nguyen, Hai P., Villivalam, Sneha Damal, Jung, Byung Chul, You, Dongjoo, Lin, Frances, Yi, Danielle, Pi, Anna, Ma, Katherine, Jung, Sunhee, Park, Sang-Hee, Jang, Cholsoon, Sul, Hei Sook, and Kang, Sona

Abstract

Skeletal muscle is a major regulator of glycemic control at rest, and glucose utilization increases drastically during exercise. Sustaining a high glucose utilization via glycolysis requires efficient replenishment of NAD+ in the cytosol. Apoptosis-inducing mitochondrion-associated factor 2 (AIFM2) was previously shown to be a NADH oxidoreductase domain-containing flavoprotein that promotes glycolysis for diet and cold-induced thermogenesis. Here, we find that AIFM2 is selectively and highly induced in glycolytic extensor digitorum longus (EDL) muscle during exercise. Overexpression (OE) of AIFM2 in myotubes is sufficient to elevate the NAD+-to-NADH ratio, increasing the glycolytic rate. Thus, OE of AIFM2 in skeletal muscle greatly increases exercise capacity, with increased glucose utilization. Conversely, muscle-specific Aifm2 depletion via in vivo transfection of hairpins against Aifm2 or tamoxifen-inducible haploinsufficiency of Aifm2 in muscles decreases exercise capacity and glucose utilization in mice. Moreover, muscle-specific introduction of NDE1, Saccharomyces cerevisiae external NADH dehydrogenase (NDE), ameliorates impairment in glucose utilization and exercise intolerance of the muscle-specific Aifm2 haploinsufficient mice. Together, we show a novel role for AIFM2 as a critical metabolic regulator for efficient utilization of glucose in glycolytic EDL muscles. [ABSTRACT FROM AUTHOR]

Published
2022
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23. The role of striated muscle Pik3r1 in glucose and protein metabolism following chronic glucocorticoid exposure

Author

Chen, Tzu-Chieh, primary, Kuo, Taiyi, additional, Dandan, Mohamad, additional, Lee, Rebecca A., additional, Chang, Maggie, additional, Villivalam, Sneha D., additional, Liao, Szu-Chi, additional, Costello, Damian, additional, Shankaran, Mahalakshmi, additional, Mohammed, Hussein, additional, Kang, Sona, additional, Hellerstein, Marc K., additional, and Wang, Jen-Chywan, additional

Published
2021
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28. JMJD8 Is a Novel Molecular Nexus Between Adipocyte-Intrinsic Inflammation and Insulin Resistance.

Author

You, Dongjoo, Jung, Byung Chul, Villivalam, Sneha Damal, Lim, Hee-Woong, and Kang, Sona

Subjects
WHITE adipose tissue, INSULIN resistance, INSULIN regulation, INSULIN sensitivity, INTERFERON regulatory factors
Abstract

Chronic low-grade inflammation, often referred to as metainflammation, develops in response to overnutrition and is a major player in the regulation of insulin sensitivity. While many studies have investigated adipose tissue inflammation from the perspective of the immune cell compartment, little is known about how adipocytes intrinsically contribute to metainflammation and insulin resistance at the molecular level. In this study, we demonstrate a novel role for Jumonji C domain-containing protein 8 (JMJD8) as an adipocyte-intrinsic molecular nexus between inflammation and insulin resistance. We determined that JMJD8 was highly enriched in white adipose tissue, especially in the adipocyte fraction. Adipose JMJD8 levels were dramatically increased in obesity-associated insulin resistance models. Its levels were increased by feeding and insulin and inhibited by fasting. A JMJD8 gain-of-function was sufficient to drive insulin resistance, whereas loss-of-function improved insulin sensitivity in mouse and human adipocytes. Consistent with this, Jmjd8-ablated mice had increased whole-body and adipose insulin sensitivity and glucose tolerance on both chow and a high-fat diet, while adipocyte-specific Jmjd8-overexpressing mice displayed worsened whole-body metabolism on a high-fat diet. We found that JMJD8 affected the transcriptional regulation of inflammatory genes. In particular, it was required for lipopolysaccharide-mediated inflammation and insulin resistance in adipocytes. For this, JMJD8 required interferon regulatory factor 3 to mediate its actions in adipocytes. Together, our results demonstrate that JMJD8 acts as a novel molecular factor that drives adipocyte inflammation in conjunction with insulin sensitivity. [ABSTRACT FROM AUTHOR]

Published
2022
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30. Wnt10b Inhibits Obesity in ob/ob and Agouti Mice

Author

Wright, Wendy S., Longo, Kenneth A., Dolinsky, Vernon W., Gerin, Isabelle, Kang, Sona, Bennett, Christina N., Chiang, Shian-Huey, Prestwich, Tyler C., Gress, Catherine, Burant, Charles F., Susulic, Vedrana S., and MacDougald, Ormond A.

Published
2007

33. Dnmt3a is an epigenetic mediator of adipose insulin resistance

Author

You, Dongjoo, primary, Nilsson, Emma, additional, Tenen, Danielle E, additional, Lyubetskaya, Anna, additional, Lo, James C, additional, Jiang, Rencong, additional, Deng, Jasmine, additional, Dawes, Brian A, additional, Vaag, Allan, additional, Ling, Charlotte, additional, Rosen, Evan D, additional, and Kang, Sona, additional

Published
2017
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35. Functional Implications of DNA Methylation in Adipose Biology.

Author

Xiang Ma, Sona Kang, Ma, Xiang, and Kang, Sona

Subjects
DNA methylation, EPIGENOMICS, BIOLOGY, ADIPOSE tissues, TYPE 2 diabetes, METABOLIC disorders
Abstract

The twin epidemics of obesity and type 2 diabetes (T2D) are a serious health, social, and economic issue. The dysregulation of adipose tissue biology is central to the development of these two metabolic disorders, as adipose tissue plays a pivotal role in regulating whole-body metabolism and energy homeostasis (1). Accumulating evidence indicates that multiple aspects of adipose biology are regulated, in part, by epigenetic mechanisms. The precise and comprehensive understanding of the epigenetic control of adipose tissue biology is crucial to identifying novel therapeutic interventions that target epigenetic issues. Here, we review the recent findings on DNA methylation events and machinery in regulating the developmental processes and metabolic function of adipocytes. We highlight the following points: 1) DNA methylation is a key epigenetic regulator of adipose development and gene regulation, 2) emerging evidence suggests that DNA methylation is involved in the transgenerational passage of obesity and other metabolic disorders, 3) DNA methylation is involved in regulating the altered transcriptional landscape of dysfunctional adipose tissue, 4) genome-wide studies reveal specific DNA methylation events that associate with obesity and T2D, and 5) the enzymatic effectors of DNA methylation have physiological functions in adipose development and metabolic function. [ABSTRACT FROM AUTHOR]

Published
2019
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38. Identification of nuclear hormone receptor pathways causing insulin resistance by transcriptional and epigenomic analysis

Author

Kang, Sona, primary, Tsai, Linus T., additional, Zhou, Yiming, additional, Evertts, Adam, additional, Xu, Su, additional, Griffin, Michael J., additional, Issner, Robbyn, additional, Whitton, Holly J., additional, Garcia, Benjamin A., additional, Epstein, Charles B., additional, Mikkelsen, Tarjei S., additional, and Rosen, Evan D., additional

Published
2014
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40. IRF4 Is a Key Thermogenic Transcriptional Partner of PGC-1α

Author

Kong, Xingxing, primary, Banks, Alexander, additional, Liu, Tiemin, additional, Kazak, Lawrence, additional, Rao, Rajesh R., additional, Cohen, Paul, additional, Wang, Xun, additional, Yu, Songtao, additional, Lo, James C., additional, Tseng, Yu-Hua, additional, Cypess, Aaron M., additional, Xue, Ruidan, additional, Kleiner, Sandra, additional, Kang, Sona, additional, Spiegelman, Bruce M., additional, and Rosen, Evan D., additional

Published
2014
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42. Arterial territory-specific phosphorylated retinoblastoma protein species and CDK2 promote differences in the vascular smooth muscle cell response to mitogens

Author

Lange, Martin, primary, Fujikawa, Tatsuya, additional, Koulova, Anna, additional, Kang, Sona, additional, Griffin, Michael, additional, Lassaletta, Antonio, additional, Erat, Anna, additional, Tobiash, Edda, additional, Bianchi, Cesario, additional, Elmadhun, Nassrene, additional, Sellke, Frank, additional, and Usheva, Anny, additional

Published
2013
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43. Role of wnts in prostate cancer bone metastases

Author

Department of Urology, The University of Michigan, Ann Arbor, Michigan, Department of Internal Medicine, The University of Michigan, Ann Arbor, Michigan, Department of Urology, The University of Michigan, Ann Arbor, Michigan ; RM 5304 CCGCB, 1500 East Medical Center Drive, Ann Arbor, MI 48109-0940., Hall, Christopher L., Kang, Sona, MacDougald, Ormond A., Keller, Evan T., Department of Urology, The University of Michigan, Ann Arbor, Michigan, Department of Internal Medicine, The University of Michigan, Ann Arbor, Michigan, Department of Urology, The University of Michigan, Ann Arbor, Michigan ; RM 5304 CCGCB, 1500 East Medical Center Drive, Ann Arbor, MI 48109-0940., Hall, Christopher L., Kang, Sona, MacDougald, Ormond A., and Keller, Evan T.

Abstract

Prostate cancer (CaP) is unique among all cancers in that when it metastasizes to bone, it typically forms osteoblastic lesions (characterized by increased bone production). CaP cells produce many factors, including Wnts that are implicated in tumor-induced osteoblastic activity. In this prospectus, we describe our research on Wnt and the CaP bone phenotype. Wnts are cysteine-rich glycoproteins that mediate bone development in the embryo and promote bone production in the adult. Wnts have been shown to have autocrine tumor effects, such as enhancing proliferation and protecting against apoptosis. In addition, we have recently identified that CaP-produced Wnts act in a paracrine fashion to induce osteoblastic activity in CaP bone metastases. In addition to Wnts, CaP cells express the soluble Wnt inhibitor dickkopf-1 (DKK-1). It appears that DKK-1 production occurs early in the development of skeletal metastases, which results in masking of osteogenic Wnts, thus favoring osteolysis at the metastatic site. As metastases progress, DKK-1 expression decreases allowing for unmasking of Wnt's osteoblastic activity and ultimately resulting in osteosclerosis at the metastatic site. We believe that DKK-1 is one of the switches that transitions the CaP bone metastasis activity from osteolytic to osteoblastic. Wnt/DKK-1 activity fits a model of CaP-induced bone remodeling occurring in a continuum composed of an osteolytic phase, mediated by receptor activator of NFkB ligand (RANKL), parathyroid hormone-related protein (PTHRP) and DKK-1; a transitional phase, where environmental alterations promote expression of osteoblastic factors (Wnts) and decreases osteolytic factors (i.e., DKK-1); and an osteoblastic phase, in which tumor growth-associated hypoxia results in production of vascular endothelial growth factor and endothelin-1, which have osteoblastic activity. This model suggests that targeting both osteolytic activity and osteoblastic activity will provide efficacy for therap

Published
2007

44. Effects of Wnt signaling on brown adipocyte differentiation and metabolism mediated by PGC-1alpha.

Author

Kang, Sona, Bajnok, Laszlo, Longo, Kenneth A, Petersen, Rasmus K, Hansen, Jacob B, Kristiansen, Karsten, MacDougald, Ormond A, Kang, Sona, Bajnok, Laszlo, Longo, Kenneth A, Petersen, Rasmus K, Hansen, Jacob B, Kristiansen, Karsten, and MacDougald, Ormond A

Abstract

Udgivelsesdato: 2005-Feb, Activation of canonical Wnt signaling inhibits brown adipogenesis of cultured cells by impeding induction of PPARgamma and C/EBPalpha. Although enforced expression of these adipogenic transcription factors restores lipid accumulation and expression of FABP4 in Wnt-expressing cells, additional expression of PGC-1alpha is required for activation of uncoupling protein 1 (UCP1). Wnt10b blocks brown adipose tissue development and expression of UCP1 when expressed from the fatty acid binding protein 4 promoter, even when mice are administered a beta3-agonist. In differentiated brown adipocytes, activation of Wnt signaling suppresses expression of UCP1 through repression of PGC-1alpha. Consistent with these in vitro observations, UCP1-Wnt10b transgenic mice, which express Wnt10b in interscapular tissue, lack functional brown adipose tissue. While interscapular tissue of UCP1-Wnt10b mice lacks expression of PGC-1alpha and UCP1, the presence of unilocular lipid droplets and expression of white adipocyte genes suggest conversion of brown adipose tissue to white. Reciprocal expression of Wnt10b with UCP1 and PGC-1alpha in interscapular tissue from cold-challenged or genetically obese mice provides further evidence for regulation of brown adipocyte metabolism by Wnt signaling. Taken together, these data suggest that activation of canonical Wnt signaling early in differentiation blocks brown adipogenesis, whereas activating Wnt signaling in mature brown adipocytes stimulates their conversion to white adipocytes.

Published
2005

45. Regulation of Early Adipose Commitment by Zfp521

Author

Kang, Sona, primary, Akerblad, Peter, additional, Kiviranta, Riku, additional, Gupta, Rana K., additional, Kajimura, Shingo, additional, Griffin, Michael J., additional, Min, Jie, additional, Baron, Roland, additional, and Rosen, Evan D., additional

Published
2012
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46. Mammalian Stem Cells Reprogramming in Response to Terahertz Radiation

Author

Bock, Jonathan, primary, Fukuyo, Yayoi, additional, Kang, Sona, additional, Phipps, M. Lisa, additional, Alexandrov, Ludmil B., additional, Rasmussen, Kim Ø., additional, Bishop, Alan R., additional, Rosen, Evan D., additional, Martinez, Jennifer S., additional, Chen, Hou-Tong, additional, Rodriguez, George, additional, Alexandrov, Boian S., additional, and Usheva, Anny, additional

Published
2010
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49. Identification of nuclear hormone receptor pathways causing insulin resistance by transcriptional and epigenomic analysis.

Author

Kang, Sona, Tsai, Linus T., Zhou, Yiming, Evertts, Adam, Xu, Su, Griffin, Michael J., Issner, Robbyn, Whitton, Holly J., Garcia, Benjamin A., Epstein, Charles B., Mikkelsen, Tarjei S., and Rosen, Evan D.

Subjects
*INSULIN resistance, *OBESITY, *AGING, *PHENOTYPES, *STEROIDS, *VITAMIN D receptors
Abstract

Insulin resistance is a cardinal feature of Type 2 diabetes (T2D) and a frequent complication of multiple clinical conditions, including obesity, ageing and steroid use, among others. How such a panoply of insults can result in a common phenotype is incompletely understood. Furthermore, very little is known about the transcriptional and epigenetic basis of this disorder, despite evidence that such pathways are likely to play a fundamental role. Here, we compare cell autonomous models of insulin resistance induced by the cytokine tumour necrosis factor-α or by the steroid dexamethasone to construct detailed transcriptional and epigenomic maps associated with cellular insulin resistance. These data predict that the glucocorticoid receptor and vitamin D receptor are common mediators of insulin resistance, which we validate using gain- and loss-of-function studies. These studies define a common transcriptional and epigenomic signature in cellular insulin resistance enabling the identification of pathogenic mechanisms. [ABSTRACT FROM AUTHOR]

Published
2015
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