Your search keyword '"Seung-Hoi Koo"' showing total 71 results

1. Central role of Prominin-1 in lipid rafts during liver regeneration

Author

Myeong-Suk Bahn, Dong-Min Yu, Myoungwoo Lee, Sung-Je Jo, Ji-Won Lee, Ho-Chul Kim, Hyun Lee, Hong Lim Kim, Arum Kim, Jeong-Ho Hong, Jun Seok Kim, Seung-Hoi Koo, Jae-Seon Lee, and Young-Gyu Ko

Subjects

Mice, Knockout, Mice, Membrane Microdomains, Multidisciplinary, Interleukin-6, Cytokine Receptor gp130, Animals, General Physics and Astronomy, AC133 Antigen, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Liver Regeneration

Abstract

Prominin-1, a lipid raft protein, is required for maintaining cancer stem cell properties in hepatocarcinoma cell lines, but its physiological roles in the liver have not been well studied. Here, we investigate the role of Prominin-1 in lipid rafts during liver regeneration and show that expression of Prominin-1 increases after 2/3 partial hepatectomy or CCl4 injection. Hepatocyte proliferation and liver regeneration are attenuated in liver-specific Prominin-1 knockout mice compared to wild-type mice. Detailed mechanistic studies reveal that Prominin-1 interacts with the interleukin-6 signal transducer glycoprotein 130, confining it to lipid rafts so that STAT3 signaling by IL-6 is effectively activated. The overexpression of the glycosylphosphatidylinsositol-anchored first extracellular domain of Prominin-1, which is the domain that binds to GP130, rescued the proliferation of hepatocytes and liver regeneration in liver-specific Prominin-1 knockout mice. In summary, Prominin-1 is upregulated in hepatocytes during liver regeneration where it recruits GP130 into lipid rafts and activates the IL6-GP130-STAT3 axis, suggesting that Prominin-1 might be a promising target for therapeutic applications in liver transplantation.

Published

2022

2. Role of CRTC2 in Metabolic Homeostasis: Key Regulator of Whole-Body Energy Metabolism?

Author

Yongmin Kwon, Hye Sook Han, and Seung Hoi Koo

Subjects

Crtc2 protein, mouse, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Review, 030204 cardiovascular system & hematology, CREB, lcsh:Diseases of the endocrine glands. Clinical endocrinology, CRTC2 protein, human, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Coactivator, Cyclic AMP, Medicine, Animals, Homeostasis, Cyclic adenosine monophosphate, Transcription, genetic, Metabolic Process, lcsh:RC648-665, biology, business.industry, Gluconeogenesis, Lipid metabolism, Energy metabolism, CRTC2, Cell biology, Metabolic pathway, Basic Research, chemistry, Liver, Transcription Coactivator, biology.protein, business, Transcription Factors

Abstract

Cyclic adenosine monophosphate (cAMP) signaling is critical for regulating metabolic homeostasis in mammals. In particular, transcriptional regulation by cAMP response element-binding protein (CREB) and its coactivator, CREB-regulated transcription coactivator (CRTC), is essential for controlling the expression of critical enzymes in the metabolic process, leading to more chronic changes in metabolic flux. Among the CRTC isoforms, CRTC2 is predominantly expressed in peripheral tissues and has been shown to be associated with various metabolic pathways in tissue-specific manners. While initial reports showed the physiological role of CRTC2 in regulating gluconeogenesis in the liver, recent studies have further delineated the role of this transcriptional coactivator in the regulation of glucose and lipid metabolism in various tissues, including the liver, pancreatic islets, endocrine tissues of the small intestines, and adipose tissues. In this review, we discuss recent studies that have utilized knockout mouse models to delineate the role of CRTC2 in the regulation of metabolic homeostasis.

Published

2020

3. Hepatocyte-specific Prominin-1 protects against liver injury-induced fibrosis by stabilizing SMAD7

Author

Hyun Lee, Dong-Min Yu, Myeong-Suk Bahn, Young-Jae Kwon, Min Jee Um, Seo Yeon Yoon, Ki-Tae Kim, Myoung-Woo Lee, Sung-Je Jo, Sungsoo Lee, Seung-Hoi Koo, Ki Hoon Jung, Jae-Seon Lee, and Young-Gyu Ko

Subjects

Liver Cirrhosis, Mice, Liver, Clinical Biochemistry, Hepatocytes, Molecular Medicine, Animals, AC133 Antigen, Molecular Biology, Biochemistry, Fibrosis, Smad7 Protein, Transcription Factors

Abstract

Prominin-1 (PROM1), also known as CD133, is expressed in hepatic progenitor cells (HPCs) and cholangiocytes of the fibrotic liver. In this study, we show that PROM1 is upregulated in the plasma membrane of fibrotic hepatocytes. Hepatocellular expression of PROM1 was also demonstrated in mice (Prom1CreER; R26TdTom) in which cells expressed TdTom under control of the Prom1 promoter. To understand the role of hepatocellular PROM1 in liver fibrosis, global and liver-specific Prom1-deficient mice were analyzed after bile duct ligation (BDL). BDL-induced liver fibrosis was aggravated with increased phosphorylation of SMAD2/3 and decreased levels of SMAD7 by global or liver-specific Prom1 deficiency but not by cholangiocyte-specific Prom1 deficiency. Indeed, PROM1 prevented SMURF2-induced SMAD7 ubiquitination and degradation by interfering with the molecular association of SMAD7 with SMURF2. We also demonstrated that hepatocyte-specific overexpression of SMAD7 ameliorated BDL-induced liver fibrosis in liver-specific Prom1-deficient mice. Thus, we conclude that PROM1 is necessary for the negative regulation of TGFβ signaling during liver fibrosis.

Published

2021

4. Salt-inducible kinase 1 regulates bone anabolism via the CRTC1–CREB–Id1 axis

Author

Bongjun Kim, Jun Oh Kwon, Zang Hee Lee, Min Kyung Kim, Hong-Hee Kim, Seung Hoi Koo, Haemin Kim, and Min-Kyoung Song

Subjects

Inhibitor of Differentiation Protein 1, 0301 basic medicine, Cancer Research, Anabolism, Immunology, Bone Morphogenetic Protein 2, Protein Serine-Threonine Kinases, Bone morphogenetic protein, CREB, Bone morphogenetic protein 2, Article, Anabolic Agents, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Osteoclast, medicine, Animals, Humans, lcsh:QH573-671, Cyclic AMP Response Element-Binding Protein, Protein kinase A, Mice, Knockout, Osteoblasts, biology, Chemistry, lcsh:Cytology, Gene Expression Regulation, Developmental, Osteoblast, Cell Biology, Cyclic AMP-Dependent Protein Kinases, Cell biology, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, biology.protein, Osteoporosis, Cell signalling, Transcription Factors

Abstract

New bone anabolic agents for the effective treatment of bone metabolic diseases like osteoporosis are of high clinical demand. In the present study, we reveal the function of salt-inducible kinase 1 (SIK1) in regulating osteoblast differentiation. Gene knockdown of SIK1 but not of SIK2 or SIK3 expression in primary preosteoblasts increased osteoblast differentiation and bone matrix mineralization. SIK1 also regulated the proliferation of osteoblastic precursor cells in osteogenesis. This negative control of osteoblasts required the catalytic activity of SIK1. SIK1 phosphorylated CREB regulated transcription coactivator 1 (CRTC1), preventing CRTC1 from enhancing CREB transcriptional activity for the expression of osteogenic genes like Id1. Furthermore, SIK1 knockout (KO) mice had higher bone mass, osteoblast number, and bone formation rate versus littermate wild-type (WT) mice. Preosteoblasts from SIK1 KO mice showed more osteoblastogenic potential than did WT cells, whereas osteoclast generation among KO and WT precursors was indifferent. In addition, bone morphogenic protein 2 (BMP2) suppressed both SIK1 expression as well as SIK1 activity by protein kinase A (PKA)–dependent mechanisms to stimulate osteogenesis. Taken together, our results indicate that SIK1 is a key negative regulator of preosteoblast proliferation and osteoblast differentiation and that the repression of SIK1 is crucial for BMP2 signaling for osteogenesis. Therefore, we propose SIK1 to be a useful therapeutic target for the development of bone anabolic strategies.

Published

2019

5. Activation of ectopic olfactory receptor 544 induces GLP-1 secretion and regulates gut inflammation

Author

Yu Eun Cheong, Min Kyung Park, Jimin Kim, Seung Hoi Koo, You Kyoung Shin, Ji-Sun Kim, GwangPyo Ko, Kyoung Heon Kim, Chunyan Wu, H.R. Kang, Chung Hwan Cho, Sung Joon Lee, Geun Hee Seol, Mi Young Jeong, Jung Yeon Kim, and Giljae Lee

Subjects

Male, Microbiology (medical), Colon, gut microbiome, Inflammation, Enteroendocrine cell, RC799-869, Biology, Diet, High-Fat, Receptors, Odorant, Microbiology, colonic inflammation, Mice, Glucagon-Like Peptide 1, medicine, Olfr544, Animals, Humans, Dicarboxylic Acids, Secretion, Obesity, Microbiome, Receptor, ectopic olfactory receptor, Mice, Knockout, Gene knockdown, Olfactory receptor, Intestinal permeability, Bacteria, digestive, oral, and skin physiology, Gastroenterology, Diseases of the digestive system. Gastroenterology, medicine.disease, Gastrointestinal Microbiome, Cell biology, Infectious Diseases, medicine.anatomical_structure, metabolome, medicine.symptom, GLP-1, Research Article, Research Paper

Abstract

Olfactory receptors are ectopically expressed in extra-nasal tissues. The gut is constantly exposed to high levels of odorants where ectopic olfactory receptors may play critical roles. Activation of ectopic olfactory receptor 544 (Olfr544) by azelaic acid (AzA), an Olfr544 ligand, reduces adiposity in mice fed a high-fat diet (HFD) by regulating fuel preference to fats. Herein, we investigated the novel function of Olfr544 in the gut. In GLUTag cells, AzA induces the cAMP-PKA-CREB signaling axis and increases the secretion of GLP-1, an enteroendocrine hormone with anti-obesity effects. In mice fed a HFD and orally administered AzA, GLP-1 plasma levels were elevated in mice. The induction of GLP-1 secretion was negated in cells with Olfr544 gene knockdown and in Olfr544-deficient mice. Gut microbiome analysis revealed that AzA increased the levels of Bacteroides acidifaciens and microbiota associated with antioxidant pathways. In fecal metabolomics analysis, the levels of succinate and trehalose, metabolites correlated with a lean phenotype, were elevated by AzA. The function of Olfr544 in gut inflammation, a key feature in obesity, was further investigated. In RNA sequencing analysis, AzA suppressed LPS-induced activation of inflammatory pathways and reduced TNF-α and IL-6 expression, thereby improving intestinal permeability. The effects of AzA on the gut metabolome, microbiome, and colon inflammation were abrogated in Olfr544-KO mice. These results collectively demonstrated that activation of Olfr544 by AzA in the gut exerts multiple effects by regulating GLP-1 secretion, gut microbiome and metabolites, and colonic inflammation in anti-obesogenic phenotypes and, thus, may be applied for obesity therapeutics.

Published

2021

6. Depletion of

Author

Seri, Choi, Dahee, Choi, Yun-Kyung, Lee, Seung Hyun, Ahn, Je Kyung, Seong, Sung Wook, Chi, Tae Jung, Oh, Sung Hee, Choi, and Seung-Hoi, Koo

Subjects

Male, Mice, Knockout, Protein-Arginine N-Methyltransferases, Adenylate Kinase, Body Weight, Diet, High-Fat, Lipid Metabolism, Mice, Glucose, Adipose Tissue, 3T3-L1 Cells, Adipocytes, Animals, Homeostasis, Obesity, Insulin Resistance, Signal Transduction

Abstract

Protein arginine methyltransferase (PRMT) 1 is involved in the regulation of various metabolic pathways such as glucose metabolism in liver and atrophy in the skeletal muscle. However, the role of PRMT1 in the fat tissues under the disease state has not been elucidated to date. In this study, we delineate the function of this protein in adipocytes in vivo. PRMT1 expression was abundant in the white adipose tissues (WAT), which was induced upon a high-fat diet in mice and by obesity in humans. We found that adipocyte-specific depletion of

Published

2020

7. Loss of the E3 ubiquitin ligase MKRN1 represses diet-induced metabolic syndrome through AMPK activation

Author

Sung Eun Kim, Jea woo Kim, Su Yeon Han, Min Sik Lee, Daehee Hwang, Je Kyung Seong, Seung Hoi Koo, Hyun Ji Han, Il Young Kim, Sehyun Chae, Soyeon Shin, Choong Sil Lee, Manhyung Jeong, Seul Gi Yoon, Yun Hee Lee, Ho Young Lee, Kyoung Jin Oh, Jung-Hoon Kim, Jaewhan Song, Kwang-Hee Bae, Jun Won Park, and Andrew H. Ko

Subjects

0301 basic medicine, Male, Cancer Research, Anabolism, Physiology, General Physics and Astronomy, Adipose tissue, lcsh:Medicine, AMP-Activated Protein Kinases, Small hairpin RNA, Mice, Ubiquitin, Mkrn1, Non-alcoholic Fatty Liver Disease, Adipocytes, lcsh:Science, lcsh:QH301-705.5, Metabolic Syndrome, Mice, Knockout, Ampk, Multidisciplinary, biology, Chemistry, Fatty liver, Diabetes, Ubiquitin ligase, Cell biology, Liver, Ribonucleoproteins, Lipogenesis, Knockout mouse, Molecular Medicine, Female, Science, Ubiquitin-Protein Ligases, Diet, High-Fat, Biochemistry, Genetics and Molecular Biology (miscellaneous), Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, medicine, Animals, Obesity, Protein kinase A, lcsh:R, AMPK, General Chemistry, medicine.disease, Microreview, Fatty Liver, 030104 developmental biology, lcsh:Biology (General), biology.protein, lcsh:Q, Metabolic syndrome

Abstract

AMP-activated protein kinase (AMPK) plays a key role in controlling energy metabolism in response to physiological and nutritional status. Although AMPK activation has been proposed as a promising molecular target for treating obesity and its related comorbidities, the use of pharmacological AMPK activators has been met with contradictory therapeutic challenges. Here we show a regulatory mechanism for AMPK through its ubiquitination and degradation by the E3 ubiquitin ligase makorin ring finger protein 1 (MKRN1). MKRN1 depletion promotes glucose consumption and suppresses lipid accumulation due to AMPK stabilisation and activation. Accordingly, MKRN1-null mice show chronic AMPK activation in both liver and adipose tissue, resulting in significant suppression of diet-induced metabolic syndrome. We demonstrate also its therapeutic effect by administering shRNA targeting MKRN1 into obese mice that reverses non-alcoholic fatty liver disease. We suggest that ubiquitin-dependent AMPK degradation represents a target therapeutic strategy for metabolic disorders., AMPK activation has been suggested as treatment for obesity and its complications. Here the authors show that the ubiquitin ligase MKRN1 binds to AMPK and mediates its ubiquitination and degradation. Loss of MKRN1 leads to AMPK activation, increased glucose consumption and decreased lipid accumulation.

Published

2018

8. The SMILE transcriptional corepressor inhibits cAMP response element–binding protein (CREB)–mediated transactivation of gluconeogenic genes

Author

Yoon Seok Jung, Hye Sook Han, Seung Hoi Koo, Robert A. Harris, Ji Min Lee, and Hueng Sik Choi

Subjects

Male, Transcriptional Activation, 0301 basic medicine, Leucine zipper, CREB, Biochemistry, Mice, 03 medical and health sciences, Transactivation, 0302 clinical medicine, Coactivator, Animals, Gene Regulation, Cyclic AMP Response Element-Binding Protein, Promoter Regions, Genetic, Molecular Biology, Regulation of gene expression, biology, Chemistry, Gluconeogenesis, Cell Biology, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Phosphoenolpyruvate Carboxylase, Cell biology, CRTC2, Mice, Inbred C57BL, Basic-Leucine Zipper Transcription Factors, 030104 developmental biology, Gene Expression Regulation, Liver, Transcription Coactivator, Glucose-6-Phosphatase, biology.protein, Corepressor, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Under fasting conditions, activation of several hepatic genes sets the stage for gluconeogenesis in the liver. cAMP response element–binding protein (CREB), CREB-regulated transcription coactivator 2 (CRTC2), and peroxisome proliferator–activated receptor γ coactivator 1-alpha (PGC-1α) are essential for this transcriptional induction of gluconeogenic genes. PGC-1α induction is mediated by activation of a CREB/CRTC2 signaling complex, and recent findings have revealed that small heterodimer partner–interacting leucine zipper protein (SMILE), a member of the CREB/ATF family of basic region–leucine zipper (bZIP) transcription factors, is an insulin-inducible corepressor that decreases PGC-1α expression and abrogates its stimulatory effect on hepatic gluconeogenesis. However, the molecular mechanism whereby SMILE suppresses PGC-1α expression is unknown. Here, we investigated SMILE's effects on the CREB/CRTC2 signaling pathway and glucose metabolism. We found that SMILE significantly inhibits CREB/CRTC2-induced PGC-1α expression by interacting with and disrupting the CREB/CRTC2 complex. Consequently, SMILE decreased PGC-1α–induced hepatic gluconeogenic gene expression. Furthermore, SMILE inhibited CREB/CRTC2-induced phosphoenolpyruvate carboxykinase (PEPCK) and glucose-6-phosphatase (G6Pase) gene expression by directly repressing the expression of these genes and by indirectly inhibiting the expression of PGC-1α via CREB/CRTC2 repression. Indeed, enhanced gluconeogenesis and circulating blood glucose levels in mice injected with an adenovirus construct containing a constitutively active CRTC2 variant (CRTC2–S171A) were significantly reduced by WT SMILE, but not by leucine zipper–mutated SMILE. These results reveal that SMILE represses CREB/CRTC2-induced PGC-1α expression, an insight that may help inform potential therapeutic approaches targeting PGC-1α–mediated regulation of hepatic glucose metabolism.

Published

2018

9. PDK4 Deficiency Suppresses Hepatic Glucagon Signaling by Decreasing cAMP Levels

Author

Jae-Han Jeon, Inkyu Lee, Yong Hyun Jeon, Jeong Eun Kim, Woong Kwon, Younghoon Go, Nam Ho Jeoung, Ling He, Hye Jin Ham, Bo Yoon Park, Byung-Gyu Kim, Eun Kyung Yoo, Keun-Gyu Park, Robert A. Harris, and Seung Hoi Koo

Subjects

Male, 0301 basic medicine, Pyruvate decarboxylation, medicine.medical_specialty, Pyruvate dehydrogenase kinase, Endocrinology, Diabetes and Metabolism, Blotting, Western, PDK4, Protein Serine-Threonine Kinases, Real-Time Polymerase Chain Reaction, Pathophysiology, Glucagon, Mice, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, Cyclic AMP, Internal Medicine, medicine, Animals, Beta oxidation, Cells, Cultured, Triglycerides, Sulfonamides, Kinase, Gluconeogenesis, Pyruvate Dehydrogenase Acetyl-Transferring Kinase, Glucose Tolerance Test, Isoquinolines, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Liver, chemistry, Hepatocytes, Etomoxir

Abstract

In fasting or diabetes, gluconeogenic genes are transcriptionally activated by glucagon stimulation of the cAMP-protein kinase A (PKA)–CREB signaling pathway. Previous work showed pyruvate dehydrogenase kinase (PDK) inhibition in skeletal muscle increases pyruvate oxidation, which limits the availability of gluconeogenic substrates in the liver. However, this study found upregulation of hepatic PDK4 promoted glucagon-mediated expression of gluconeogenic genes, whereas knockdown or inhibition of hepatic PDK4 caused the opposite effect on gluconeogenic gene expression and decreased hepatic glucose production. Mechanistically, PDK4 deficiency decreased ATP levels, thus increasing phosphorylated AMPK (p-AMPK), which increased p-AMPK–sensitive phosphorylation of cyclic nucleotide phosphodiesterase 4B (p-PDE4B). This reduced cAMP levels and consequently p-CREB. Metabolic flux analysis showed that the reduction in ATP was a consequence of a diminished rate of fatty acid oxidation (FAO). However, overexpression of PDK4 increased FAO and increased ATP levels, which decreased p-AMPK and p-PDE4B and allowed greater accumulation of cAMP and p-CREB. The latter were abrogated by the FAO inhibitor etomoxir, suggesting a critical role for PDK4 in FAO stimulation and the regulation of cAMP levels. This finding strengthens the possibility of PDK4 as a target against diabetes.

Published

2018

10. Olfactory receptor 544 reduces adiposity by steering fuel preference toward fats

Author

Dahee Choi, Chunyan Wu, In Geol Choi, Duleepa Pathiraja, Su Hyeon Hwang, Kim Yeon Ji, Sung Joon Lee, Yaoyao Jia, Joobong Choi, and Seung Hoi Koo

Subjects

0301 basic medicine, Olfactory system, medicine.medical_specialty, Lipolysis, Adipose tissue, Diet, High-Fat, Receptors, Odorant, Mice, 03 medical and health sciences, 0302 clinical medicine, Metabolic Diseases, Adipose Tissue, Brown, 3T3-L1 Cells, Internal medicine, Glucose Intolerance, Brown adipose tissue, Ketogenesis, medicine, Humans, Animals, PPAR alpha, Obesity, Adiposity, Mice, Knockout, Olfactory receptor, Chemistry, Brief Report, Thermogenesis, General Medicine, Cyclic AMP-Dependent Protein Kinases, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Liver, Ketone bodies, PPARGC1A, Insulin Resistance, Energy Metabolism, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Olfactory receptors (ORs) are present in tissues outside the olfactory system; however, the function of these receptors remains relatively unknown. Here, we determined that olfactory receptor 544 (Olfr544) is highly expressed in the liver and adipose tissue of mice and regulates cellular energy metabolism and obesity. Azelaic acid (AzA), an Olfr544 ligand, specifically induced PKA-dependent lipolysis in adipocytes and promoted fatty acid oxidation (FAO) and ketogenesis in liver, thus shifting the fuel preference to fats. After 6 weeks of administration, mice fed a high-fat diet (HFD) exhibited a marked reduction in adiposity. AzA treatment induced expression of PPAR-α and genes required for FAO in the liver and induced the expression of PPAR-γ coactivator 1-α (Ppargc1a) and uncoupling protein-1 (Ucp1) genes in brown adipose tissue (BAT). Moreover, treatment with AzA increased insulin sensitivity and ketone body levels. This led to a reduction in the respiratory quotient and an increase in the FAO rate, as indicated by indirect calorimetry. AzA treatment had similar antiobesogenic effects in HFD-fed ob/ob mice. Importantly, AzA-associated metabolic changes were completely abrogated in HFD-fed Olfr544–/– mice. To our knowledge, this is the first report to show that Olfr544 orchestrates the metabolic interplay between the liver and adipose tissue, mobilizing stored fats from adipose tissue and shifting the fuel preference to fats in the liver and BAT.

Published

2017

11. Prominin-1-Radixin axis controls hepatic gluconeogenesis by regulating PKA activity

Author

Jae Seon Lee, Hong Lim Kim, Hyun Geun Lee, Young Gyu Ko, Dong Min Yu, Jun Sub Park, Junseok Kim, H. Lee, Seung Hoi Koo, and Sungsoo Lee

Subjects

Cell, CREB, Biochemistry, Glucagon, 03 medical and health sciences, Mice, 0302 clinical medicine, Radixin, Genetics, medicine, Animals, AC133 Antigen, Protein kinase A, Molecular Biology, 030304 developmental biology, 0303 health sciences, Messenger RNA, Gene knockdown, biology, Chemistry, Gluconeogenesis, Membrane Proteins, Articles, Cell biology, Cytoskeletal Proteins, medicine.anatomical_structure, Glucose, Liver, biology.protein, Hepatocytes, 030217 neurology & neurosurgery

Abstract

Prominin‐1 (Prom1) is a major cell surface marker of cancer stem cells, but its physiological functions in the liver have not been elucidated. We analyzed the levels of mRNA transcripts in serum‐starved primary WT (Prom1 (+/+)) and KO (Prom1 (−/−)) mouse hepatocytes using RNA sequencing (RNA‐seq) data, and found that CREB target genes were downregulated. This initial observation led us to determine that Prom1 deficiency inhibited cAMP response element‐binding protein (CREB) activation and gluconeogenesis, but not cyclic AMP (cAMP) accumulation, in glucagon‐, epinephrine‐, or forskolin‐treated liver tissues and primary hepatocytes, and mitigated glucagon‐induced hyperglycemia. Because Prom1 interacted with radixin, Prom1 deficiency prevented radixin from localizing to the plasma membrane. Moreover, systemic adenoviral knockdown of radixin inhibited CREB activation and gluconeogenesis in glucagon‐treated liver tissues and primary hepatocytes, and mitigated glucagon‐elicited hyperglycemia. Based on these results, we conclude that Prom1 regulates hepatic PKA signaling via radixin functioning as an A kinase‐anchored protein (AKAP).

Published

2019

12. PRMT1 Is Required for the Maintenance of Mature β-Cell Identity

Author

Seung Hoi Koo, Je Kyung Seong, Kanghoon Lee, Haejeong Heo, Eun-Ha Kim, Seyun Kim, Eun Hye Seo, Hee-Jin Kim, Jae Myoung Suh, Hyunki Kim, Yong Kyung Kim, Byoung Ha Yoon, Joonyub Lee, Mirang Kim, Chang-Myung Oh, Hail Kim, Junguee Lee, Hyeongseok Kim, Mi Young Kim, Young Seok Ju, Kijong Yi, Heein Song, and Minho Shong

Subjects

0301 basic medicine, CCCTC-Binding Factor, Protein-Arginine N-Methyltransferases, Endocrinology, Diabetes and Metabolism, Down-Regulation, 030209 endocrinology & metabolism, Biology, Methylation, Histone H4, Histones, 03 medical and health sciences, Gene Knockout Techniques, Mice, 0302 clinical medicine, Downregulation and upregulation, Insulin-Secreting Cells, Glucose Intolerance, Insulin Secretion, Internal Medicine, Animals, RNA-Seq, Gene, Transcription factor, Regulation of gene expression, Mice, Knockout, Cell Differentiation, Chromatin, Cell biology, Histone Code, 030104 developmental biology, Gene Expression Regulation, CTCF, PDX1, Chromatin Immunoprecipitation Sequencing

Abstract

Loss of functional β-cell mass is an essential feature of type 2 diabetes, and maintaining mature β-cell identity is important for preserving a functional β-cell mass. However, it is unclear how β-cells achieve and maintain their mature identity. Here we demonstrate a novel function of protein arginine methyltransferase 1 (PRMT1) in maintaining mature β-cell identity. Prmt1 knockout in fetal and adult β-cells induced diabetes, which was aggravated by high-fat diet–induced metabolic stress. Deletion of Prmt1 in adult β-cells resulted in the immediate loss of histone H4 arginine 3 asymmetric dimethylation (H4R3me2a) and the subsequent loss of β-cell identity. The expression levels of genes involved in mature β-cell function and identity were robustly downregulated as soon as Prmt1 deletion was induced in adult β-cells. Chromatin immunoprecipitation sequencing and assay for transposase-accessible chromatin sequencing analyses revealed that PRMT1-dependent H4R3me2a increases chromatin accessibility at the binding sites for CCCTC-binding factor (CTCF) and β-cell transcription factors. In addition, PRMT1-dependent open chromatin regions may show an association with the risk of diabetes in humans. Together, our results indicate that PRMT1 plays an essential role in maintaining β-cell identity by regulating chromatin accessibility.

Published

2019

13. Skeletal muscle-specific Prmt1 deletion causes muscle atrophy via deregulation of the PRMT6-FOXO3 axis

Author

Seri Choi, Sung Chun Cho, Je Kyung Seong, Hyeon Ju Jeong, Dahee Choi, Seung Hoi Koo, Jong-Sun Kang, and Hyebeen Kim

Subjects

0301 basic medicine, Protein-Arginine N-Methyltransferases, Methyltransferase, Arginine, Ubiquitin-Protein Ligases, Histone Deacetylase 2, Muscle Proteins, Biology, Methylation, Proto-Oncogene Mas, Histone Deacetylases, Tripartite Motif Proteins, 03 medical and health sciences, Mice, medicine, Autophagy, Animals, Humans, Phosphorylation, Muscle, Skeletal, Molecular Biology, YY1 Transcription Factor, Mice, Knockout, 030102 biochemistry & molecular biology, Regeneration (biology), Forkhead Box Protein O3, Skeletal muscle, Cell Biology, Metabolism, Muscle atrophy, Cell biology, Muscular Atrophy, 030104 developmental biology, medicine.anatomical_structure, HEK293 Cells, FOXO3, medicine.symptom, Microtubule-Associated Proteins, Research Paper, Signal Transduction

Abstract

Protein arginine methyltransferases (PRMTs) have emerged as important regulators of skeletal muscle metabolism and regeneration. However, the direct roles of the various PRMTs during skeletal muscle remodeling remain unclear. Using skeletal muscle-specific prmt1 knockout mice, we examined the function and downstream targets of PRMT1 in muscle homeostasis. We found that muscle-specific PRMT1 deficiency led to muscle atrophy. PRMT1-deficient muscles exhibited enhanced expression of a macroautophagic/autophagic marker LC3-II, FOXO3 and muscle-specific ubiquitin ligases, TRIM63/MURF-1 and FBXO32, likely contributing to muscle atrophy. The mechanistic study reveals that PRMT1 regulates FOXO3 through PRMT6 modulation. In the absence of PRMT1, increased PRMT6 specifically methylates FOXO3 at arginine 188 and 249, leading to its activation. Finally, we demonstrate that PRMT1 deficiency triggers FOXO3 hyperactivation, which is abrogated by PRMT6 depletion. Taken together, PRMT1 is a key regulator for the PRMT6-FOXO3 axis in the control of autophagy and protein degradation underlying muscle maintenance. Abbreviations: Ad-RNAi: adenovirus-delivered small interfering RNA; AKT: thymoma viral proto-oncogene; AMPK: AMP-activated protein kinase; Baf A1: bafilomycin A1; CSA: cross-sectional area; EDL: extensor digitorum longus; FBXO32: F-box protein 32; FOXO: forkhead box O; GAS: gatrocnemieus; HDAC: histone deacetylase; IGF: insulin-like growth factor; LAMP: lysosomal-associated membrane protein; MAP1LC3B/LC3B: microtubule-associated protein 1 light chain 3 beta; mKO: Mice with skeletal muscle-specific deletion of Prmt1; MTOR: mechanistic target of rapamycin kinase; MYH: myosin heavy chain; MYL1/MLC1f: myosin, light polypeptide 1; PRMT: protein arginine N-methyltransferase; sgRNA: single guide RNA; SQSTM1: sequestosome 1; SOL: soleus; TA: tibialis anterior; TRIM63/MURF-1: tripartite motif-containing 63; YY1: YY1 transcription factor

Published

2019

14. Prmt7 Deficiency Causes Reduced Skeletal Muscle Oxidative Metabolism and Age-Related Obesity

Author

Jong-Sun Kang, Hyejin Lee, Hyeon Ju Jeong, Seung Hoi Koo, Kyu Sil Choi, Dahee Choi, Tuan Anh Vuong, Sung Chun Cho, and Hana Cho

Subjects

Male, 0301 basic medicine, Aging, Protein-Arginine N-Methyltransferases, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, p38 mitogen-activated protein kinases, Regulator, Biology, Myoblasts, Mice, 03 medical and health sciences, Oxygen Consumption, Endurance training, Physical Conditioning, Animal, Diabetes mellitus, Internal medicine, Internal Medicine, medicine, Animals, Myocyte, Obesity, Muscle, Skeletal, Promoter Regions, Genetic, Protein kinase A, Mice, Knockout, Activating Transcription Factor 2, Skeletal muscle, medicine.disease, Lipids, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Physical Endurance, Female, Energy Metabolism, Signal Transduction

Abstract

Maintenance of skeletal muscle function is critical for metabolic health and the disruption of which exacerbates many chronic diseases such as obesity and diabetes. Skeletal muscle responds to exercise or metabolic demands by a fiber-type switch regulated by signaling-transcription networks that remains to be fully defined. Here, we report that protein arginine methyltransferase 7 (Prmt7) is a key regulator for skeletal muscle oxidative metabolism. Prmt7 is expressed at the highest levels in skeletal muscle and decreased in skeletal muscles with age or obesity. Prmt7−/− muscles exhibit decreased oxidative metabolism with decreased expression of genes involved in muscle oxidative metabolism, including PGC-1α. Consistently, Prmt7−/− mice exhibited significantly reduced endurance exercise capacities. Furthermore, Prmt7−/− mice exhibit decreased energy expenditure, which might contribute to the exacerbated age-related obesity of Prmt7−/− mice. Similarly to Prmt7−/− muscles, Prmt7 depletion in myoblasts also reduces PGC-1α expression and PGC-1α–promoter driven reporter activities. Prmt7 regulates PGC-1α expression through interaction with and activation of p38 mitogen-activated protein kinase (p38MAPK), which in turn activates ATF2, an upstream transcriptional activator for PGC-1α. Taken together, Prmt7 is a novel regulator for muscle oxidative metabolism via activation of p38MAPK/ATF2/PGC-1α.

Published

2016

15. Cardiac specific PRMT1 ablation causes heart failure through CaMKII dysregulation

Author

Tuan Anh Vuong, Jong-Sun Kang, Hyun Ji Kim, Byeong Yun Ahn, Dong I. Lee, Seung Hoi Koo, Jung Hoon Pyun, Seri Choi, Hana Cho, and Myong Ho Jeong

Subjects

0301 basic medicine, Cardiac function curve, Protein-Arginine N-Methyltransferases, Arginine, Science, General Physics and Astronomy, 030204 cardiovascular system & hematology, environment and public health, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Electrocardiography, Mice, 0302 clinical medicine, Ca2+/calmodulin-dependent protein kinase, medicine, Myocyte, Animals, Humans, Myocytes, Cardiac, lcsh:Science, Protein kinase A, CAMK, Heart Failure, Mice, Knockout, Multidisciplinary, business.industry, Myocardium, musculoskeletal, neural, and ocular physiology, Dilated cardiomyopathy, General Chemistry, medicine.disease, Immunohistochemistry, Cell biology, Electrophysiology, 030104 developmental biology, nervous system, Echocardiography, Heart failure, cardiovascular system, lcsh:Q, business, Calcium-Calmodulin-Dependent Protein Kinase Type 2, tissues

Abstract

Dysregulation of Ca2+/calmodulin-dependent protein kinase (CaMK)II is closely linked with myocardial hypertrophy and heart failure. However, the mechanisms that regulate CaMKII activity are incompletely understood. Here we show that protein arginine methyltransferase 1 (PRMT1) is essential for preventing cardiac CaMKII hyperactivation. Mice null for cardiac PRMT1 exhibit a rapid progression to dilated cardiomyopathy and heart failure within 2 months, accompanied by cardiomyocyte hypertrophy and fibrosis. Consistently, PRMT1 is downregulated in heart failure patients. PRMT1 depletion in isolated cardiomyocytes evokes hypertrophic responses with elevated remodeling gene expression, while PRMT1 overexpression protects against pathological responses to neurohormones. The level of active CaMKII is significantly elevated in PRMT1-deficient hearts or cardiomyocytes. PRMT1 interacts with and methylates CaMKII at arginine residues 9 and 275, leading to its inhibition. Accordingly, pharmacological inhibition of CaMKII restores contractile function in PRMT1-deficient mice. Thus, our data suggest that PRMT1 is a critical regulator of CaMKII to maintain cardiac function., The mechanisms that regulate the activity of Ca2 +/calmodulin-dependent protein kinase II (CaMKII) in the context of heart failure are incompletely understood. Here the authors show that protein arginine methyltransferase 1 (PRMT1) prevents cardiac hyperactivation of CaMKII and heart failure development by methylating CaMKII at arginine residues 9 and 275.

Published

2018

16. Insulin-Inducible SMILE Inhibits Hepatic Gluconeogenesis

Author

Chul-Ho Lee, Seung Hoi Koo, Ji Min Lee, Kyoung Jin Oh, Seri Choi, Hye Sook Han, Hueng Sik Choi, Woo Young Seo, Byeong Hun Choi, Yong-Soo Lee, Robert A. Harris, and Don Kyu Kim

Subjects

Chromatin Immunoprecipitation, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Blotting, Western, Gene Expression, Mice, Inbred Strains, Diet, High-Fat, Polymerase Chain Reaction, Glucagon, Cell Line, Eating, Mice, Internal medicine, Internal Medicine, medicine, Animals, Hypoglycemic Agents, Insulin, Protein kinase B, Mice, Knockout, biology, Gluconeogenesis, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Receptor, Insulin, Mice, Inbred C57BL, Insulin receptor, Hepatocyte nuclear factors, Basic-Leucine Zipper Transcription Factors, Endocrinology, Hepatocyte Nuclear Factor 4, Liver, Hepatocyte nuclear factor 4, Hepatocytes, biology.protein, Signal transduction, Proto-Oncogene Proteins c-akt, Transcription Factors

Abstract

The role of a glucagon/cAMP-dependent protein kinase–inducible coactivator PGC-1α signaling pathway is well characterized in hepatic gluconeogenesis. However, an opposing protein kinase B (PKB)/Akt-inducible corepressor signaling pathway is unknown. A previous report has demonstrated that small heterodimer partner–interacting leucine zipper protein (SMILE) regulates the nuclear receptors and transcriptional factors that control hepatic gluconeogenesis. Here, we show that hepatic SMILE expression was induced by feeding in normal mice but not in db/db and high-fat diet (HFD)-fed mice. Interestingly, SMILE expression was induced by insulin in mouse primary hepatocyte and liver. Hepatic SMILE expression was not altered by refeeding in liver-specific insulin receptor knockout (LIRKO) or PKB β-deficient (PKBβ−/−) mice. At the molecular level, SMILE inhibited hepatocyte nuclear factor 4–mediated transcriptional activity via direct competition with PGC-1α. Moreover, ablation of SMILE augmented gluconeogenesis and increased blood glucose levels in mice. Conversely, overexpression of SMILE reduced hepatic gluconeogenic gene expression and ameliorated hyperglycemia and glucose intolerance in db/db and HFD-fed mice. Therefore, SMILE is an insulin-inducible corepressor that suppresses hepatic gluconeogenesis. Small molecules that enhance SMILE expression would have potential for treating hyperglycemia in diabetes.

Published

2015

17. Salt-Inducible Kinase 1 Terminates cAMP Signaling by an Evolutionarily Conserved Negative-Feedback Loop in β-Cells

Author

Hana Cho, Min Jung Kim, Young Sil Yoon, Jin-Young Park, Ji Hyun Lee, Dong Jun Sung, Su Kyung Park, Seong-Tae Kim, Jae-Hyung Park, Chang Yun Jung, Dae Kyu Song, Keun-Gyu Park, and Seung Hoi Koo

Subjects

medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Phosphodiesterase 3, Haploinsufficiency, In Vitro Techniques, Protein Serine-Threonine Kinases, Biology, Mice, Insulin-Secreting Cells, Insulin receptor substrate, Internal medicine, Insulin Secretion, Cyclic AMP, Internal Medicine, medicine, Animals, Insulin, Glucose homeostasis, Protein kinase A, Feedback, Physiological, Kinase, Phosphodiesterase, Biological Evolution, Cyclic Nucleotide Phosphodiesterases, Type 4, Rats, Glucose, Endocrinology, Signal transduction, Signal Transduction

Abstract

Pancreatic β-cells are critical in the regulation of glucose homeostasis by controlled secretion of insulin in mammals. Activation of protein kinase A by cAMP is shown to be responsible for enhancing this pathway, which is countered by phosphodiesterase (PDE) that converts cAMP to AMP and turns off the signal. Salt-inducible kinases (SIKs) were also known to inhibit cAMP signaling, mostly by promoting inhibitory phosphorylation on CREB-regulated transcription coactivators. Here, we showed that SIK1 regulates insulin secretion in β-cells by modulating PDE4D and cAMP concentrations. Haploinsufficiency of SIK1 led to the improved glucose tolerance due to the increased glucose-stimulated insulin secretion. Depletion of SIK1 promoted higher cAMP concentration and increased insulin secretion from primary islets, suggesting that SIK1 controls insulin secretion through the regulation of cAMP signaling. By using a consensus phosphorylation site of SIK1, we identified PDE4D as a new substrate for this kinase family. In vitro kinase assay as well as mass spectrometry analysis revealed that the predicted Ser136 and the adjacent Ser141 of PDE4D are critical in SIK1-mediated phosphorylation. We found that overexpression of either SIK1 or PDE4D in β-cells reduced insulin secretion, while inhibition of PDE4 activity by rolipram or knockdown of PDE4D restored it, showing indeed that SIK1-dependent phosphorylation of PDE4D is critical in reducing cAMP concentration and insulin secretion from β-cells. Taken together, we propose that SIK1 serves as a part of a self-regulatory circuit to modulate insulin secretion from pancreatic β-cells by controlling cAMP concentration through modulation of PDE4D activity.

Published

2015

18. HBx induces the proliferation of hepatocellular carcinoma cells via AP1 over-expressed as a result of ER stress

Author

So Young Kim, Yi Yi Kyaw, Aye Aye Win, Seung Hoi Koo, Hyeong Hoe Kim, Hyun Kook Cho, and JaeHun Cheong

Subjects

Hepatitis B virus, Primary Cell Culture, Biology, Endoplasmic Reticulum, Biochemistry, Mice, Genes, Reporter, Animals, Humans, Viral Regulatory and Accessory Proteins, Cyclic AMP Response Element-Binding Protein, Luciferases, Molecular Biology, Cell Proliferation, c-jun, Hep G2 Cells, Cell Biology, Endoplasmic Reticulum Stress, Molecular biology, digestive system diseases, Liver regeneration, Gene Expression Regulation, Neoplastic, Transcription Factor AP-1, HBx, Insulin receptor, AP-1 transcription factor, Cell Transformation, Neoplastic, Host-Pathogen Interactions, Hepatocytes, Trans-Activators, Unfolded protein response, Cancer research, Hepatic stellate cell, biology.protein, Signal transduction, Protein Binding, Signal Transduction

Abstract

Hepatocellular carcinoma (HCC) is one of the most common cancers worldwide and chronic hepatitis B virus (HBV) infection is the most common risk factor for HCC. The HBV proteins can induce oncogenic or synergy effects with a hyperproliferative response on transformation into HCC. CREBH (cAMP-responsive, element-binding protein H), activated by stress in the endoplasmic reticulum (ER), is an ER-resident transmembrane bZIP (basic leucine zipper) transcription factor that is specifically expressed in the liver. In the present study, we address the role played by CREBH activated by ER stress in HBV-induced hepatic cell proliferation. We confirmed CREBH activation by ER stress and showed that it occurred as a result of/via hepatitis B virus X (HBx)-induced ER stress. CREBH activated by HBx increased the expression of AP-1 target genes through c-Jun induction. Under pathological conditions such as liver damage or liver regeneration, activated CREBH may have an important role to play in hepatic inflammation and cell proliferation, as an insulin receptor with dual functions under these conditions. We showed that CREBH activated by HBx interacted with HBx protein, leading to a synergistic effect on the expression of AP-1 target genes and the proliferation of HCC cells and mouse primary hepatocytes. In conclusion, in HBV-infected hepatic cells or patients with chronic HBV, CREBH may induce proliferation of hepatic cells in co-operation with HBx, resulting in HCC.

Published

2015

19. Overweight in Mice and Enhanced Adipogenesis In Vitro Are Associated With Lack of the Hedgehog Coreceptor Boc

Author

Jong-Sun Kang, Seung Hoi Koo, Shin Bum Jo, Hyejin Lee, Anthony I. Romer, Hyo Jeong Lim, Min Jung Kim, and Robert S. Krauss

Subjects

Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Adipokine, Receptors, Cell Surface, White adipose tissue, In Vitro Techniques, Biology, Mice, chemistry.chemical_compound, Adipocyte, Internal medicine, Internal Medicine, medicine, Animals, Receptor, Hedgehog, Cells, Cultured, 2. Zero hunger, Adipogenesis, Reverse Transcriptase Polymerase Chain Reaction, Lipid metabolism, Overweight, Mice, Mutant Strains, Endocrinology, chemistry, Immunoglobulin G, Adipocyte hypertrophy, Obesity Studies

Abstract

Obesity arises from a combination of genetic, environmental, and behavioral factors. However, the processes that regulate white adipose tissue (WAT) expansion at the level of the adipocyte are not well understood. The Hedgehog (HH) pathway plays a conserved role in adipogenesis, inhibiting fat formation in vivo and in vitro, but it has not been shown that mice with reduced HH pathway activity have enhanced adiposity. We report that mice lacking the HH coreceptor BOC displayed age-related overweight and excess WAT. They also displayed alterations in some metabolic parameters but normal food intake. Furthermore, they had an exacerbated response to a high-fat diet, including enhanced weight gain and adipocyte hypertrophy, livers with greater fat accumulation, and elevated expression of genes related to adipogenesis, lipid metabolism, and adipokine production. Cultured Boc−/− mouse embryo fibroblasts showed enhanced adipogenesis relative to Boc+/+ cells, and they expressed reduced levels of HH pathway target genes. Therefore, a loss-of-function mutation in an HH pathway component is associated with WAT accumulation and overweight in mice. Variant alleles of such HH regulators may contribute to WAT accumulation in human individuals with additional genetic or lifestyle-based predisposition to obesity.

Published

2015

20. CREB/CRTC2 controls GLP-1-dependent regulation of glucose homeostasis

Author

Hana Cho, Ji Hyun Lee, Seung Hoi Koo, and Xianlan Wen

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Transcription, Genetic, medicine.drug_class, Enteroendocrine Cells, Incretin, Carbohydrate metabolism, CREB, digestive system, Biochemistry, Oxidative Phosphorylation, Cell Line, 03 medical and health sciences, Mice, Glucagon-Like Peptide 1, Internal medicine, Genetics, medicine, Glucose homeostasis, Animals, Homeostasis, Calcium Signaling, Molecular Biology, G protein-coupled receptor, Mice, Knockout, Bile acid, biology, Chemistry, digestive, oral, and skin physiology, G protein-coupled bile acid receptor, CRTC2, 030104 developmental biology, Endocrinology, Glucose, biology.protein, Calcium, hormones, hormone substitutes, and hormone antagonists, Biotechnology, Transcription Factors

Abstract

Glucagon-like peptide 1 (GLP-1) is a major incretin that controls glucose homeostasis. The secretion of mature GLP-1 is regulated via GPCRs, including bile acid receptor G protein-coupled bile acid receptor 1, which uses cAMP signaling to enhance the exocytosis of GLP-1-containing vesicles. However, the role of cAMP-mediated transcription has not been clearly demonstrated to date. In this study, we explored the role of cAMP response element-binding protein/CREB-regulated transcription coactivator 2 (CREB/CRTC2)-dependent transcription on GLP-1 secretion in the L cells. We found that the reduced CREB/CRTC2 activity impaired the cAMP-dependent increase in GLP-1 secretion, whereas expression of constitutively active CRTC2 increased GLP-1 exocytosis from the L cells. Close investigation revealed that expression of not only proglucagon but also PC1/3, an endopeptidase for GLP-1 maturation, is transcriptionally regulated by CREB/CRTC2. Furthermore, expression of peroxisome proliferator-activating receptor coactivator 1 α is also reduced upon depletion of CRTC2, leading to the decreased expression of oxidative phosphorylation (OxPhos) genes, reduced ATP levels, and calcium concentrations in the L cells. Finally, we observed that intestine-specific CRTC2 knockout mice displayed reduced GLP-1 expression, leading to the lower plasma GLP-1 levels, impaired glucose tolerance, and decreased insulin-containing β cells in pancreatic islets. Our data show that the CREB/CRTC2-dependent transcriptional pathway is critical for regulating glucose homeostasis by controlling production of GLP-1 from the L cells at the level of transcription, maturation, and exocytosis.-Lee, J.-H., Wen, X., Cho, H., Koo, S.-H. CREB/CRTC2 controls GLP-1-dependent regulation of glucose homeostasis.

Published

2017

21. NFIL3 is a negative regulator of hepatic gluconeogenesis

Author

Seung Hoi Koo, Hye Sook Han, and Geon Kang

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Response element, Carbohydrate metabolism, CREB, Binding, Competitive, 03 medical and health sciences, Mice, Endocrinology, Insulin resistance, Internal medicine, medicine, Glucose homeostasis, Animals, Cyclic AMP Response Element-Binding Protein, Promoter Regions, Genetic, Cells, Cultured, Gene knockdown, biology, Gluconeogenesis, medicine.disease, 030104 developmental biology, Basic-Leucine Zipper Transcription Factors, Glucose, Gene Expression Regulation, Liver, biology.protein, Hepatocytes, Ectopic expression

Abstract

Objective Nuclear factor interleukin-3 regulated (NFIL3) has been known as an important transcriptional regulator of the development and the differentiation of immune cells. Although expression of NFIL3 is regulated by nutritional cues in the liver, the role of NFIL3 in the glucose metabolism has not been extensively studied. Thus, we wanted to explore the potential role of NFIL3 in the control of hepatic glucose metabolism. Materials/Methods Mouse primary hepatocytes were cultured to perform western blot analysis, Q-PCR and chromatin immunoprecipitation assay. 293 T cells were cultured to perform luciferase assay. Male C57BL/6 mice (fed a normal chow diet or high fat diet for 27 weeks) as well as ob / ob mice were used for experiments with adenoviral delivery. Results We observed that NFIL3 reduced glucose production in hepatocytes by reducing expression of gluconeogenic gene transcription. The repression by NFIL3 required its basic leucine zipper DNA binding domain, and it competed with CREB onto the binding of cAMP response element in the gluconeogenic promoters. The protein levels of hepatic NFIL3 were decreased in the mouse models of genetic- and diet-induced obesity and insulin resistance, and ectopic expression of NFIL3 in the livers of insulin resistant mice ameliorated hyperglycemia and glucose intolerance, with concomitant reduction in expression of hepatic gluconeogenic genes. Finally, we witnessed that knockdown of NFIL3 in the livers of normal chow-fed mice promoted elevations in the glucose levels and expression of hepatic gluconeogenic genes. Conclusions In this study, we showed that NFIL3 functions as an important regulator of glucose homeostasis in the liver by limiting CREB-mediated hepatic gluconeogenesis. Thus, enhancement of hepatic NFIL3 activity in insulin resistant state could be potentially beneficial in relieving glycemic symptoms in the metabolic diseases.

Published

2017

22. ROR alpha Induces KLF4-Mediated M2 Polarization in the Liver Macrophagesthat Protect against Nonalcoholic Steatohepatitis

Author

Seung Hoi Koo, Hyeon Ji Kim, Mi-Ock Lee, Yong-Hyun Han, Hyelin Na, Jun Seok Kim, Ju Yeon Kim, and Min Woo Nam

Subjects

0301 basic medicine, Male, Cellular differentiation, Regulator, Kruppel-Like Transcription Factors, Biology, Diet, High-Fat, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Kruppel-Like Factor 4, Mice, 0302 clinical medicine, Non-alcoholic Fatty Liver Disease, M2 polarity, Animals, Kupffer cells, RORα, lcsh:QH301-705.5, Cells, Cultured, Orphan receptor, Activator (genetics), Cell Differentiation, Nuclear Receptor Subfamily 1, Group F, Member 1, KLF4, Cell biology, Interleukin-10, Mice, Inbred C57BL, Interleukin 10, 030104 developmental biology, Nuclear receptor, lcsh:Biology (General), Apoptosis, 030220 oncology & carcinogenesis, Immunology, non-alcoholic steatohepatitis

Abstract

The regulation of M1/M2 polarization in liver macrophages is closely associated with the progression of nonalcoholic steatohepatitis (NASH); however, the mechanism involved in this process remains unclear. Here, we describe the orphan nuclear receptor retinoic-acid-related orphan receptor alpha (ROR alpha) as a key regulator of M1/M2 polarization in hepatic residential Kupffer cells (KCs) and infiltrated monocyte-derived macrophages. ROR alpha enhanced M2 polarization in KCs by inducing the kruppel-like factor 4. M2 polarization was defective in KCs and bone-marrow-derived macrophages of the myeloid-specific ROR alpha null mice, and these mice were susceptible to HFD-induced NASH. We found that IL-10 played an important role in connecting the function of M2 KCs to lipid accumulation and apoptosis in hepatocytes. Importantly, M2 polarization was controlled by a ROR alpha activator, JC1-40, which improved symptoms of NASH. Our results suggest that the M2-promoting effects of ROR alpha in liver macrophages may provide better therapeutic strategies against NASH.

Published

2017

23. Fibroblast growth factor 21 analogue LY2405319 lowers blood glucose in streptozotocin-induced insulin-deficient diabetic mice by restoring brown adipose tissue function

Author

Hikweon Lee, Seung Hoi Koo, Keun-Gyu Park, Jeongshik Kim, Mi Sun Choe, Kwi-Hyun Bae, Yong Hyun Jeon, Yeon-Kyung Choi, Inkyu Lee, Younghoon Go, Robert A. Harris, and J. W. Perfield

Subjects

Blood Glucose, Male, medicine.medical_specialty, FGF21, Endocrinology, Diabetes and Metabolism, Glucose uptake, medicine.medical_treatment, Streptozocin, Diabetes Mellitus, Experimental, Mice, Endocrinology, Adipose Tissue, Brown, Mice, Inbred NOD, Diabetes mellitus, Internal medicine, Brown adipose tissue, Internal Medicine, Animals, Homeostasis, Insulin, Medicine, Glucose homeostasis, business.industry, Lipid metabolism, medicine.disease, Streptozotocin, Fibroblast Growth Factors, Mice, Inbred C57BL, Diabetes Mellitus, Type 1, medicine.anatomical_structure, business, Injections, Intraperitoneal, medicine.drug

Abstract

Aim To investigate the effects of LY2405319, an analogue of fibroblast growth factor 21 (FGF21), on glucose homeostasis in streptozotocin (STZ)-induced insulin-deficient mice (STZ mice). Methods Nine-week-old male C57BL/6J mice were administered a single intraperitoneal injection of STZ (150 mg/kg). One week later, after confirmation of hyperglycaemia, saline or LY2405319 (5 mg/kg) was injected subcutaneously daily for 4 weeks. Changes in glucose homeostasis, energy metabolism and brown adipose tissue (BAT) function were assessed. Results The STZ mice had elevated blood glucose and reduced plasma FGF21 levels, impaired glucose uptake in the BAT, and BAT mitochondria with absent or swollen cristae and fewer lipid vacuoles. LY2405319 significantly reduced blood glucose levels and this was associated with increased BAT glucose uptake and changes in gene expression and morphology, indicating improved mitochondrial lipid metabolism in the BAT. Importantly, the ability of LY2405319 to lower blood glucose in STZ mice was compromised after removing interscapular BAT. Conclusions Our results show that LY2405319 reduces blood glucose levels in insulin-deficient diabetes by improving BAT metabolism. Additional studies investigating the therapeutic potential of FGF21 for the treatment of type 1 diabetes are warranted.

Published

2014

24. SIK2 Is Critical in the Regulation of Lipid Homeostasis and Adipogenesis In Vivo

Author

Chul-Ho Lee, Hye Sook Han, Seong-Tae Kim, Young Sil Yoon, Jin-Young Park, Seung Hoi Koo, Keun-Gyu Park, Yong-Hoon Kim, and Yoshihiro Ogawa

Subjects

Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Glucose uptake, Blotting, Western, Activating transcription factor, AMP-Activated Protein Kinases, Deoxyglucose, Protein Serine-Threonine Kinases, Biology, CREB, Mice, chemistry.chemical_compound, Internal medicine, Adipocyte, Internal Medicine, medicine, Animals, Protein kinase A, Cells, Cultured, Adipogenesis, Adiponectin, 3T3 Cells, Lipid Metabolism, Endocrinology, Liver, chemistry, Hepatocytes, biology.protein, GLUT4, Transcription Factors

Abstract

Cyclic AMP promotes chronic expression of target genes mainly by protein kinase A–dependent activation of CREB transcription factor machineries in the metabolic tissues. Here, we wanted to elaborate whether CREB-regulated transcription factor (CRTC)2 and its negative regulator salt-inducible kinase (SIK)2 are involved in the transcriptional control of the metabolic pathway in adipocytes. SIK2 knockout (SIK2 KO) mice exhibited higher blood glucose levels that were associated with impaired glucose and insulin tolerance. Hypertriglyceridemia was apparent in SIK2 KO mice, mainly due to the increased lipolysis from white adipocytes and the decreased fatty acid uptake in the peripheral tissues. Investigation of white adipocytes revealed the increases in fat cell size and macrophage infiltration, which could be linked to the metabolic anomaly that is associated in these mice. Interestingly, SIK2 KO promoted the enhancement in the CRTC2-CREB transcriptional pathway in white adipocytes. SIK2 KO mice displayed increased expression of activating transcription factor (ATF)3 and subsequent downregulation of GLUT4 expression and reduction in high–molecular weight adiponectin levels in the plasma, leading to the reduced glucose uptake in the muscle and white adipocytes. The effect of SIK2-dependent regulation of adipocyte metabolism was further confirmed by in vitro cell cultures of 3T3 L1 adipocytes and the differentiated preadipocytes from the SIK2 or CRTC2 KO mice. Collectively, these data suggest that SIK2 is critical in regulating whole-body glucose metabolism primarily by controlling the CRTC2-CREB function of the white adipocytes.

Published

2014

25. Ursodeoxycholic Acid Inhibits Liver X Receptor α-mediated Hepatic Lipogenesis via Induction of the Nuclear Corepressor SMILE

Author

Chul-Ho Lee, Yong Deuk Kim, Ji Min Lee, Hueng Sik Choi, Gil Tae Gang, Seung Hoi Koo, and Don Kyu Kim

Subjects

Male, Transcriptional Activation, Hydrocarbons, Fluorinated, Blotting, Western, Biology, Diet, High-Fat, environment and public health, Biochemistry, Mice, Gene expression, Coactivator, Animals, Humans, Gene Regulation, Liver X receptor, Molecular Biology, Cells, Cultured, Liver X Receptors, Sulfonamides, Gene knockdown, Reverse Transcriptase Polymerase Chain Reaction, Lipogenesis, Ursodeoxycholic Acid, Hep G2 Cells, Cell Biology, Orphan Nuclear Receptors, Molecular biology, Fatty Acid Synthase, Type I, Mice, Inbred C57BL, Fatty acid synthase, Basic-Leucine Zipper Transcription Factors, HEK293 Cells, Liver, Nuclear receptor, Small heterodimer partner, biology.protein, RNA Interference, Sterol Regulatory Element Binding Protein 1, Corepressor, Acetyl-CoA Carboxylase, Protein Binding

Abstract

Small heterodimer partner interacting leucine zipper protein (SMILE) has been identified as a nuclear corepressor of the nuclear receptor (NRs) family. Here, we examined the role of SMILE in the regulation of nuclear receptor liver X receptor (LXRα)-mediated sterol regulatory element binding protein-1c (SREBP-1c) gene expression. We found that SMILE inhibited T0901317 (T7)-induced transcriptional activity of LXRα, which functions as a major regulator of lipid metabolism by inducing SREBP-1c, fatty acid synthase (FAS), and acetyl-CoA carboxylase (ACC) gene expression. Moreover, we demonstrated that SMILE physically interacts with LXRα and represses T7-induced LXRα transcriptional activity by competing with coactivator SRC-1. Adenoviral overexpression of SMILE (Ad-SMILE) attenuated fat accumulation and lipogenic gene induction in the liver of T7 administered or of high fat diet (HFD)-fed mice. Furthermore, we investigated the mechanism by which ursodeoxycholic acid (UDCA) inhibits LXRα-induced lipogenic gene expression. Interestingly, UDCA treatment significantly increased SMILE promoter activity and gene expression in an adenosine monophosphate-activated kinase-dependent manner. Furthermore, UDCA treatment repressed T7-induced SREBP-1c, FAS, and ACC protein levels, whereas knockdown of endogenous SMILE gene expression by adenovirus SMILE shRNA (Ad-shSMILE) significantly reversed UDCA-mediated repression of SREBP-1c, FAS, and ACC protein levels. Collectively, these results demonstrate that UDCA activates SMILE gene expression through adenosine monophosphate-activated kinase phosphorylation, which leads to repression of LXRα-mediated hepatic lipogenic enzyme gene expression.

Published

2014

26. PRMT1 Is Required for the Maintenance of Mature β-Cell Identity.

Author

Hyunki Kim, Byoung-Ha Yoon, Chang-Myung Oh, Joonyub Lee, Kanghoon Lee, Heein Song, Eunha Kim, Kijong Yi, Mi-Young Kim, Hyeongseok Kim, Yong Kyung Kim, Eun-Hye Seo, Haejeong Heo, Hee-Jin Kim, Junguee Lee, Jae Myoung Suh, Seung-Hoi Koo, Je Kyung Seong, Seyun Kim, and Young Seok Ju

Subjects

PROTEIN arginine methyltransferases, TYPE 2 diabetes, TRANSCRIPTION factors, DEPERSONALIZATION, ARGININE, BINDING sites, DNA methyltransferases, PROTEIN metabolism, GLUCOSE intolerance, CHROMOSOMES, BIOCHEMISTRY, CELL differentiation, GENETICS, ANIMAL experimentation, ISLANDS of Langerhans, PHENOMENOLOGY, GENES, TRANSFERASES, METHYLATION, GENETIC techniques, MICE

Abstract

Loss of functional β-cell mass is an essential feature of type 2 diabetes, and maintaining mature β-cell identity is important for preserving a functional β-cell mass. However, it is unclear how β-cells achieve and maintain their mature identity. Here we demonstrate a novel function of protein arginine methyltransferase 1 (PRMT1) in maintaining mature β-cell identity. Prmt1 knockout in fetal and adult β-cells induced diabetes, which was aggravated by high-fat diet-induced metabolic stress. Deletion of Prmt1 in adult β-cells resulted in the immediate loss of histone H4 arginine 3 asymmetric dimethylation (H4R3me2a) and the subsequent loss of β-cell identity. The expression levels of genes involved in mature β-cell function and identity were robustly downregulated as soon as Prmt1 deletion was induced in adult β-cells. Chromatin immunoprecipitation sequencing and assay for transposase-accessible chromatin sequencing analyses revealed that PRMT1-dependent H4R3me2a increases chromatin accessibility at the binding sites for CCCTC-binding factor (CTCF) and β-cell transcription factors. In addition, PRMT1-dependent open chromatin regions may show an association with the risk of diabetes in humans. Together, our results indicate that PRMT1 plays an essential role in maintaining β-cell identity by regulating chromatin accessibility. [ABSTRACT FROM AUTHOR]

Published

2020

27. Inverse Agonist of Nuclear Receptor ERRγ Mediates Antidiabetic Effect Through Inhibition of Hepatic Gluconeogenesis

Author

Yong-Hoon Kim, Dongryeol Ryu, Seung Bum Park, Su Sung Kim, Chul-Ho Lee, Yo Na Kim, Gil Tae Gang, Inkyu Lee, Jin-Young Park, Cheol Soo Choi, Hueng Sik Choi, Minseob Koh, Taebo Sim, Seung Hoi Koo, and Don Kyu Kim

Subjects

Male, medicine.medical_specialty, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Blotting, Western, Biology, Polymerase Chain Reaction, Cell Line, Rats, Sprague-Dawley, Mice, Internal medicine, Gene expression, Internal Medicine, medicine, Animals, Humans, Hypoglycemic Agents, Inverse agonist, Receptor, Original Research, Metabolic disorder, Gluconeogenesis, nutritional and metabolic diseases, Type 2 Diabetes Mellitus, medicine.disease, Rats, Mice, Inbred C57BL, Tamoxifen, Metabolism, Endocrinology, Liver, Receptors, Estrogen, Nuclear receptor, Hepatocytes, medicine.drug

Abstract

Type 2 diabetes mellitus (T2DM) is a progressive metabolic disorder with diverse pathological manifestations and is often associated with abnormal regulation of hepatic glucose production. Many nuclear receptors known to control the hepatic gluconeogenic program are potential targets for the treatment of T2DM and its complications. Nevertheless, the therapeutic potential of the estrogen-related receptor γ (ERRγ) in T2DM remains unknown. In this study, we show that the nuclear receptor ERRγ is a major contributor to hyperglycemia under diabetic conditions by controlling hepatic glucose production. Hepatic ERRγ expression induced by fasting and diabetic conditions resulted in elevated levels of gluconeogenic gene expression and blood glucose in wild-type mice. Conversely, ablation of hepatic ERRγ gene expression reduced the expression of gluconeogenic genes and normalized blood glucose levels in mouse models of T2DM: db/db and diet-induced obesity (DIO) mice. In addition, a hyperinsulinemic-euglycemic clamp study and long-term studies of the antidiabetic effects of GSK5182, the ERRγ-specific inverse agonist, in db/db and DIO mice demonstrated that GSK5182 normalizes hyperglycemia mainly through inhibition of hepatic glucose production. Our findings suggest that the ability of GSK5182 to control hepatic glucose production can be used as a novel therapeutic approach for the treatment of T2DM.

Published

2013

28. C1-Ten Is a Protein Tyrosine Phosphatase of Insulin Receptor Substrate 1 (IRS-1), Regulating IRS-1 Stability and Muscle Atrophy

Author

Jeongeun Noh, Parkyong Song, Ara Koh, Jaewang Ghim, Jang Hyun Choi, Yong Ryoul Yang, Sehoon Park, Jaeyoon Kim, Nick R. Leslie, Mi Nam Lee, Pann-Ghill Suh, Dongryeol Ryu, Heeyoon Jeong, Sung Ho Ryu, Seung Hoi Koo, and Per Olof Berggren

Subjects

Male, medicine.medical_specialty, Anabolism, Insulin Receptor Substrate Proteins, medicine.medical_treatment, Muscle Fibers, Skeletal, Down-Regulation, Mice, Obese, Biology, Dexamethasone, Cell Line, Muscle hypertrophy, Mice, Insulin resistance, Atrophy, Tensins, Internal medicine, Phosphoprotein Phosphatases, medicine, Animals, Humans, Insulin, Phosphorylation, RNA, Small Interfering, Glucocorticoids, Molecular Biology, Protein Stability, Articles, Cell Biology, medicine.disease, Muscle atrophy, IRS1, Muscular Atrophy, HEK293 Cells, Endocrinology, RNA Interference, Phosphatidylinositol 3-Kinase, medicine.symptom, Signal Transduction

Abstract

Muscle atrophy occurs under various catabolic conditions, including insulin deficiency, insulin resistance, or increased levels of glucocorticoids. This results from reduced levels of insulin receptor substrate 1 (IRS-1), leading to decreased phosphatidylinositol 3-kinase activity and thereby activation of FoxO transcription factors. However, the precise mechanism of reduced IRS-1 under a catabolic condition is unknown. Here, we report that C1-Ten is a novel protein tyrosine phosphatase (PTPase) of IRS-1 that acts as a mediator to reduce IRS-1 under a catabolic condition, resulting in muscle atrophy. C1-Ten preferentially dephosphorylated Y612 of IRS-1, which accelerated IRS-1 degradation. These findings suggest a novel type of IRS-1 degradation mechanism which is dependent on C1-Ten and extends our understanding of the molecular mechanism of muscle atrophy under catabolic conditions. C1-Ten expression is increased by catabolic glucocorticoid and decreased by anabolic insulin. Reflecting these hormonal regulations, the muscle C1-Ten is upregulated in atrophy but downregulated in hypertrophy. This reveals a previously unidentified role of C1-Ten as a relevant PTPase contributing to skeletal muscle atrophy.

Published

2013

29. Prdm4 induction by the small molecule butein promotes white adipose tissue browning

Author

So Mi Kwon, Prashant Rajbhandari, Seo Hyuk Chang, Kye Won Park, Sukchan Lee, Seung Hoi Koo, Jin Mo Ku, No Joon Song, Peter Tontonoz, Seri Choi, Laurent Vergnes, Jung Hoon Yoon, Suji Kim, Karen Reue, and Jeong-Soo Lee

Subjects

0301 basic medicine, obesity, Biochemistry & Molecular Biology, Ucp1, Adipose Tissue, White, Adipose tissue, Mice, Obese, White, White adipose tissue, Prdm4, Bioinformatics, Diet, High-Fat, Butein, Inbred C57BL, metabolic diseases, Article, Obese, 03 medical and health sciences, chemistry.chemical_compound, Mice, Medicinal and Biomolecular Chemistry, Chalcones, Adipose Tissue, Brown, Browning, Animals, Molecular Biology, Human obesity, Chemistry, Brown adipocytes, Brown, Cell Biology, Small molecule, Thermogenin, Cell biology, Diet, Mice, Inbred C57BL, DNA-Binding Proteins, High-Fat, 030104 developmental biology, Energy expenditure, Adipose Tissue, Biochemistry and Cell Biology, Transcription Factors

Abstract

Increasing the thermogenic activity of adipocytes holds promise as an approach to combating human obesity and related metabolic diseases. We identified induction of mouse PR domain containing 4 (Prdm4) by the small molecule butein as a means to induce expression of uncoupling protein 1 (Ucp1), increase energy expenditure, and stimulate the generation of thermogenic adipocytes. This study highlights a Prdm4-dependent pathway, modulated by small molecules, that stimulates browning of white adipose tissue.

Published

2016

30. Metformin stimulates IGFBP-2 gene expression through PPARalpha indiabetic states

Author

Seung Hoi Koo, Hye Suk Kang, Inkyu Lee, Ho Chan Cho, Hueng Sik Choi, Jae-Ho Lee, Byung Hyun Park, Goo Taeg Oh, Dae Kyu Song, and Seung Soon Im

Subjects

0301 basic medicine, Male, medicine.medical_specialty, endocrine system diseases, 030209 endocrinology & metabolism, Type 2 diabetes, Biology, Article, Diabetes Mellitus, Experimental, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, Sirtuin 1, Diabetes mellitus, Internal medicine, medicine, Animals, Humans, Hypoglycemic Agents, PPAR alpha, Obesity, Cells, Cultured, Aged, Regulation of gene expression, Multidisciplinary, Adenylate Kinase, AMPK, Middle Aged, medicine.disease, Metformin, Insulin-Like Growth Factor Binding Protein 2, 030104 developmental biology, Endocrinology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Sirtuin, biology.protein, Female, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

The anti-diabetic drug, metformin, exerts its action through AMP-activated protein kinase (AMPK), and Sirtuin (Sirt1) signaling. Insulin-like growth factor (IGF)-binding protein 2 (IGFBP-2) prevents IGF-1 binding to its receptors, thereby contributing to modulate insulin sensitivity. In this study, we demonstrate that metformin upregulates Igfbp-2 expression through the AMPK-Sirt1-PPARα cascade pathway. In the liver of high fat diet, ob/ob, and db/db mice, Igfbp-2 expression was significantly decreased compared to the expression levels in the wild-type mice (p Igfbp-2 expression by metformin administration was disrupted by gene silencing of Ampk and Sirt1, and this phenomenon was not observed in Pparα-null mice. Notably, activation of IGF-1 receptor (IGF-1R)-dependent signaling by IGF-1 was inhibited by metformin. Finally, when compared to untreated type 2 diabetes patients, the metformin-treated diabetic patients showed increased IGFBP-2 levels with diminished serum IGF-1 levels. Taken together, these findings indicate that IGFBP-2 might be a new target of metformin action in diabetes and the metformin-AMPK-Sirt1-PPARα-IGFBP-2 network may provide a novel pathway that could be applied to ameliorate metabolic syndromes by controlling IGF-1 bioavailability.

Published

2016

31. Orphan Nuclear Receptor Estrogen-Related Receptor γ (ERRγ) Is Key Regulator of Hepatic Gluconeogenesis

Author

Won-Jea Cho, Chul-Ho Lee, Minseob Koh, Hueng Sik Choi, Seung Bum Park, Yong-Hoon Kim, Min Jung Kim, Min Woo Lee, Seung Hoi Koo, Dongryeol Ryu, Don Kyu Kim, and Donghyun Lim

Subjects

Male, medicine.medical_specialty, G6PC, Mice, Transgenic, Biology, Biochemistry, Mice, Estrogen-related receptor, PCK1, Internal medicine, medicine, Animals, Humans, Inverse agonist, Glucose homeostasis, Gene Regulation, Promoter Regions, Genetic, Receptor, Molecular Biology, Heat-Shock Proteins, Regulation of gene expression, Gluconeogenesis, Cell Biology, Orphan Nuclear Receptors, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Rats, Mice, Inbred C57BL, Glucose, Endocrinology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Liver, Receptors, Estrogen, Nuclear receptor, Hepatocytes, Trans-Activators, Insulin Resistance, Transcription Factors

Abstract

Glucose homeostasis is tightly controlled by hormonal regulation of hepatic glucose production. Dysregulation of this system is often associated with insulin resistance and diabetes, resulting in hyperglycemia in mammals. Here, we show that the orphan nuclear receptor estrogen-related receptor γ (ERRγ) is a novel downstream mediator of glucagon action in hepatic gluconeogenesis and demonstrate a beneficial impact of the inverse agonist GSK5182. Hepatic ERRγ expression was increased by fasting-dependent activation of the cAMP-response element-binding protein-CRTC2 pathway. Overexpression of ERRγ induced Pck1 and G6PC gene expression and glucose production in primary hepatocytes, whereas abolition of ERRγ gene expression attenuated forskolin-mediated induction of gluconeogenic gene expression. Deletion and mutation analyses of the Pck1 promoter showed that ERRγ directly regulates the Pck1 gene transcription via ERR response elements of the Pck1 promoter as confirmed by ChIP assay and in vivo imaging analysis. We also demonstrate that GSK5182, an inverse agonist of ERRγ, specifically inhibits the transcriptional activity of ERRγ in a PGC-1α dependent manner. Finally, the ERRγ inverse agonist ameliorated hyperglycemia through inhibition of hepatic gluconeogenesis in db/db mice. Control of hepatic glucose production by an ERRγ-specific inverse agonist is a new potential therapeutic approach for the treatment of type 2 diabetes.

Published

2012

32. Retinoic acid receptor-related orphan receptor α-induced activation of adenosine monophosphate-activated protein kinase results in attenuation of hepatic steatosis

Author

Min-Ho Lee, Hyunjin Kang, Suckchang Hong, Sang Gun Kim, Tae Young Na, Young Sil Yoon, Mi-Ock Lee, Eun Jin Kim, Jinyoung Park, Ho Young Son, Hyeung Geun Park, Seung Hoi Koo, and Won-Jea Cho

Subjects

Adenosine monophosphate, medicine.medical_specialty, Receptors, Retinoic Acid, Mice, Inbred Strains, Diet, High-Fat, Mice, Random Allocation, chemistry.chemical_compound, AMP-Activated Protein Kinase Kinases, Reference Values, Internal medicine, medicine, Animals, Liver X receptor, Protein kinase A, Cells, Cultured, Liver X Receptors, Orphan receptor, Hepatology, biology, Retinoic Acid Receptor alpha, AMPK, Lipid Metabolism, Orphan Nuclear Receptors, Adenosine Monophosphate, Enzyme Activation, Fatty Liver, Disease Models, Animal, Retinoic acid receptor, Fatty acid synthase, Endocrinology, chemistry, Retinoic acid receptor alpha, Hepatocytes, biology.protein, Protein Kinases

Abstract

There is increasing evidence that the retinoic acid receptor–related orphan receptor α (RORα) plays an important role in the regulation of metabolic pathways, particularly of fatty acid and cholesterol metabolism; however, the role of RORα in the regulation of hepatic lipogenesis has not been studied. Here, we report that RORα attenuates hepatic steatosis, probably via activation of the adenosine monophosphate (AMP)-activated protein kinase (AMPK) and repression of the liver X receptor α (LXRα). First, RORα and its activator, cholesterol sulfate (CS), induced phosphorylation of AMPK, which was accompanied by the activation of serine–threonine kinase liver kinase B1 (LKB1). Second, the activation of RORα, either by transient transfection or CS treatment, decreased the TO901317-induced transcriptional expression of LXRα and its downstream target genes, such as the sterol regulatory element binding protein-1 (SREBP-1) and fatty acid synthase. RORα interacted physically with LXRα and inhibited the LXRα response element in the promoter of LXRα, indicating that RORα interrupts the autoregulatory activation loop of LXRα. Third, infection with adenovirus encoding RORα suppressed the lipid accumulation that had been induced by a free-fatty–acid mixture in cultured cells. Furthermore, we observed that the level of expression of the RORα protein was decreased in the liver of mice that were fed a high-fat diet. Restoration of RORα via tail-vein injection of adenovirus (Ad)-RORα decreased the high-fat-diet–induced hepatic steatosis. Finally, we synthesized thiourea derivatives that activated RORα, thereby inducing activation of AMPK and repression of LXRα. These compounds decreased hepatic triglyceride levels and lipid droplets in the high-fat-diet–fed mice. Conclusion: We found that RORα induced activation of AMPK and inhibition of the lipogenic function of LXRα, which may be key phenomena that provide the beneficial effects of RORα against hepatic steatosis. (HEPATOLOGY 2012;)

Published

2012

33. Atypical antipsychotic drugs perturb AMPK-dependent regulation of hepatic lipid metabolism

Author

Su Yeon Lee, Injae Hwang, Jinyoung Park, Kyoung Jin Oh, Jae Bum Kim, Heon Jeong Lee, Tae Sik Park, and Seung Hoi Koo

Subjects

Male, medicine.medical_specialty, Physiology, Endocrinology, Diabetes and Metabolism, p38 mitogen-activated protein kinases, Drug Evaluation, Preclinical, Biology, Rats, Sprague-Dawley, Mice, Physiology (medical), Internal medicine, Transcriptional regulation, medicine, Animals, Humans, Transcription factor, Beta oxidation, Cells, Cultured, Sterol Regulatory Element Binding Proteins, Adenylate Kinase, AMPK, Lipid metabolism, Hep G2 Cells, Lipid Metabolism, Rats, Sterol regulatory element-binding protein, Mice, Inbred C57BL, Endocrinology, Gene Expression Regulation, Liver, Hepatocytes, Phosphorylation, lipids (amino acids, peptides, and proteins), Antipsychotic Agents

Abstract

Dysregulation of lipid metabolism is a key feature of metabolic disorder related to side effects of antipsychotic drugs. Here, we investigated the molecular mechanism by which second-generation atypical antipsychotic drugs (AAPDs) affect hepatic lipid metabolism in liver. AAPDs augmented hepatic lipid accumulation by activating expression of sterol regulatory element-binding protein (SREBP) transcription factors, with subsequent induction of downstream target genes involved in lipid and cholesterol synthesis in hepatocytes. We confirmed the direct involvement of SREBPs on AAPD-induced expression of lipogenic and cholesterogenic genes by utilization of adenovirus for dominant negative SREBP (Ad-SREBP-DN). Interestingly, AAPDs significantly decreased phosphorylation of AMPKα and expression of fatty acid oxidation genes. Treatment of constitutive active AMPK restored AAPD-mediated dysregulation of genes involved in both lipid synthesis and fatty acid oxidation. Moreover, AAPDs decreased transcriptional activity of PPARα, a critical transcriptional regulator for controlling hepatic fatty acid oxidation, via an AMPK-dependent manner. Close investigations revealed that mutations at the known p38 MAPK phosphorylation sites (S6/12/21A), but not mutations at the putative AMPKα phosphorylation sites (S167/373/453A), block AAPD-dependent reduction of PPARα transcriptional activity, suggesting that p38 MAPK might be also involved in the regulatory pathway as a downstream effector of AAPDs/AMPK. Taken together, these data suggest that AAPD-stimulated hepatic dysregulation of lipid metabolism could result from the inhibition of AMPK activity, and pharmaceutical means to potentiate AMPK activity would contribute to restore hepatic lipid homeostasis that occurs during AAPD treatment.

Published

2011

34. Endoplasmic Reticulum Stress Promotes LIPIN2-Dependent Hepatic Insulin Resistance

Author

Woo Young Seo, Su Sung Kim, Cheol Soo Choi, Young Sil Yoon, Seung Hoi Koo, Yo Na Kim, Dongryeol Ryu, Hye Jin Kim, and Tae Sik Park

Subjects

Blood Glucose, Lipopolysaccharides, Male, medicine.medical_specialty, Chromatin Immunoprecipitation, Thapsigargin, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Blotting, Western, Phosphatidate Phosphatase, Type 2 diabetes, Endoplasmic Reticulum, Polymerase Chain Reaction, chemistry.chemical_compound, Mice, Insulin resistance, Internal medicine, Internal Medicine, medicine, Animals, Obesity, Cells, Cultured, Diacylglycerol kinase, biology, Insulin, Endoplasmic reticulum, Tunicamycin, medicine.disease, Activating Transcription Factor 4, Dietary Fats, Mice, Inbred C57BL, Insulin receptor, Endocrinology, Metabolism, chemistry, Liver, biology.protein, Unfolded protein response, Insulin Resistance

Abstract

OBJECTIVE Diet-induced obesity (DIO) is linked to peripheral insulin resistance—a major predicament in type 2 diabetes. This study aims to identify the molecular mechanism by which DIO-triggered endoplasmic reticulum (ER) stress promotes hepatic insulin resistance in mouse models. RESEARCH DESIGN AND METHODS C57BL/6 mice and primary hepatocytes were used to evaluate the role of LIPIN2 in ER stress-induced hepatic insulin resistance. Tunicamycin, thapsigargin, and lipopolysaccharide were used to invoke acute ER stress conditions. To promote chronic ER stress, mice were fed with a high-fat diet for 8–12 weeks. To verify the role of LIPIN2 in hepatic insulin signaling, adenoviruses expressing wild-type or mutant LIPIN2, and shRNA for LIPIN2 were used in animal studies. Plasma glucose, insulin levels as well as hepatic free fatty acids, diacylglycerol (DAG), and triacylglycerol were assessed. Additionally, glucose tolerance, insulin tolerance, and pyruvate tolerance tests were performed to evaluate the metabolic phenotype of these mice. RESULTS LIPIN2 expression was enhanced in mouse livers by acute ER stress–inducers or by high-fat feeding. Transcriptional activation of LIPIN2 by ER stress is mediated by activating transcription factor 4, as demonstrated by LIPIN2 promoter assays, Western blot analyses, and chromatin immunoprecipitation assays. Knockdown of hepatic LIPIN2 in DIO mice reduced fasting hyperglycemia and improved hepatic insulin signaling. Conversely, overexpression of LIPIN2 impaired hepatic insulin signaling in a phosphatidic acid phosphatase activity–dependent manner. CONCLUSIONS These results demonstrate that ER stress–induced LIPIN2 would contribute to the perturbation of hepatic insulin signaling via a DAG-protein kinase C ε–dependent manner in DIO mice.

Published

2011

35. AMPK-dependent Repression of Hepatic Gluconeogenesis via Disruption of CREB·CRTC2 Complex by Orphan Nuclear Receptor Small Heterodimer Partner

Author

Hueng Sik Choi, Woo Young Seo, Kwang-Hoon Song, Dongryeol Ryu, Yong-Hoon Kim, Dipanjan Chanda, Don Kyu Kim, Seung Hoi Koo, Jung Ran Noh, Chul-Ho Lee, Yong Deuk Kim, Min Woo Lee, Ji Min Lee, and John Y.L. Chiang

Subjects

Recombinant Fusion Proteins, Receptors, Cytoplasmic and Nuclear, AMP-Activated Protein Kinases, Biology, CREB, Biochemistry, Mice, AMP-activated protein kinase, Coactivator, Animals, Humans, Hypoglycemic Agents, Gene Regulation, Cyclic AMP Response Element-Binding Protein, Promoter Regions, Genetic, Molecular Biology, Cells, Cultured, Regulation of gene expression, Gene knockdown, Gluconeogenesis, Cell Biology, Metformin, Rats, Cell biology, CRTC2, Gene Expression Regulation, Nuclear receptor, Glucose-6-Phosphatase, Hepatocytes, Trans-Activators, Cancer research, Small heterodimer partner, biology.protein, Phosphoenolpyruvate Carboxykinase (ATP)

Abstract

Orphan nuclear receptor small heterodimer partner (SHP) plays a key role in transcriptional repression of gluconeogenic enzyme gene expression. Here, we show that SHP inhibited protein kinase A-mediated transcriptional activity of cAMP-response element-binding protein (CREB), a major regulator of glucose metabolism, to modulate hepatic gluconeogenic gene expression. Deletion analysis of phosphoenolpyruvate carboxykinase (PEPCK) promoter demonstrated that SHP inhibited forskolin-mediated induction of PEPCK gene transcription via inhibition of CREB transcriptional activity. In vivo imaging demonstrated that SHP inhibited CREB-regulated transcription coactivator 2 (CRTC2)-mediated cAMP-response element-driven promoter activity. Furthermore, overexpression of SHP using adenovirus SHP decreased CRTC2-dependent elevations in blood glucose levels and PEPCK or glucose-6-phosphatase (G6Pase) expression in mice. SHP and CREB physically interacted and were co-localized in vivo. Importantly, SHP inhibited both wild type CRTC2 and S171A (constitutively active form of CRTC2) coactivator activity and disrupted CRTC2 recruitment on the PEPCK gene promoter. In addition, metformin or overexpression of a constitutively active form of AMPK (Ad-CA-AMPK) inhibited S171A-mediated PEPCK and G6Pase gene expression, and hepatic glucose production and knockdown of SHP partially relieved the metformin- and Ad-CA-AMPK-mediated repression of hepatic gluconeogenic enzyme gene expression in primary rat hepatocytes. In conclusion, our results suggest that a delayed effect of metformin-mediated induction of SHP gene expression inhibits CREB-dependent hepatic gluconeogenesis.

Published

2010

36. The Orphan Nuclear Receptor Estrogen Receptor-related Receptor γ Negatively Regulates BMP2-induced Osteoblast Differentiation and Bone Formation

Author

Yong-Soo Lee, Sun Hun Kim, Seung Hoi Koo, Hueng Sik Choi, Byung Chul Jeong, Renny T. Franceschi, Yun Yong Park, Hong Ran Choi, Don Kyu Kim, Jeong Tae Koh, and In-Ho Bae

Subjects

Transcriptional Activation, musculoskeletal diseases, Bone sialoprotein, medicine.medical_specialty, Cellular differentiation, Bone Morphogenetic Protein 2, Down-Regulation, Core Binding Factor Alpha 1 Subunit, Biology, Biochemistry, Bone morphogenetic protein 2, Cell Line, Mice, Calcification, Physiologic, Osteogenesis, Internal medicine, medicine, Animals, Humans, Transcription, Chromatin, and Epigenetics, Molecular Biology, Osteoblasts, Gene Expression Profiling, Stem Cells, Cell Differentiation, Osteoblast, Cell Biology, Cell biology, RUNX2, medicine.anatomical_structure, Endocrinology, Receptors, Estrogen, Nuclear receptor, Organ Specificity, embryonic structures, Osteocalcin, biology.protein, Estrogen-related receptor gamma, E1A-Associated p300 Protein, Protein Binding

Abstract

Estrogen receptor-related receptor gamma (ERRgamma/ERR3/NR3B3) is a member of the orphan nuclear receptor with important functions in development and homeostasis. Recently it has been reported that ERRalpha is involved in osteoblast differentiation and bone formation. In the present study we examined the role of ERRgamma in osteoblast differentiation. Here, we showed that ERRgamma is expressed in osteoblast progenitors and primary osteoblasts, and its expression is increased temporarily by BMP2. Overexpression of ERRgamma reduced BMP2-induced alkaline phosphatase activity and osteocalcin production as well as calcified nodule formation, whereas inhibition of ERRgamma expression significantly enhanced BMP2-induced osteogenic differentiation and mineralization, suggesting that endogenous ERRgamma plays an important role in osteoblast differentiation. In addition, ERRgamma significantly repressed Runx2 transactivity on osteocalcin and bone sialoprotein promoters. We also observed that ERRgamma physically interacts with Runx2 in vitro and in vivo and competes with p300 to repress Runx2 transactivity. Notably, intramuscular injection of ERRgamma strongly inhibited BMP2-induced ectopic bone formation in a dose-dependent manner. Taken together, these results suggest that ERRgamma is a novel negative regulator of osteoblast differentiation and bone formation via its regulation of Runx2 transactivity.

Published

2009

37. Salt-inducible Kinase Regulates Hepatic Lipogenesis by Controlling SREBP-1c Phosphorylation

Author

Seong-Tae Kim, Woo Young Seo, Young Sil Yoon, Min Woo Lee, and Seung Hoi Koo

Subjects

Molecular Sequence Data, AMP-Activated Protein Kinases, Protein Serine-Threonine Kinases, Biochemistry, Gene Expression Regulation, Enzymologic, Rats, Sprague-Dawley, Mice, AMP-activated protein kinase, Gene expression, Animals, Humans, Amino Acid Sequence, Phosphorylation, Molecular Biology, Cells, Cultured, Regulation of gene expression, Gene knockdown, biology, Kinase, Lipogenesis, Cell Biology, Microarray Analysis, Rats, Metabolism and Bioenergetics, Liver, Hepatocytes, biology.protein, Sterol Regulatory Element Binding Protein 1, lipids (amino acids, peptides, and proteins), Sequence Alignment

Abstract

Liver plays a major role in regulating energy homeostasis in mammals. During feeding conditions, excessive glucose is converted into a preferred storage form of energy sources as triacylglycerol in liver via a collective metabolic pathway termed lipogenesis. Sterol regulatory element-binding protein 1c is a master regulator for this process by activating number of enzyme genes, such as Fasn or Acaca, that are involved in this pathway at the transcriptional level. Here we show that the salt-inducible kinase (SIK) family of proteins regulates the hepatic lipogenesis by modulating SREBP-1c activity. Overexpression of SIK1 inhibits hepatic expression of lipogenic genes, such as Fasn, whereas knockdown of SIK1 in liver greatly enhances their expression. Regulation of the Fasn gene by SIK kinases is mediated at the level of transcription via phosphorylation and inactivation of nuclear SREBP-1c. Among candidate sites for SIK-dependent regulation of SREBP-1c, the serine 329 residue is shown to be a critical regulatory site for SIK-mediated repression of SREBP-1c activity by in vitro kinase assay and reverse transcription-PCR analysis in primary hepatocytes. Finally, reduced hepatic triacylglycerol levels and lipogenic gene expression by adenoviral SIK1 transgenic expression are restored to normal levels by co-infection of mutant SREBP-1c, suggesting that SIK-dependent regulation of hepatic lipogenesis is indeed mediated through the phosphorylation of SREBP-1c in vivo. The process for the development of nonalcoholic fatty liver involves de novo lipogenesis via the activation of SREBP-1c. Modulation of SREBP-1c activity by SIK proteins would provide an attractive means for the regulation of such diseases.

Published

2009

38. Insulin modulates gluconeogenesis by inhibition of the coactivator TORC2

Author

Seung Hoi Koo, Thomas Vargas, Jose E. Heredia, Yi Liu, John R. Yates, Marc Montminy, Susan Hedrick, and Renaud Dentin

Subjects

Male, medicine.medical_specialty, Ubiquitin-Protein Ligases, medicine.medical_treatment, FOXO1, Protein Serine-Threonine Kinases, Biology, Glucagon, Cell Line, Eating, Mice, Internal medicine, Coactivator, Diabetes Mellitus, medicine, Animals, Homeostasis, Humans, Insulin, Glucose homeostasis, Phosphorylation, Protein kinase B, Multidisciplinary, Ubiquitin, Gluconeogenesis, Nuclear Proteins, Fasting, CRTC2, Glucose, Endocrinology, Gene Expression Regulation, Trans-Activators, Protein Processing, Post-Translational, Transcription Factors

Abstract

During feeding, increases in circulating pancreatic insulin inhibit hepatic glucose output through the activation of the Ser/Thr kinase AKT and subsequent phosphorylation of the forkhead transcription factor FOXO1 (refs 1-3). Under fasting conditions, FOXO1 increases gluconeogenic gene expression in concert with the cAMP responsive coactivator TORC2 (refs 4-8). In response to pancreatic glucagon, TORC2 is de-phosphorylated at Ser 171 and transported to the nucleus, in which it stimulates the gluconeogenic programme by binding to CREB. Here we show in mice that insulin inhibits gluconeogenic gene expression during re-feeding by promoting the phosphorylation and ubiquitin-dependent degradation of TORC2. Insulin disrupts TORC2 activity by induction of the Ser/Thr kinase SIK2, which we show here undergoes AKT2-mediated phosphorylation at Ser 358. Activated SIK2 in turn stimulated the Ser 171 phosphorylation and cytoplasmic translocation of TORC2. Phosphorylated TORC2 was degraded by the 26S proteasome during re-feeding through an association with COP1, a substrate receptor for an E3 ligase complex that promoted TORC2 ubiquitination at Lys 628. Because TORC2 protein levels and activity were increased in diabetes owing to a block in TORC2 phosphorylation, our results point to an important role for this pathway in the maintenance of glucose homeostasis.

Published

2007

39. Cyclic AMP Response Element-binding Protein H (CREBH) Mediates the Inhibitory Actions of Tumor Necrosis Factor α in Osteoblast Differentiation by Stimulating Smad1 Degradation*

Author

Won Gu Jang, Sin Hye Oh, Seung Hoi Koo, Don Kyu Kim, Eun Jung Kim, Byung Chul Jeong, Jeong Tae Koh, Hueng Sik Choi, and Hyuck Choi

Subjects

Male, medicine.medical_specialty, Chromatin Immunoprecipitation, Immunology, Blotting, Western, Activating transcription factor, Bone Morphogenetic Protein 2, SMAD, macromolecular substances, Biology, Real-Time Polymerase Chain Reaction, Biochemistry, Bone morphogenetic protein 2, Smad1 Protein, Mice, Osteogenesis, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Bone regeneration, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Transcription factor, Cells, Cultured, Osteoblasts, integumentary system, ATF6, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha, musculoskeletal, neural, and ocular physiology, NF-kappa B, Osteoblast, Cell Differentiation, Cell Biology, 3T3 Cells, Alkaline Phosphatase, Endoplasmic Reticulum Stress, Cell biology, RUNX2, Mice, Inbred C57BL, medicine.anatomical_structure, Endocrinology, nervous system, Proteolysis, Signal Transduction

Abstract

Endoplasmic reticulum (ER) stress transducers, such as old astrocyte specifically induced substance (OASIS) and activating transcription factor 6 (ATF6), which are induced by bone morphogenetic protein 2 (BMP2), regulate bone formation and osteoblast differentiation. Here, we examined the role of cAMP response element-binding protein H (CREBH), a member of the same family of ER membrane-bound basic leucine zipper (bZIP) transcription factors as OASIS and ATF6, in osteoblast differentiation and bone formation. Proinflammatory cytokine TNFα increased CREBH expression by up-regulating the nuclear factor-κB (NF-κB) signaling pathway in osteoblasts, increased the level of N-terminal fragment of CREBH in the nucleus, and inhibited BMP2 induction of osteoblast specific gene expression. Overexpression of CREBH suppressed BMP2-induced up-regulation of the osteogenic markers runt-related transcription factor 2 (Runx2), alkaline phosphatase (ALP), and osteocalcin (OC) in MC3T3-E1 cells and primary osteoblasts, as well as BMP2-induced ALP activity and OC protein production. In contrast, knockdown of CREBH attenuated the inhibitory effect of TNFα on BMP2-induced osteoblast differentiation. Mechanistic studies revealed that CREBH increased the expression of Smad ubiquitination regulatory factor 1 (Smurf1), leading to ubiquitin-dependent degradation of Smad1, whereas knockdown of CREBH inhibited TNFα-mediated degradation of Smad1 by Smurf1. Consistent with these in vitro findings, administration of Ad-CREBH inhibited BMP2-induced ectopic and orthotopic bone formation in vivo. Taken together, these results suggest that CREBH is a novel negative regulator of osteoblast differentiation and bone formation. Background: Severe inflammatory reactions delay wound healing of bone. Results: Tumor necrosis factor α (TNFα) inhibition of osteoblast differentiation is associated with increased cAMP response element-binding protein H (CREBH) and Smurf1 expression. Conclusion: CREBH mediates the inhibitory actions of TNFα in bone regeneration. Significance: CREBH is identified as a new mediator of inflammation-dependent bone degradation and a potential therapeutic target.

Published

2015

40. Vibrio vulnificus Secretes an Insulin-degrading Enzyme That Promotes Bacterial Proliferation in Vivo

Author

Na Young Park, Kun-Soo Kim, Ara Koh, In Hwang Kim, Ji Hyun Lee, Ik Jung Kim, Seung Hoi Koo, Jin-Young Park, Keun-Woo Lee, and Yancheng Wen

Subjects

Blood Glucose, Operon, Host–pathogen interaction, medicine.medical_treatment, Vibrio vulnificus, Biochemistry, Insulysin, Microbiology, Diabetes Mellitus, Experimental, Mice, Mice, Inbred NOD, Insulin-degrading enzyme, medicine, Animals, Humans, Insulin, Molecular Biology, Pathogen, Cell Proliferation, biology, Wild type, Proteolytic enzymes, Cell Biology, Gene Expression Regulation, Bacterial, biology.organism_classification, Disease Models, Animal, Vibrio Infections, Host-Pathogen Interactions, bacteria

Abstract

We describe a novel insulin-degrading enzyme, SidC, that contributes to the proliferation of the human bacterial pathogen Vibrio vulnificus in a mouse model. SidC is phylogenetically distinct from other known insulin-degrading enzymes and is expressed and secreted specifically during host infection. Purified SidC causes a significant decrease in serum insulin levels and an increase in blood glucose levels in mice. A comparison of mice infected with wild type V. vulnificus or an isogenic sidC-deletion strain showed that wild type bacteria proliferated to higher levels. Additionally, hyperglycemia leads to increased proliferation of V. vulnificus in diabetic mice. Consistent with these observations, the sid operon was up-regulated in response to low glucose levels through binding of the cAMP-receptor protein (CRP) complex to a region upstream of the operon. We conclude that glucose levels are important for the survival of V. vulnificus in the host, and that this pathogen uses SidC to actively manipulate host endocrine signals, making the host environment more favorable for bacterial survival and growth.

Published

2015

41. The Kinase LKB1 Mediates Glucose Homeostasis in Liver and Therapeutic Effects of Metformin

Author

Katja A. Lamia, Nabeel Bardeesy, Reuben J. Shaw, Ronald A. DePinho, Marc Montminy, Seung Hoi Koo, Debbie S. Vasquez, and Lewis C. Cantley

Subjects

Blood Glucose, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Mice, Obese, AMP-Activated Protein Kinases, Protein Serine-Threonine Kinases, Article, Small hairpin RNA, Mice, AMP-activated protein kinase, Multienzyme Complexes, Internal medicine, Coactivator, medicine, Animals, Homeostasis, Humans, Hypoglycemic Agents, Glucose homeostasis, Phosphorylation, skin and connective tissue diseases, Protein kinase A, Multidisciplinary, biology, Lipogenesis, Gluconeogenesis, AMPK, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Metformin, CRTC2, Enzyme Activation, Glucose, Endocrinology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Liver, Hyperglycemia, Trans-Activators, biology.protein, Female, HeLa Cells, Signal Transduction, Transcription Factors, medicine.drug

Abstract

The Peutz-Jegher syndrome tumor-suppressor gene encodes a protein-threonine kinase, LKB1, which phosphorylates and activates AMPK [adenosine monophosphate (AMP)–activated protein kinase]. The deletion of LKB1 in the liver of adult mice resulted in a nearly complete loss of AMPK activity. Loss of LKB1 function resulted in hyperglycemia with increased gluconeogenic and lipogenic gene expression. In LKB1-deficient livers, TORC2, a transcriptional coactivator of CREB (cAMP response element–binding protein), was dephosphorylated and entered the nucleus, driving the expression of peroxisome proliferator-activated receptor-γ coactivator 1α (PGC-1α), which in turn drives gluconeogenesis. Adenoviral small hairpin RNA (shRNA) for TORC2 reduced PGC-1α expression and normalized blood glucose levels in mice with deleted liver LKB1, indicating that TORC2 is a critical target of LKB1/AMPK signals in the regulation of gluconeogenesis. Finally, we show that metformin, one of the most widely prescribed type 2 diabetes therapeutics, requires LKB1 in the liver to lower blood glucose levels.

Published

2005

42. PGC-1 promotes insulin resistance in liver through PPAR-α-dependent induction of TRB-3

Author

Hiroaki Satoh, Chih-Hao Lee, Marc Montminy, Rohit N. Kulkarni, Stephan Herzig, Jerrold M. Olefsky, Susan Hedrick, Seung Hoi Koo, and Ronald M. Evans

Subjects

Male, medicine.medical_specialty, Glucose uptake, medicine.medical_treatment, Mice, Obese, Receptors, Cytoplasmic and Nuclear, Peroxisome proliferator-activated receptor, Cell Cycle Proteins, General Biochemistry, Genetics and Molecular Biology, Mice, Insulin resistance, Internal medicine, medicine, Animals, Humans, Rats, Wistar, Protein kinase B, Mice, Knockout, chemistry.chemical_classification, Base Sequence, biology, Insulin, DNA, General Medicine, medicine.disease, Rats, Mice, Inbred C57BL, Insulin receptor, Endocrinology, Diabetes Mellitus, Type 2, Liver, chemistry, Nuclear receptor, TRIB3, biology.protein, RNA Interference, Insulin Resistance, Signal Transduction, Transcription Factors

Abstract

Insulin resistance is a major hallmark in the development of type 2 diabetes, which is characterized by an impaired ability of insulin to inhibit glucose output from the liver and to promote glucose uptake in muscle. The nuclear hormone receptor coactivator PGC-1 (peroxisome proliferator-activated (PPAR)-gamma coactivator-1) has been implicated in the onset of type 2 diabetes. Hepatic PGC-1 expression is elevated in mouse models of this disease, where it promotes constitutive activation of gluconeogenesis and fatty acid oxidation through its association with the nuclear hormone receptors HNF-4 and PPAR-alpha, respectively. Here we show that PGC-1-deficient mice, generated by adenoviral delivery of PGC-1 RNA interference (RNAi) to the liver, experience fasting hypoglycemia. Hepatic insulin sensitivity was enhanced in PGC-1-deficient mice, reflecting in part the reduced expression of the mammalian tribbles homolog TRB-3, a fasting-inducible inhibitor of the serine-threonine kinase Akt/PKB (ref. 6). We show here that, in the liver, TRB-3 is a target for PPAR-alpha. Knockdown of hepatic TRB-3 expression improved glucose tolerance, whereas hepatic overexpression of TRB-3 reversed the insulin-sensitive phenotype of PGC-1-deficient mice. These results indicate a link between nuclear hormone receptor and insulin signaling pathways, and suggest a potential role for TRB-3 inhibitors in the treatment of type 2 diabetes.

Published

2004

43. Systemic autophagy insufficiency compromises adaptation to metabolic stress and facilitates progression from obesity to diabetes

Author

Hong Lim Kim, Yu Mi Lim, Jin Kim, Hae Youn Lee, Wenying Quan, Seung Hoi Koo, Dongryeol Ryu, Hwanju Cheon, Masaaki Komatsu, Myung-Shik Lee, Kyu Yeon Hur, and H.Y. Lim

Subjects

Male, medicine.medical_specialty, General Physics and Astronomy, Inflammation, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, Insulin resistance, Stress, Physiological, Diabetes mellitus, Internal medicine, Autophagy, Diabetes Mellitus, medicine, Animals, Humans, Obesity, Mice, Knockout, Multidisciplinary, Inflammasome, General Chemistry, medicine.disease, Adaptation, Physiological, Mice, Inbred C57BL, Endocrinology, Disease Progression, Female, medicine.symptom, Haploinsufficiency, Flux (metabolism), Intracellular, medicine.drug

Abstract

Despite growing interest in the relationship between autophagy and systemic metabolism, how global changes in autophagy affect metabolism remains unclear. Here we show that mice with global haploinsufficiency of an essential autophagy gene (Atg7(+/-) mice) do not show metabolic abnormalities but develop diabetes when crossed with ob/ob mice. Atg7(+/-) -ob/ob mice show aggravated insulin resistance with increased lipid content and inflammatory changes, suggesting that autophagy haploinsufficiency impairs the adaptive response to metabolic stress. We further demonstrate that intracellular lipid content and insulin resistance after lipid loading are increased as a result of autophagy insufficiency, and provide evidence for increased inflammasome activation in Atg7(+/-) -ob/ob mice. Imatinib or trehalose improves metabolic parameters of Atg7(+/-) -ob/ob mice and enhances autophagic flux. These results suggest that systemic autophagy insufficiency could be a factor in the progression from obesity to diabetes, and autophagy modulators have therapeutic potential against diabetes associated with obesity and inflammation.

Published

2014

44. Arginine Methylation of CRTC2 Is Critical in the Transcriptional Control of Hepatic Glucose Metabolism

Author

Keun-Gyu Park, Seong-Tae Kim, Seung Hoi Koo, Seri Choi, Hye Sook Han, Geon Kang, Chang Yun Jung, Young Sil Yoon, and Dahee Choi

Subjects

Protein-Arginine N-Methyltransferases, medicine.medical_specialty, Transcription, Genetic, Arginine, Carbohydrate metabolism, CREB, Methylation, Biochemistry, Cell Line, Mice, Insulin resistance, Internal medicine, Coactivator, Cyclic AMP, medicine, Transcriptional regulation, Animals, Humans, Obesity, Molecular Biology, biology, Gluconeogenesis, Cell Biology, medicine.disease, CRTC2, Glucose, Endocrinology, Liver, biology.protein, Insulin Resistance, Transcription Factors

Abstract

Fasting glucose homeostasis is maintained in part through cAMP (adenosine 3′,5′-monophosphate)– dependent transcriptional control of hepatic gluconeogenesis by the transcription factor CREB (cAMP response element–binding protein) and its coactivator CRTC2 (CREB-regulated transcriptional coactivator 2). We showed that PRMT6 (protein arginine methyltransferase 6) promotes fasting-induced transcriptional activation of the gluconeogenic program involving CRTC2. Mass spectrometric analysis indicated that PRMT6 associated with CRTC2. In cells, PRMT6 mediated asymmetric dimethylation of multiple arginine residues of CRTC2, which enhanced the association of CRTC2 with CREB on the promoters of gluconeogenic enzyme–encoding genes. In mice, ectopic expression of PRMT6 promoted higher blood glucose concentrations, which were associated with increased expression of genes encoding gluconeogenic factors, whereas knockdown of hepatic PRMT6 decreased fasting glycemia and improved pyruvate tolerance. The abundance of hepatic PRMT6 was increased in mouse models of obesity and insulin resistance, and adenovirus-mediated depletion of PRMT6 restored euglycemia in these mice. We propose that PRMT6 is involved in the regulation of hepatic glucose metabolism in a CRTC2-dependent manner.

Published

2014

45. In Vino Veritas: A Tale of Two Sirt1s?

Author

Marc Montminy and Seung Hoi Koo

Subjects

Male, Aging, endocrine system diseases, Longevity, Administration, Oral, Carbohydrate metabolism, Resveratrol, General Biochemistry, Genetics and Molecular Biology, Mice, chemistry.chemical_compound, Sirtuin 1, Stilbenes, Animals, Homeostasis, Humans, Insulin, Sirtuins, Glucose homeostasis, Obesity, Transcription factor, biology, Biochemistry, Genetics and Molecular Biology(all), food and beverages, Acetylation, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Cell biology, Glucose, Diabetes Mellitus, Type 2, Biochemistry, chemistry, Trans-Activators, biology.protein, NAD+ kinase, Histone deacetylase, Energy Metabolism, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, Transcription Factors

Abstract

Resveratrol increases life span in lower organisms by activating the NAD+-dependent histone deacetylase Sirt1. Studies by Lagouge et al. (2006) and Baur et al. (2006) now show that resveratrol promotes longevity and improves glucose homeostasis in mice by stimulating the Sirt1-mediated deacetylation of the transcriptional coactivator PGC-1α.

Published

2006

46. Ring finger protein20 regulates hepatic lipid metabolism through protein kinase A-dependent sterol regulatory element binding protein1c degradation

Author

Jae Bum Kim, Hagoon Jang, Gha Young Lee, Seung Hoi Koo, Lee Jaeho, and Sung Sik Choe

Subjects

Male, Ubiquitin-Protein Ligases, Nutritional Status, Biology, Article, chemistry.chemical_compound, Steatohepatitis/Metabolic Liver Disease, Mice, Chlorocebus aethiops, Animals, Humans, Protein kinase A, Fatty acid synthesis, Hepatology, Fatty acid metabolism, Catabolism, Protein Stability, Lipid Metabolism, Cyclic AMP-Dependent Protein Kinases, Mice, Mutant Strains, Sterol regulatory element-binding protein, Ubiquitin ligase, Fatty Liver, Mice, Inbred C57BL, Fatty acid synthase, chemistry, Biochemistry, Gene Expression Regulation, Liver, Lipogenesis, COS Cells, biology.protein, Sterol Regulatory Element Binding Protein 1, HeLa Cells

Abstract

Sterol regulatory element binding proteins (SREBPs) play key roles in lipid homeostasis from yeast to humans.1,2 In mammals, three different SREBP isoforms, including SREBP1a, SREBP1c (also known as ADD1), and SREBP2, are encoded by two genes: SREBF1 and SREBF2. SREBP1 regulates fatty acid metabolism, whereas SREBP2 controls cholesterol metabolism.3 When the cellular sterol level is low, SREBP cleavage-activating protein (SCAP) escorts the SREBP precursors from the endoplasmic reticulum (ER) to the Golgi, where SREBPs are cleaved by Site-1 and Site-2 proteases.4 Subsequently, the mature forms of SREBPs are translocated into the nucleus and stimulate the expression of target genes.5,6 SREBP1a and SREBP1c are generated through transcription from alternative promoters and splicing from a single SREBF1 gene. In metabolic tissues such as adipose tissue and liver, SREBP1c is the predominant isoform of SREBP1.1,7 SREBP1c governs de novo lipogenesis by stimulating its target genes, including fatty acid synthase (FASN), acetyl-CoA carboxylase1 (ACC1), steroyl-CoA desaturase1 (SCD1), and long-chain fatty acid elongase (ELOVL6).8–10 Furthermore, SREBP1c is sensitively regulated by nutritional and hormonal changes to achieve energy balance. For example, SREBP1c is suppressed by fasting, whereas SREBP1c is activated by feeding in adipose tissue and liver.11,12 In parallel, the expression of most lipogenic genes, including FASN, ACC1, and SCD1, is also modulated in a fashion analogous to that of nutritionally regulated SREBP1c.12–14 Accordingly, it has been reported that various hormones, such as insulin, glucagon, and adrenaline, participate in the regulation of SREBP1c and its target lipogenic genes.15,16 Insulin, a key postprandial hormone, stimulates the expression and activity of SREBP1c to accommodate anabolic processes, such as fatty acid synthesis, upon feeding.12,17 In contrast, glucagon, a key catabolic hormone, suppresses the activity of SREBP1c in fasting states, leading to a decrease in lipogenesis.18 In the nucleus, mature SREBPs are very unstable and are rapidly degraded by the proteasome.19,20 Previous reports have shown that SREBP1 is phosphorylated by glycogen synthase kinase-3 beta (GSK-3β), which leads to F-box and WD repeat domain-containing7 (FBXW7)-dependent ubiquitination of SREBP1.21,22 However, a recent in vivo study revealed that inhibition of FBXW7 does not alter the expression of SREBP1c or lipogenic genes in the liver.23 Although SREBP1c-mediated lipogenic program in liver is rapidly repressed by nutritional deprivations, the factors that are involved in the suppression of SREBP1c activity during fasting have not been thoroughly characterized. The finding that ring finger protein20 (RNF20) ubiquitin ligase was identified as one of the novel SREBP1c-interating proteins led us to test whether fasting signaling would promote SREBP1c degradation in an RNF20-dependent manner. In this study, we demonstrate that RNF20 promotes polyubiquitination and degradation of SREBP1c. Overexpression of RNF20 represses SREBP1c activity, leading to a decrease in the expression of lipogenic genes. In obese db/db mice, RNF20 overexpression alleviates hepatic steatosis by reducing the lipogenic program by way of SREBP1c down-regulation. Furthermore, activated PKA, a major signaling cascade that mediates the fasting state, induces degradation of SREBP1c by increasing RNF20 expression. Taken together, these data suggest that RNF20 plays a critical role in the regulation of hepatic lipid metabolism by modulating the protein stability and transcriptional activity of SREBP1c during hormonal changes.

Published

2013

47. Smad6 inhibits non-canonical TGF-β1 signalling by recruiting the deubiquitinase A20 to TRAF6

Author

Sung Kyun Lee, Jun Hwan Kim, Jin-Seok Park, Youn Sook Lee, Su Myung Jung, Seung Hoi Koo, Ji-Hyung Lee, Young Sun Oh, Yoe Sik Bae, Seong-Jin Kim, Jin-Young Park, Jae Young Lee, and Seok Hee Park

Subjects

MAP Kinase Kinase 4, Smad6 Protein, medicine.medical_treatment, Ubiquitin-Protein Ligases, Primary Cell Culture, General Physics and Astronomy, Apoptosis, p38 Mitogen-Activated Protein Kinases, General Biochemistry, Genetics and Molecular Biology, Deubiquitinating enzyme, Transforming Growth Factor beta1, Mice, medicine, Animals, Humans, Intestinal Mucosa, Phosphorylation, Tumor Necrosis Factor alpha-Induced Protein 3, TNF Receptor-Associated Factor 6, Multidisciplinary, biology, Intracellular Signaling Peptides and Proteins, Ubiquitination, Epithelial Cells, General Chemistry, MAP Kinase Kinase Kinases, Cell biology, DNA-Binding Proteins, Intestines, Mice, Inbred C57BL, Cysteine Endopeptidases, Signalling, Cytokine, HEK293 Cells, Non canonical, Gene Expression Regulation, Liver, biology.protein, Hepatocytes, Transforming growth factor, Signal Transduction

Abstract

Transforming growth factor (TGF)-beta, a pivotal cytokine involved in a variety of cellular functions, transmits signals through Smad-dependent canonical and Smad-independent noncanonical pathways. In contrast to the canonical TGF-beta pathway, it is unknown how noncanonical TGF-beta pathways are negatively regulated. Here we demonstrate that the inhibitory Smad Smad6, but not Smad7, negatively regulates TGF-beta 1-induced activation of the TRAF6-TAK1-p38 MAPK/JNK pathway, a noncanonical TGF-beta pathway. TGF-beta 1-induced Smad6 abolishes K63-linked polyubiquitination of TRAF6 by recruiting the A20 deubiquitinating enzyme in AML-12 mouse liver cells and primary hepatocytes. In addition, the knockdown of Smad6 or A20 in an animal model or cell culture system maintains TAK1 and p38 MAPK/JNK phosphorylation and increases apoptosis, emphasizing the crucial role of the Smad6-A20 axis in negative regulation of the TGF-beta 1-TRAF6-TAK1-p38 MAPK/JNK pathway. Therefore, our findings provide insight into the molecular mechanisms underlying negative regulation of noncanonical TGF-beta pathways.

Published

2013

48. Hepatic cannabinoid receptor type 1 mediates alcohol-induced regulation of bile acid enzyme genes expression via CREBH

Author

Tiangang Li, Chul-Ho Lee, John Y.L. Chiang, Sung-Hoon Ahn, Seung Hoi Koo, Hueng Sik Choi, Tae Sik Park, Jagannath Misra, Won-Il Jeong, Dipanjan Chanda, Jung Ran Kim, Yong-Hoon Kim, Don Kyu Kim, and Joseph Sang-Il Kwon

Subjects

Male, Anatomy and Physiology, Mouse, medicine.medical_treatment, Gene Expression, lcsh:Medicine, Mice, Receptor, Cannabinoid, CB1, Molecular Cell Biology, Homeostasis, Insulin, Signaling in Cellular Processes, Cyclic AMP Response Element-Binding Protein, lcsh:Science, Cellular Stress Responses, Gene knockdown, Multidisciplinary, Bile acid, Hep G2 Cells, Animal Models, Signaling in Selected Disciplines, Endocannabinoid system, Liver, Organ Specificity, Signal transduction, Research Article, Signal Transduction, Transcriptional Activation, medicine.medical_specialty, medicine.drug_class, Endocrine System, Biology, digestive system, Gene Expression Regulation, Enzymologic, Bile Acids and Salts, Model Organisms, Internal medicine, medicine, Animals, Humans, Cell damage, Ethanol, Endocrine Physiology, lcsh:R, Metabolism, medicine.disease, Mice, Inbred C57BL, Endocrinology, lcsh:Q, Transcriptional Signaling, Insulin Resistance, Physiological Processes, Gene Deletion, Endocannabinoids, Endocrinological Signaling

Abstract

Bile acids concentration in liver is tightly regulated to prevent cell damage. Previous studies have demonstrated that deregulation of bile acid homeostasis can lead to cholestatic liver disease. Recently, we have shown that ER-bound transcription factor Crebh is a downstream effector of hepatic Cb1r signaling pathway. In this study, we have investigated the effect of alcohol exposure on hepatic bile acid homeostasis and elucidated the mediatory roles of Cb1r and Crebh in this process. We found that alcohol exposure or Cb1r-agonist 2-AG treatment increases hepatic bile acid synthesis and serum ALT, AST levels in vivo alongwith significant increase in Crebh gene expression and activation. Alcohol exposure activated Cb1r, Crebh, and perturbed bile acid homeostasis. Overexpression of Crebh increased the expression of key bile acid synthesis enzyme genes via direct binding of Crebh to their promoters, whereas Cb1r knockout and Crebh-knockdown mice were protected against alcohol-induced perturbation of bile acid homeostasis. Interestingly, insulin treatment protected against Cb1r-mediated Crebh-induced disruption of bile acid homeostasis. Furthermore, Crebh expression and activation was found to be markedly increased in insulin resistance conditions and Crebh knockdown in diabetic mice model (db/db) significantly reversed alcohol-induced disruption of bile acid homeostasis. Overall, our study demonstrates a novel regulatory mechanism of hepatic bile acid metabolism by alcohol via Cb1r-mediated activation of Crebh, and suggests that targeting Crebh can be of therapeutic potential in ameliorating alcohol-induced perturbation of bile acid homeostasis.

Published

2013

49. Phosphoenolpyruvate Carboxykinase and Glucose-6-phosphatase Are Required for Steroidogenesis in Testicular Leydig Cells*

Author

Surendar Tadi, Chul-Ho Lee, Yong Hyeon Yim, Ji-Hoon Park, Gi Ryang Kweon, Balachandar Nedumaran, Keesook Lee, Hueng Sik Choi, Gil Tae Gang, Robert A. Harris, Seung Hoi Koo, Ryun Sup Ahn, Seung Won Ahn, and Yong Deuk Kim

Subjects

Male, medicine.medical_specialty, endocrine system, endocrine system diseases, Receptors, Cytoplasmic and Nuclear, AMP-Activated Protein Kinases, Biochemistry, digestive system, Gene Expression Regulation, Enzymologic, Mice, AMP-activated protein kinase, Internal medicine, medicine, Cyclic AMP, Animals, Humans, Gene Regulation, Protein kinase A, Promoter Regions, Genetic, Molecular Biology, Regulation of gene expression, Gene knockdown, Leydig cell, biology, Activator (genetics), DAX-1 Orphan Nuclear Receptor, AMPK, nutritional and metabolic diseases, Leydig Cells, Cell Biology, medicine.anatomical_structure, Endocrinology, biology.protein, Glucose-6-Phosphatase, Phosphoenolpyruvate carboxykinase, hormones, hormone substitutes, and hormone antagonists, Phosphoenolpyruvate Carboxykinase (ATP), HeLa Cells

Abstract

Cyclic AMP (cAMP) induces steroidogenic enzyme gene expression and stimulates testosterone production in Leydig cells. Phosphoenolpyruvate carboxykinase (PEPCK) is expressed in Leydig cells, but its role has not been defined. In this study, we found that PEPCK and glucose-6-phosphatase (Glc-6-Pase) are increased significantly following cAMP treatment of mouse Leydig cells. Moreover, cAMP treatment increased recruitment of the cAMP-response element-binding transcription factor and decreased recruitment of the corepressor DAX-1 on the pepck promoter. Furthermore, cAMP induced an increase in ATP that correlated with a decrease in phospho-AMP-activated protein kinase (AMPK). In contrast, knockdown or inhibition of PEPCK decreased ATP and increased phospho-AMPK. Treatment with an AMPK activator or overexpression of the constitutively active form of AMPK inhibited cAMP-induced steroidogenic enzyme promoter activities and gene expression. Liver receptor homolog-1 (LRH-1) was involved in cAMP-induced steroidogenic enzyme gene expression but was inhibited by AMPK activation in Leydig cells. Additionally, inhibition or knockdown of PEPCK and Glc-6-Pase decreased cAMP-mediated induction of steroidogenic enzyme gene expression and steroidogenesis. Finally, pubertal mouse (8-week-old) testes and human chorionic gonadotropin-induced prepubertal mouse testes showed increased PEPCK and Glc-6-Pase gene expression. Taken together, these results suggest that induction of PEPCK and Glc-6-Pase by cAMP plays an important role in Leydig cell steroidogenesis.

Published

2012

50. Activation of Cannabinoid Receptor Type 1 (Cb1r) Disrupts Hepatic Insulin Receptor Signaling via Cyclic AMP-response Element-binding Protein H (Crebh)-mediated Induction of Lipin1 Gene*

Author

Min Woo Lee, Seung Hoi Koo, Hueng Sik Choi, Yong-Hoon Kim, Don Kyu Kim, Su Yeon Lee, Tae Sik Park, Chul-Ho Lee, and Dipanjan Chanda

Subjects

Transcriptional Activation, Blotting, Western, Phosphatidate Phosphatase, Arachidonic Acids, Protein Kinase C-epsilon, Biology, Biochemistry, Cell Line, Glycerides, Diglycerides, Rats, Sprague-Dawley, Mice, Receptor, Cannabinoid, CB1, Animals, Gene Regulation, Phosphorylation, Protein kinase A, Cyclic AMP Response Element-Binding Protein, Promoter Regions, Genetic, Molecular Biology, Cells, Cultured, Diacylglycerol kinase, Regulation of gene expression, Gene knockdown, Insulin receptor signaling pathway, Reverse Transcriptase Polymerase Chain Reaction, Nuclear Proteins, Cell Biology, Molecular biology, Receptor, Insulin, Rats, Mice, Inbred C57BL, Insulin receptor, Liver, Mutation, biology.protein, lipids (amino acids, peptides, and proteins), RNA Interference, Signal transduction, Endocannabinoids, Signal Transduction

Abstract

Activation of hepatic cannabinoid 1 receptor (Cb1r) signaling has been implicated in the development of phenotypes associated with fatty liver, hypertriglyceridemia, and insulin resistance. In the current study, we have elucidated the critical role of endoplasmic reticulum-bound transcription factor cyclic AMP-response element-binding protein H (Crebh) in mediating activated Cb1r signaling in inducing phosphatidic acid phosphatase Lipin1 gene expression and subsequently deregulating hepatic insulin receptor signaling. Cb1r agonist (2-arachidonoylglycerol (2-AG)) treatment induced Lipin1 gene expression in a Crebh-dependent manner via recruiting CREBH to the endogenous Lipin1 gene promoter. Adenoviral overexpression of Crebh or 2-AG treatment in mice induced Lipin1 gene expression to increase the hepatic diacylglycerol (DAG) level and phosphorylation of protein kinase Cϵ (PKCϵ). This in turn inhibited hepatic insulin receptor signaling. Knockdown of Crebh or Cb1r antagonism attenuated 2-AG-mediated induction of Lipin1 gene expression and decreased DAG production in mouse liver and subsequently restored insulin receptor signaling. Similarly, knockdown of Lipin1 attenuated the 2-AG-induced increase in the DAG level and PKCϵ phosphorylation. Finally, shRNA-mediated knockdown of Crebh partially but significantly blunted Lipin1 expression and the DAG level in db/db mice. These results demonstrate a novel mechanism by which Cb1r signaling induces Lipin1 gene expression and increases DAG production by activating Crebh, thereby deregulating insulin receptor signaling pathway and lipid homeostasis.

Published

2012