Your search keyword '"Hedrick JA"' showing total 7 results

1. Agonists at GPR119 mediate secretion of GLP-1 from mouse enteroendocrine cells through glucose-independent pathways.

Author

Lan H, Lin HV, Wang CF, Wright MJ, Xu S, Kang L, Juhl K, Hedrick JA, and Kowalski TJ

Subjects

Animals, Calcium metabolism, Cell Line, Colforsin pharmacology, Colon cytology, Endocannabinoids, Enteroendocrine Cells metabolism, Glucose pharmacology, Insulin-Secreting Cells metabolism, Male, Mice, Mice, Inbred C57BL, Oleic Acids pharmacology, Enteroendocrine Cells drug effects, Glucagon-Like Peptide 1 metabolism, Insulin-Secreting Cells drug effects, Receptors, G-Protein-Coupled agonists

Abstract

Background and Purpose: The G protein-coupled receptor 119 (GPR119) mediates insulin secretion from pancreatic β cells and glucagon-like peptide 1 (GLP-1) release from intestinal L cells. While GPR119-mediated insulin secretion is glucose dependent, it is not clear whether or not GPR119-mediated GLP-1 secretion similarly requires glucose. This study was designed to address the glucose-dependence of GPR119-mediated GLP-1 secretion, and to explore the cellular mechanisms of hormone secretion in L cells versus those in β cells., Experimental Approach: GLP-1 secretion in response to GPR119 agonists and ion channel modulators, with and without glucose, was analysed in the intestinal L cell line GLUTag, in primary intestinal cell cultures and in vivo. Insulin secretion from Min6 cells, a pancreatic β cell line, was analysed for comparison., Key Results: In GLUTag cells, GPR119 agonists stimulated GLP-1 secretion both in the presence and in the absence of glucose. In primary mouse colon cultures, GPR119 agonists stimulated GLP-1 secretion under glucose-free conditions. Moreover, a GPR119 agonist increased plasma GLP-1 in mice without a glucose load. However, in Min6 cells, GPR119-mediated insulin secretion was glucose-dependent. Among the pharmacological agents tested in this study, nitrendipine, an L-type voltage-dependent calcium channel blocker, dose-dependently reduced GLP-1 secretion from GLUTag cells, but had no effect in Min6 cells in the absence of glucose., Conclusions and Implications: Unlike that in pancreatic β cells, GPR119-mediated GLP-1 secretion from intestinal L cells was glucose-independent in vitro and in vivo, probably because of a higher basal calcium tone in the L cells., (© 2011 Merck Sharp & Dohme Corp. British Journal of Pharmacology © 2011 The British Pharmacological Society.)

Published

2012

2. Gender-dependent effect of Gpbar1 genetic deletion on the metabolic profiles of diet-induced obese mice.

Author

Vassileva G, Hu W, Hoos L, Tetzloff G, Yang S, Liu L, Kang L, Davis HR, Hedrick JA, Lan H, Kowalski T, and Gustafson EL

Subjects

Animals, Cholesterol blood, Disease Models, Animal, Energy Metabolism genetics, Energy Metabolism physiology, Fatty Liver epidemiology, Female, Incidence, Insulin Resistance genetics, Insulin Resistance physiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Obesity physiopathology, Receptors, G-Protein-Coupled physiology, Risk Factors, Triglycerides blood, Dietary Fats adverse effects, Gene Deletion, Obesity etiology, Obesity metabolism, Receptors, G-Protein-Coupled genetics, Sex Characteristics

Abstract

G-protein-coupled bile acid receptor 1 (GPBAR1/TGR5/M-Bar/GPR131) is a cell surface receptor involved in the regulation of bile acid metabolism. We have previously shown that Gpbar1-null mice are resistant to cholesterol gallstone disease when fed a lithogenic diet. Other published studies have suggested that Gpbar1 is involved in both energy homeostasis and glucose homeostasis. Here, we examine the functional role of Gpbar1 in diet-induced obese mice. We found that body weight, food intake, and fasted blood glucose levels were similar between Gpbar1-null mice and their wild-type (WT) littermates when fed a chow or high-fat diet (HFD) for 2 months. However, insulin tolerance tests revealed improved insulin sensitivity in male Gpbar1(-/-) mice fed chow, but impaired insulin sensitivity when fed a HFD. In contrast, female Gpbar1(-/-) mice exhibited improved insulin sensitivity when fed a HFD compared with their WT littermates. Female Gpbar1(-/-) mice had significantly lower plasma cholesterol and triglyceride levels than their WT littermates on both diets. Male Gpbar1(-/-) mice on HFD displayed increased hepatic steatosis when compared with Gpbar1(+)(/)(+) males and Gpbar1(-/-) females on HFD. These results suggest a gender-dependent regulation of Gpbar1 function in metabolic disease.

Published

2010

3. GPR119 is required for physiological regulation of glucagon-like peptide-1 secretion but not for metabolic homeostasis.

Author

Lan H, Vassileva G, Corona A, Liu L, Baker H, Golovko A, Abbondanzo SJ, Hu W, Yang S, Ning Y, Del Vecchio RA, Poulet F, Laverty M, Gustafson EL, Hedrick JA, and Kowalski TJ

Subjects

Animals, Appetite Regulation drug effects, Appetite Regulation genetics, Cells, Cultured, Endocannabinoids, Female, Gene Targeting, Glucose metabolism, Homeostasis drug effects, Incretins metabolism, Incretins pharmacology, Lipid Metabolism drug effects, Lipid Metabolism genetics, Lysophosphatidylcholines metabolism, Lysophosphatidylcholines pharmacology, Male, Metabolic Networks and Pathways drug effects, Mice, Mice, Inbred C57BL, Mice, Knockout, Oleic Acids metabolism, Oleic Acids pharmacology, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled metabolism, Secretory Pathway drug effects, Glucagon-Like Peptide 1 metabolism, Homeostasis genetics, Metabolic Networks and Pathways genetics, Receptors, G-Protein-Coupled physiology, Secretory Pathway genetics

Abstract

G protein-coupled receptor 119 (GPR119) is expressed in pancreatic islets and intestine, and is involved in insulin and incretin hormone release. GPR119-knockout (Gpr119(-/-)) mice were reported to have normal islet morphology and normal size, body weight (BW), and fed/fasted glucose levels. However, the physiological function of GPR119 and its role in maintaining glucose homeostasis under metabolic stress remain unknown. Here, we report the phenotypes of an independently generated line of Gpr119(-/-) mice under basal and high-fat diet (HFD)-induced obesity. Under low-fat diet feeding, Gpr119(-/-) mice show normal plasma glucose and lipids, but have lower BWs and lower post-prandial levels of active glucagon-like peptide 1 (GLP-1). Nutrient-stimulated GLP-1 release is attenuated in Gpr119(-/-) mice, suggesting that GPR119 plays a role in physiological regulation of GLP-1 secretion. Under HFD-feeding, both Gpr119(+)(/)(+) and Gpr119(-/-) mice gain weight similarly, develop hyperinsulinemia and hyperleptinemia, but not hyperglycemia or dyslipidemia. Glucose and insulin tolerance tests did not reveal a genotypic difference. These data show that GPR119 is not essential for the maintenance of glucose homeostasis. Moreover, we found that oleoylethanolamide (OEA), reported as a ligand for GPR119, was able to suppress food intake in both Gpr119(+)(/)(+) and Gpr119(-/-) mice, indicating that GPR119 is not required for the hypophagic effect of OEA. Our results demonstrate that GPR119 is important for incretin and insulin secretion, but not for appetite suppression.

Published

2009

4. Endogenous and synthetic agonists of GPR119 differ in signalling pathways and their effects on insulin secretion in MIN6c4 insulinoma cells.

Author

Ning Y, O'Neill K, Lan H, Pang L, Shan LX, Hawes BE, and Hedrick JA

Subjects

Acids, Heterocyclic pharmacology, Animals, Calcium metabolism, Calcium Channels metabolism, Cells, Cultured, Cyclic AMP metabolism, Endocannabinoids, Glucose metabolism, Insulin Secretion, KATP Channels metabolism, Lysophosphatidylcholines metabolism, Mice, Oleic Acids metabolism, Oxadiazoles pharmacology, Pyridones pharmacology, Rats, Signal Transduction drug effects, Insulin metabolism, Insulinoma metabolism, Receptors, G-Protein-Coupled agonists

Abstract

Background and Purpose: GPR119 is a G protein-coupled receptor that is preferentially expressed in islet cells and mediates insulin secretion. Oleoyl-lysophosphatidylcholine and oleoylethanolamide (OEA) act as endogenous ligands for this receptor, whereas PSN375963 and PSN632408 are two recently reported synthetic agonists. In this study, we explored mechanisms underlying GPR119-induced insulin secretion. In addition, we assessed the potential utility of the synthetic agonists as tools for exploring GPR119 biology., Experimental Approach: We examined natural and synthetic GPR119 agonist activity at GPR119 in MIN6c4 and RINm5f insulinoma cells. We evaluated insulin secretion, intracellular calcium [Ca(2+)](i), ion channel involvement and levels of cAMP., Key Results: We report that increases in insulin secretion induced by OEA were associated with increased cAMP and a potentiation of glucose-stimulated increases in [Ca(2+)](i). We also demonstrate that ATP-sensitive K(+) and voltage-dependent calcium channels were required for GPR119-mediated increases in glucose-stimulated insulin secretion. In contrast to OEA, the synthetic GPR119 agonist PSN375963 and PSN632408 have divergent effects on insulin secretion, cAMP and intracellular calcium in MIN6c4 cells., Conclusions and Implications: The endogenous ligand OEA signals through GPR119 in a manner similar to glucagon-like peptide-1 (GLP-1) and its receptor with respect to insulin secretion, [Ca(2+)](i) and cAMP. In addition, PSN375963 and PSN632408 substantially differ from OEA and from one another. These studies suggest that the commercially available synthetic agonists, although they do activate GPR119, may also activate GPR119-independent pathways and are thus unsuitable as GPR119-specific pharmacological tools.

Published

2008

5. Lack of FFAR1/GPR40 does not protect mice from high-fat diet-induced metabolic disease.

Author

Lan H, Hoos LM, Liu L, Tetzloff G, Hu W, Abbondanzo SJ, Vassileva G, Gustafson EL, Hedrick JA, and Davis HR

Subjects

Adiposity, Animals, Body Weight physiology, Glucose Tolerance Test, Hyperinsulinism physiopathology, Insulin metabolism, Metabolic Diseases etiology, Metabolic Diseases genetics, Mice, Mice, Knockout, Receptors, G-Protein-Coupled genetics, Dietary Fats administration & dosage, Metabolic Diseases physiopathology, Receptors, G-Protein-Coupled physiology

Abstract

Objective: FFAR1/GPR40 is a G-protein-coupled receptor expressed predominantly in pancreatic islets mediating free fatty acid-induced insulin secretion. However, the physiological role of FFAR1 remains controversial. It was previously reported that FFAR1 knockout (Ffar1(-/-)) mice were resistant to high-fat diet-induced hyperinuslinemia, hyperglycemia, hypertriglyceridemia, and hepatic steatosis. A more recent report suggested that although FFAR1 was necessary for fatty acid-induced insulin secretion in vivo, deletion of FFAR1 did not protect pancreatic islets against fatty acid-induced islet dysfunction. This study is designed to investigate FFAR1 function in vivo using a third line of independently generated Ffar1(-/-) mice in the C57BL/6 background., Research Design and Methods: We used CL-316,243, a beta3 adrenergic receptor agonist, to acutely elevate blood free fatty acids and to study its effect on insulin secretion in vivo. Ffar1(+/+) (wild-type) and Ffar1(-/-) (knockout) mice were placed on two distinct high-fat diets to study their response to diet-induced obesity., Results: Insulin secretion was reduced by approximately 50% in Ffar1(-/-) mice, confirming that FFAR1 contributes significantly to fatty acid stimulation of insulin secretion in vivo. However, Ffar1(+/+) and Ffar1(-/-) mice had similar weight, adiposity, and hyperinsulinemia on high-fat diets, and Ffar1(-/-) mice showed no improvement in glucose or insulin tolerance tests. In addition, high-fat diet induced comparable levels of lipid accumulation in livers of Ffar1(+/+) and Ffar1(-/-) mice., Conclusions: FFAR1 is required for normal insulin secretion in response to fatty acids; however, Ffar1(-/-) mice are not protected from high-fat diet-induced insulin resistance or hepatic steatosis.

Published

2008

6. P518/Qrfp sequence polymorphisms in SAMP6 osteopenic mouse.

Author

Zhang Q, Qiu P, Arreaza MG, Simon JS, Golovko A, Laverty M, Vassileva G, Gustafson EL, Rojas-Triana A, Bober LA, Hedrick JA, Monsma FJ Jr, Greene JR, Bayne ML, and Murgolo NJ

Subjects

Amino Acid Sequence, Animals, Bone Density, Humans, Intercellular Signaling Peptides and Proteins, Ligands, Mice, Mice, Inbred Strains, Molecular Sequence Data, Rats, Sequence Homology, Amino Acid, Tissue Distribution, Bone Diseases, Metabolic genetics, Open Reading Frames genetics, Peptides genetics, Polymorphism, Single Nucleotide genetics, Promoter Regions, Genetic genetics, Quantitative Trait, Heritable, Receptors, G-Protein-Coupled genetics

Abstract

Mice lacking GPR103A expression display osteopenia. Analysis of mouse quantitative trait loci literature associated with bone mineral density suggested GPR103A ligand P518/Qrfp (chromosome 2qB) as a candidate osteoporosis gene. Promoter and coding regions of mouse P518/Qrfp were sequenced from genomic DNA obtained from the osteoporosis-prone strain SAMP6 and control strains SAMR1, A/J, AKR/J, BALB/c, C3H/HeJ, C57BL/6J, and DBA/2J. Four single-nucleotide polymorphisms (SNPs) were identified in only SAMP6 genomic DNA, g.-1773 T-->C, g.110 A-->G (N37S), g.188 G-->A (R63K), and g.135 T-->C (H45H). The promoter SNP generated a novel neuron-restrictive silencing factor binding site, a repressor that decreases gene expression in nonneuronal tissues. TaqMan analysis demonstrated fivefold lower P518/Qrfp liver expression in SAMP6 versus SAMR1 or C57BL/6J control strains. Tissue distribution of human, mouse, and rat P518/Qrfp and its receptors showed expression in bone and spinal cord. A direct role for P518/Qrfp function in maintaining bone mineral density is suggested.

Published

2007

7. Identification of viral macrophage inflammatory protein (vMIP)-II as a ligand for GPR5/XCR1.

Author

Shan L, Qiao X, Oldham E, Catron D, Kaminski H, Lundell D, Zlotnik A, Gustafson E, and Hedrick JA

Subjects

Animals, Base Sequence, Calcium metabolism, Cell Line, Cloning, Molecular, DNA Primers genetics, Gene Expression, Humans, Ligands, Lymphokines metabolism, Mice, Receptors, Cell Surface genetics, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sialoglycoproteins metabolism, Tissue Distribution, Chemokines metabolism, Chemokines, C, Macrophage Inflammatory Proteins metabolism, Membrane Proteins, Receptors, Cell Surface metabolism, Receptors, G-Protein-Coupled, Viral Proteins metabolism

Abstract

Lymphotactin is unique among chemokines in that it contains only two of four conserved cysteines and may possess a structure less constrained than other chemokines. The viral chemokine vMIP-II, which presumably has a structure similar to that of CC chemokines has been shown to inhibit many chemokine receptors, but its activity at GPR5/XCR1 has not been described. Interestingly, vMIP-II (but not vMIP-I) was found to be a potent antagonist of lymphotactin activity at GPR5/XCR1, extending the range of chemokine classes that this viral protein is known to inhibit to include the C class chemokine. In addition, we have extended previous analyses of GPR5/XCR1 expression and show that this receptor is expressed in leukocyte cells previously shown to be responsive to lymphotactin., (Copyright 2000 Academic Press.)

Published

2000