Your search keyword '"Andersson, Lotta E."' showing total 8 results

1. Glutamine-Elicited Secretion of Glucagon-Like Peptide 1 Is Governed by an Activated Glutamate Dehydrogenase.

Author

Andersson, Lotta E., Shcherbina, Liliya, Al-Majdoub, Mahmoud, Vishnu, Neelanjan, Arroyo, Claudia Balderas, Carrara, Jonathan Aste, Wollheim, Claes B., Fex, Malin, Mulder, Hindrik, Wierup, Nils, and Spégel, Peter

Subjects

*GLUCOSE metabolism, *GLUTAMINE metabolism, *ANIMAL experimentation, *BIOCHEMISTRY, *BIOLOGICAL models, *CELL lines, *COMPARATIVE studies, *CYTOLOGICAL techniques, *ENZYME inhibitors, *ENZYME-linked immunosorbent assay, *EPITHELIAL cells, *FLAVONOIDS, *GLUTAMIC acid, *INSULIN, *ISLANDS of Langerhans, *PHENOMENOLOGY, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *MITOCHONDRIA, *OXIDOREDUCTASES, *PEPTIDES, *RATS, *RECTAL medication, *RESEARCH, *GLUCAGON-like peptide 1, *EVALUATION research, *CHEMICAL inhibitors, *PHARMACODYNAMICS

Abstract

Glucagon-like peptide 1 (GLP-1), secreted from intestinal L cells, glucose dependently stimulates insulin secretion from β-cells. This glucose dependence prevents hypoglycemia, rendering GLP-1 analogs a useful and safe treatment modality in type 2 diabetes. Although the amino acid glutamine is a potent elicitor of GLP-1 secretion, the responsible mechanism remains unclear. We investigated how GLP-1 secretion is metabolically coupled in L cells (GLUTag) and in vivo in mice using the insulin-secreting cell line INS-1 832/13 as reference. A membrane-permeable glutamate analog (dimethylglutamate [DMG]), acting downstream of electrogenic transporters, elicited similar alterations in metabolism as glutamine in both cell lines. Both DMG and glutamine alone elicited GLP-1 secretion in GLUTag cells and in vivo, whereas activation of glutamate dehydrogenase (GDH) was required to stimulate insulin secretion from INS-1 832/13 cells. Pharmacological inhibition in vivo of GDH blocked secretion of GLP-1 in response to DMG. In conclusion, our results suggest that nonelectrogenic nutrient uptake and metabolism play an important role in L cell stimulus-secretion coupling. Metabolism of glutamine and related analogs by GDH in the L cell may explain why GLP-1 secretion, but not that of insulin, is activated by these secretagogues in vivo. [ABSTRACT FROM AUTHOR]

Published

2018

2. Glycogen metabolism in the glucose-sensing and supply-driven β-cell.

Author

Andersson, Lotta E., Nicholas, Lisa M., Filipsson, Karin, Sun, Jiangming, Medina, Anya, Al-Majdoub, Mahmoud, Fex, Malin, Mulder, Hindrik, and Spégel, Peter

Subjects

*GLYCOGEN synthases, *INSULIN, *ISLANDS of Langerhans, *GLYCOGENOLYSIS, *LABORATORY rodents

Abstract

Glycogen metabolism in β-cells may affect downstream metabolic pathways controlling insulin release. We examined glycogen metabolism in human islets and in the rodent-derived INS-1 832/13 β-cells and found them to express the same isoforms of key enzymes required for glycogen metabolism. Our findings indicate that glycogenesis is insulin-independent but influenced by extracellular glucose concentrations. Levels of glycogen synthase decrease with increasing glucose concentrations, paralleling accumulation of glycogen. We did not find cAMP-elicited glycogenolysis and insulin secretion to be causally related. In conclusion, our results reveal regulated glycogen metabolism in human islets and insulin-secreting cells. Whether glycogen metabolism affects insulin secretion under physiological conditions remains to be determined. [ABSTRACT FROM AUTHOR]

Published

2016

3. Inhibition of the malate-aspartate shuttle in mouse pancreatic islets abolishes glucagon secretion without affecting insulin secretion.

Author

Stamenkovic, Jelena A., Andersson, Lotta E., Adriaenssens, Alice E., Bagge, Annika, Sharoyko, Vladimir V., Gribble, Fiona, Reimann, Frank, Wollheim, Claes B., Mulder, Hindrik, and Spégel, Peter

Subjects

*TYPE 2 diabetes, *PHYSIOLOGICAL effects of insulin, *ISLANDS of Langerhans, *MALATES, *ASPARTATES, *GLUCAGON, *PYRUVATES, *LABORATORY mice, *PHYSIOLOGY

Abstract

Altered secretion of insulin as well as glucagon has been implicated in the pathogenesis of Type 2 diabetes (T2D), but the mechanisms controlling glucagon secretion from α-cells largely remain unresolved. Therefore, we studied the regulation of glucagon secretion from αTC1-6 (αTC1 clone 6) cells and compared it with insulin release from INS-1 832/13 cells. We found that INS-1 832/13 and αTC1-6 cells respectively secreted insulin and glucagon concentration-dependently in response to glucose. In contrast, tight coupling of glycolytic and mitochondrial metabolism was observed only in INS-1 832/13 cells. Although glycolytic metabolism was similar in the two cell lines, TCA (tricarboxylic acid) cycle metabolism, respiration and ATP levels were less glucose-responsive in αTC1-6 cells. Inhibition of the malate–aspartate shuttle, using phenyl succinate (PhS), abolished glucose-provoked ATP production and hormone secretion from αTC1-6 but not INS-1 832/13 cells. Blocking the malate–aspartate shuttle increased levels of glycerol 3-phosphate only in INS-1 832/13 cells. Accordingly, relative expression of constituents in the glycerol phosphate shuttle compared with malate–aspartate shuttle was lower in αTC1-6 cells. Our data suggest that the glycerol phosphate shuttle augments the malate–aspartate shuttle in INS-1 832/13 but not αTC1-6 cells. These results were confirmed in mouse islets, where PhS abrogated secretion of glucagon but not insulin. Furthermore, expression of the rate-limiting enzyme of the glycerol phosphate shuttle was higher in sorted primary β- than in α-cells. Thus, suppressed glycerol phosphate shuttle activity in the α-cell may prevent a high rate of glycolysis and consequently glucagon secretion in response to glucose. Accordingly, pyruvate- and lactate-elicited glucagon secretion remains unaffected since their signalling is independent of mitochondrial shuttles. [ABSTRACT FROM AUTHOR]

Published

2015

4. Characterization of Stimulus-Secretion Coupling in the Human Pancreatic EndoC-βH1 Beta Cell Line.

Author

Andersson, Lotta E., Valtat, Bérengère, Bagge, Annika, Sharoyko, Vladimir V., Nicholls, David G., Ravassard, Philippe, Scharfmann, Raphael, Spégel, Peter, and Mulder, Hindrik

Subjects

*PANCREATIC beta cells, *CELL metabolism, *CELL lines, *GENE expression, *COMPARATIVE studies, *INTRACELLULAR calcium

Abstract

Aims/Hypothesis: Studies on beta cell metabolism are often conducted in rodent beta cell lines due to the lack of stable human beta cell lines. Recently, a human cell line, EndoC-βH1, was generated. Here we investigate stimulus-secretion coupling in this cell line, and compare it with that in the rat beta cell line, INS-1 832/13, and human islets. Methods: Cells were exposed to glucose and pyruvate. Insulin secretion and content (radioimmunoassay), gene expression (Gene Chip array), metabolite levels (GC/MS), respiration (Seahorse XF24 Extracellular Flux Analyzer), glucose utilization (radiometric), lactate release (enzymatic colorimetric), ATP levels (enzymatic bioluminescence) and plasma membrane potential and cytoplasmic Ca2+ responses (microfluorometry) were measured. Metabolite levels, respiration and insulin secretion were examined in human islets. Results: Glucose increased insulin release, glucose utilization, raised ATP production and respiratory rates in both lines, and pyruvate increased insulin secretion and respiration. EndoC-βH1 cells exhibited higher insulin secretion, while plasma membrane depolarization was attenuated, and neither glucose nor pyruvate induced oscillations in intracellular calcium concentration or plasma membrane potential. Metabolite profiling revealed that glycolytic and TCA-cycle intermediate levels increased in response to glucose in both cell lines, but responses were weaker in EndoC-βH1 cells, similar to those observed in human islets. Respiration in EndoC-βH1 cells was more similar to that in human islets than in INS-1 832/13 cells. Conclusions/Interpretation: Functions associated with early stimulus-secretion coupling, with the exception of plasma membrane potential and Ca2+ oscillations, were similar in the two cell lines; insulin secretion, respiration and metabolite responses were similar in EndoC-βH1 cells and human islets. While both cell lines are suitable in vitro models, with the caveat of replicating key findings in isolated islets, EndoC-βH1 cells have the advantage of carrying the human genome, allowing studies of human genetic variants, epigenetics and regulatory RNA molecules. [ABSTRACT FROM AUTHOR]

Published

2015

5. Genotype-based treatment of type 2 diabetes with an α2A-adrenergic receptor antagonist.

Author

Yunzhao Tang, Axelsson, Annika S., Spégel, Peter, Andersson, Lotta E., Mulder, Hindrik, Groop, Leif C., Renström, Erik, and Rosengren, Anders H.

Published

2014

6. Time-resolved metabolomics analysis of β-cells implicates the pentose phosphate pathway in the control of insulin release.

Author

SPÉGEL, Peter, SHAROYKO, Vladimir V., GOEHRING, Isabel, DANIELSSON, Anders P. H., MALMGREN, Siri, NAGORNY, Cecilia L. F., ANDERSSON, Lotta E., KOECK, Thomas, SHARP, Geoffrey W. G., STRAUB, Susanne G., WOLLHEIM, Claes B., and MULDER, Hindrik

Subjects

TYPE 2 diabetes, INSULIN, CELL metabolism, METABOLITES, DEHYDROEPIANDROSTERONE, ISLANDS of Langerhans

Abstract

Insulin secretion is coupled with changes in β-cell metabolism. To define this process, 195 putative metabolites, mitochondrial respiration, NADP+, NADPH and insulin secretion were measured within 15 min of stimulation of clonal INS-1 832/13 β-cells with glucose. Rapid responses in the major metabolic pathways of glucose occurred, involving several previously suggested metabolic coupling factors. The complexity of metabolite changes observed disagreed with the concept of one single metabolite controlling insulin secretion. The complex alterations in metabolite levels suggest that a coupling signal should reflect large parts of the β-cell metabolic response. This was fulfilled by the NADPH/NADP+ ratio, which was elevated (8-fold; P<0.01) at 6 min after glucose stimulation. The NADPH/NADP+ ratio paralleled an increase in ribose 5-phosphate (>2.5-fold; P<0.001). Inhibition of the pentose phosphate pathway by trans-dehydroepiandrosterone (DHEA) suppressed ribose 5-phosphate levels and production of reduced glutathione, as well as insulin secretion in INS-1 832/13 β- cells and rat islets without affecting ATP production. Metabolite profiling of rat islets confirmed the glucose-induced rise in ribose 5-phosphate, which was prevented by DHEA. These findings implicate the pentose phosphate pathway, and support a role for NADPH and glutathione, in β-cell stimulus-secretion coupling. [ABSTRACT FROM AUTHOR]

Published

2013

7. Chronic High Glucose and Pyruvate Levels Differentially Affect Mitochondrial Bioenergetics and Fuel-stimulated Insulin Secretion from Clonal INS-1 832/13 Cells.

Author

Göhring, Isabel, Sharoyko, Vladimir V., Malmgren, Siri, Andersson, Lotta E., Spégel, Peter, Nicholls, David G., and Mulder, Hindrik

Subjects

*BLOOD sugar, *GLUCOSE, *TYPE 2 diabetes, *PYRUVATES, *ORGANIC acids

Abstract

Background: Elevated glucose may cause-cell dysfunction in type 2 diabetes, i.e., glucotoxicity. Results: Elevated glucose, but not pyruvate, perturbed insulin secretion and content, plasma and mitochondrial membrane potentials, and proton leak, while increasing glycolytic metabolites in β-cells. Conclusion: Early metabolism of glucose exerts a toxic effect on clonal insulin-producing cells. Significance: Unraveling these mechanisms may provide protection of β-cells in diabetes. [ABSTRACT FROM AUTHOR]

Published

2014

8. Coordinate Changes in Histone Modifications, mRNA Levels, and Metabolite Profiles in Clonal INS-1 832/13 β-Cells Accompany Functional Adaptations to Lipotoxicity.

Author

Malmgren, Siri, Spégel, Peter, Danielsson, Anders P. H., Nagorny, Cecilia L., Andersson, Lotta E., Dekker Nitert, Marloes, Ridderstråle, Martin, Mulder, Hindrik, and Ling, Charlotte

Subjects

*HISTONES, *MICRORNA, *METABOLITES, *DNA replication, *TYPE 2 diabetes, *BIOCHEMISTRY

Abstract

Lipotoxicity is a presumed pathogenetic process whereby elevated circulating and stored lipids in type 2 diabetes cause pancreatic β-cell failure. To resolve the underlying molecular mechanisms, we exposed clonal INS-1 832/13 β-cells to palmitate for 48 h. We observed elevated basal insulin secretion but impaired glucose-stimulated insulin secretion in palmitate-exposed cells. Glucose utilization was unchanged, palmitate oxidation was increased, and oxygen consumption was impaired. Halting exposure of the clonal INS-1 832/13 β-cells to palmitate largely recovered all of the lipid-induced functional changes. Metabolite profiling revealed profound but reversible increases in cellular lipids. Glucose-induced increases in tricarboxylic acid cycle intermediates were attenuated by exposure to palmitate. Analysis of gene expression by microarray showed increased expression of 982 genes and decreased expression of 1032 genes after exposure to palmitate. Increases were seen in pathways for steroid biosynthesis, cell cycle, fatty acid metabolism, DNA replication, and biosynthesis of unsaturated fatty acids; decreases occurred in the aminoacyl-tRNA synthesis pathway. The activity of histone-modifying enzymes and histone modifications of differentially expressed genes were reversibly altered upon exposure to palmitate. Thus, Insig1, Lss, Peci, Idi1, Hmgcs1, and Casr were subject to epigenetic regulation. Our analyses demonstrate that coordinate changes in histone modifications, mRNA levels, and metabolite profiles accompanied functional adaptations of clonal β-cells to lipotoxicity. It is highly likely that these changes are pathogenetic, accounting for loss of glucose responsiveness and perturbed insulin secretion. [ABSTRACT FROM AUTHOR]

Published

2013