Defective insulin secretory response to intravenous glucose in C57Bl/6J compared to C57Bl/6N mice

Fergusson, Grace; Ethier, Mélanie; Guévremont, Mélanie; Chrétien, Chloé; Attané, Camille; Joly, Etienne; Fioramonti, Xavier; Prentki, Marc; Poitout, Vincent; Alquier, Thierry

doi:10.1016/j.molmet.2014.09.006

Cited by 82 publications

(97 citation statements)

References 29 publications

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“…One-step hyperglycemic clamps were performed on conscious animals as previously described (29). A 20% dextrose solution was infused through the jugular vein to clamp plasma glucose at approximately 350 mg/dL for 60 minutes and was adjusted based on glucose measurements (Roche Accu-Check; Roche).…”

Section: Assessment Of Insulin Secretion By Hyperglycemic Clampmentioning

confidence: 99%

An Acetate-Specific GPCR, FFAR2, Regulates Insulin Secretion

Priyadarshini

Villa

Fuller

et al. 2015

Molecular Endocrinology

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G protein-coupled receptors have been well described to contribute to the regulation of glucose-stimulated insulin secretion (GSIS). The short-chain fatty acid-sensing G protein-coupled receptor, free fatty acid receptor 2 (FFAR2), is expressed in pancreatic β-cells, and in rodents, its expression is altered during insulin resistance. Thus, we explored the role of FFAR2 in regulating GSIS. First, assessing the phenotype of wild-type and Ffar2(-/-) mice in vivo, we observed no differences with regard to glucose homeostasis on normal or high-fat diet, with a marginally significant defect in insulin secretion in Ffar2(-/-) mice during hyperglycemic clamps. In ex vivo insulin secretion studies, we observed diminished GSIS from Ffar2(-/-) islets relative to wild-type islets under high-glucose conditions. Further, in the presence of acetate, the primary endogenous ligand for FFAR2, we observed FFAR2-dependent potentiation of GSIS, whereas FFAR2-specific agonists resulted in either potentiation or inhibition of GSIS, which we found to result from selective signaling through either Gαq/11 or Gαi/o, respectively. Lastly, in ex vivo insulin secretion studies of human islets, we observed that acetate and FFAR2 agonists elicited different signaling properties at human FFAR2 than at mouse FFAR2. Taken together, our studies reveal that FFAR2 signaling occurs by divergent G protein pathways that can selectively potentiate or inhibit GSIS in mouse islets. Further, we have identified important differences in the response of mouse and human FFAR2 to selective agonists, and we suggest that these differences warrant consideration in the continued investigation of FFAR2 as a novel type 2 diabetes target.

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Section: Assessment Of Insulin Secretion By Hyperglycemic Clampmentioning

confidence: 99%

An Acetate-Specific GPCR, FFAR2, Regulates Insulin Secretion

Priyadarshini

Villa

Fuller

et al. 2015

Molecular Endocrinology

Self Cite

156

205

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“…On the other hand, NNT deficiency had the opposite effect; with very little CORT secretion because of adrenal cortex dysfunction (31), NNT deficiency was associated with severe hyperglycemia. Peripheral insulin resistance and impaired insulin secretion likely contribute to this effect (29,33) and could explain why psychological stress during the Trier social stress test (TSST) in humans preferentially favors hyperglycemia in those with preexisting diabetes and insulin resistance (49). Furthermore, stress-related cortisol levels also exhibit racial and ethnic differences (50), although the underlying mechanisms remain unclear.…”

Section: Discussionmentioning

confidence: 99%

“…On the other hand, although NNT deficiency was associated with hypocortisolemia, it caused the most severe hyperglycemic response to stress (Fig. 4A), possibly as a result of impaired insulin secretion and action (33). Because stress-induced CORT and glucose increases were measured concurrently, we could analyze their relationships as representing an aspect of the organism's sensitivity to CORT.…”

Section: Normal Function Mtdnamentioning

confidence: 99%

Mitochondrial functions modulate neuroendocrine, metabolic, inflammatory, and transcriptional responses to acute psychological stress

Picard

McManus

Gray

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

220

155

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The experience of psychological stress triggers neuroendocrine, inflammatory, metabolic, and transcriptional perturbations that ultimately predispose to disease. However, the subcellular determinants of this integrated, multisystemic stress response have not been defined. Central to stress adaptation is cellular energetics, involving mitochondrial energy production and oxidative stress. We therefore hypothesized that abnormal mitochondrial functions would differentially modulate the organism's multisystemic response to psychological stress. By mutating or deleting mitochondrial genes encoded in the mtDNA [NADH dehydrogenase 6 (ND6) and cytochrome c oxidase subunit I (COI)] or nuclear DNA [adenine nucleotide translocator 1 (ANT1) and nicotinamide nucleotide transhydrogenase (NNT)], we selectively impaired mitochondrial respiratory chain function, energy exchange, and mitochondrial redox balance in mice. The resulting impact on physiological reactivity and recovery from restraint stress were then characterized. We show that mitochondrial dysfunctions altered the hypothalamicpituitary-adrenal axis, sympathetic adrenal-medullary activation and catecholamine levels, the inflammatory cytokine IL-6, circulating metabolites, and hippocampal gene expression responses to stress. Each mitochondrial defect generated a distinct whole-body stressresponse signature. These results demonstrate the role of mitochondrial energetics and redox balance as modulators of key pathophysiological perturbations previously linked to disease. This work establishes mitochondria as stress-response modulators, with implications for understanding the mechanisms of stress pathophysiology and mitochondrial diseases. stress reactivity | mitochondria | HPA axis | catecholamines | hippocampus R epeated exposure to psychological stress can predispose to disease (1, 2). The underlying mechanisms involve dysregulation of peripheral stress response elements including the hypothalamic-pituitary-adrenal (HPA) axis and glucocorticoids (3), the sympathetic adrenal-medullary (SAM) axis and catecholamines (4), systemic inflammation (5), and the "diabetic-like" state of excess circulating glucose and lipids (i.e., metabolic oversupply) promoted by stress hormones (6, 7). In addition, stress leads to neuronal remodeling, which involves changes in brain gene expression, particularly within the hippocampus (8, 9). However, the subcellular factors that modify these systemic responses to stress have not been defined. The objective of this study was to determine if mitochondria mediate physiological stress responses in mice.Mitochondria are symbiotic organelles that contain their own genetic material, the mtDNA, which encodes essential subunits of the respiratory chain complexes I, III, IV, and V. At complex I, electrons derived from energetic substrates (glucose and lipids) enter the respiratory chain and travel to complex IV, where they are combined with oxygen to produce energy in the form of ATP required for life (10). ATP generated inside mitochondria then is ex...

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“…The differences between our results may be related to the genetic background of the mice (C57BL/6J vs. C57BL/6N used in this study) and/or the prevention of acidosis in our study. C57BL/6J mice carry a mutation in nicotinamide nucleotide transhydrogenase, a mitochondrial enzyme involved in NADPH production, and have reduced insulin secretion relative to that seen in the C57BL/6N strain, without changes in insulin sensitivity (77). Furthermore, overproduction of H 2 O 2 , indicative of alterations in NADPH-dependent oxidases, plays a critical role in urea-induced insulin resistance in adipocytes (15).…”

Section: Metabolic Studiesmentioning

confidence: 99%

Urea impairs β cell glycolysis and insulin secretion in chronic kidney disease

Koppe¹,

Nyam²,

Vivot³

et al. 2016

Journal of Clinical Investigation

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of the Rodent Metabolic Phenotyping core facility of the CRCHUM for metabolic studies in mice; M. Guévremont, J. Morin, and the Cellular Physiology Service core of the CRCHUM for quantification of β cell mass and αLISA assay; C. Tremblay (CRCHUM) for valuable technical assistance; E. Joly for technical advice; and M. Ferdaoussi for fruitful discussions.Address correspondence to: Vincent Poitout, CRCHUM, 900 Saint-Denis Street, Montreal, Quebec, H2X 0A9, Canada. Phone: 514.890.8044; E-mail: vincent.poitout@umontreal.ca.the CHUM (protocols ND-05-035 and 16-048, respectively). Written consent for research was obtained from all donors.

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Defective insulin secretory response to intravenous glucose in C57Bl/6J compared to C57Bl/6N mice

Cited by 82 publications

References 29 publications

An Acetate-Specific GPCR, FFAR2, Regulates Insulin Secretion

An Acetate-Specific GPCR, FFAR2, Regulates Insulin Secretion

Mitochondrial functions modulate neuroendocrine, metabolic, inflammatory, and transcriptional responses to acute psychological stress

Urea impairs β cell glycolysis and insulin secretion in chronic kidney disease

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