Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.

Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.

BACKGROUND:Secretion of insulin and glucagon is triggered by elevated intracellular calcium levels. Although the precise mechanism by which the calcium signal is coupled to insulin and glucagon granule exocytosis is unclear, synaptotagmin-7 has been shown to be a positive regulator of calcium-depend...

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Main Authors: Phing-How Lou, Natalia Gustavsson, Yue Wang, George K Radda, Weiping Han
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3203149?pdf=render
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spelling doaj-0d079fbd1d7948c8b0810451cc6fd9792020-11-24T21:55:53ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-01610e2667110.1371/journal.pone.0026671Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.Phing-How LouNatalia GustavssonYue WangGeorge K RaddaWeiping HanBACKGROUND:Secretion of insulin and glucagon is triggered by elevated intracellular calcium levels. Although the precise mechanism by which the calcium signal is coupled to insulin and glucagon granule exocytosis is unclear, synaptotagmin-7 has been shown to be a positive regulator of calcium-dependent insulin and glucagon secretion, and may function as a calcium sensor for insulin and glucagon granule exocytosis. Deletion of synaptotagmin-7 leads to impaired glucose-stimulated insulin secretion and nearly abolished Ca(2+)-dependent glucagon secretion in mice. Under non-stressed resting state, however, synaptotagmin-7 KO mice exhibit normal insulin level but severely reduced glucagon level. METHODOLOGY/PRINCIPAL FINDINGS:We studied energy expenditure and metabolism in synaptotagmin-7 KO and control mice using indirect calorimetry and biochemical techniques. Synaptotagmin-7 KO mice had lower body weight and body fat content, and exhibited higher oxygen consumption and basal metabolic rate. Respiratory exchange ratio (RER) was lower in synaptotagmin-7 KO mice, suggesting an increased use of lipid in their energy production. Consistent with lower RER, gene expression profiles suggest enhanced lipolysis and increased capacity for fatty acid transport and oxidation in synaptotagmin-7 KO mice. Furthermore, expression of uncoupling protein 3 (UCP3) in skeletal muscle was approximately doubled in the KO mice compared with control mice. CONCLUSIONS:These results show that the lean phenotype in synaptotagmin-7 KO mice was mostly attributed to increased lipolysis and energy expenditure, and suggest that reduced glucagon level may have broad influence on the overall metabolism in the mouse model.http://europepmc.org/articles/PMC3203149?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Phing-How Lou
Natalia Gustavsson
Yue Wang
George K Radda
Weiping Han
spellingShingle Phing-How Lou
Natalia Gustavsson
Yue Wang
George K Radda
Weiping Han
Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
PLoS ONE
author_facet Phing-How Lou
Natalia Gustavsson
Yue Wang
George K Radda
Weiping Han
author_sort Phing-How Lou
title Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
title_short Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
title_full Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
title_fullStr Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
title_full_unstemmed Increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
title_sort increased lipolysis and energy expenditure in a mouse model with severely impaired glucagon secretion.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-01-01
description BACKGROUND:Secretion of insulin and glucagon is triggered by elevated intracellular calcium levels. Although the precise mechanism by which the calcium signal is coupled to insulin and glucagon granule exocytosis is unclear, synaptotagmin-7 has been shown to be a positive regulator of calcium-dependent insulin and glucagon secretion, and may function as a calcium sensor for insulin and glucagon granule exocytosis. Deletion of synaptotagmin-7 leads to impaired glucose-stimulated insulin secretion and nearly abolished Ca(2+)-dependent glucagon secretion in mice. Under non-stressed resting state, however, synaptotagmin-7 KO mice exhibit normal insulin level but severely reduced glucagon level. METHODOLOGY/PRINCIPAL FINDINGS:We studied energy expenditure and metabolism in synaptotagmin-7 KO and control mice using indirect calorimetry and biochemical techniques. Synaptotagmin-7 KO mice had lower body weight and body fat content, and exhibited higher oxygen consumption and basal metabolic rate. Respiratory exchange ratio (RER) was lower in synaptotagmin-7 KO mice, suggesting an increased use of lipid in their energy production. Consistent with lower RER, gene expression profiles suggest enhanced lipolysis and increased capacity for fatty acid transport and oxidation in synaptotagmin-7 KO mice. Furthermore, expression of uncoupling protein 3 (UCP3) in skeletal muscle was approximately doubled in the KO mice compared with control mice. CONCLUSIONS:These results show that the lean phenotype in synaptotagmin-7 KO mice was mostly attributed to increased lipolysis and energy expenditure, and suggest that reduced glucagon level may have broad influence on the overall metabolism in the mouse model.
url http://europepmc.org/articles/PMC3203149?pdf=render
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AT nataliagustavsson increasedlipolysisandenergyexpenditureinamousemodelwithseverelyimpairedglucagonsecretion
AT yuewang increasedlipolysisandenergyexpenditureinamousemodelwithseverelyimpairedglucagonsecretion
AT georgekradda increasedlipolysisandenergyexpenditureinamousemodelwithseverelyimpairedglucagonsecretion
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