Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells

Type 2 diabetes mellitus (T2DM) has been associated with insulin resistance and the failure of β-cells to produce and secrete enough insulin as the disease progresses. However, clinical treatments based solely on insulin secretion and action have had limited success. The focus is therefore shifting...

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Autores principales: Grubelnik, Vladimir, Markovič, Rene, Lipovšek, Saška, Leitinger, Gerd, Gosak, Marko, Dolenšek, Jurij, Valladolid-Acebes, Ismael, Berggren, Per-Olof, Stožer, Andraž, Perc, Matjaž, Marhl, Marko
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society 2020
Materias:
Physics and Biophysics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7029933/
https://www.ncbi.nlm.nih.gov/pubmed/32218947
http://dx.doi.org/10.1098/rsos.191171
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author Grubelnik, Vladimir
Markovič, Rene
Lipovšek, Saška
Leitinger, Gerd
Gosak, Marko
Dolenšek, Jurij
Valladolid-Acebes, Ismael
Berggren, Per-Olof
Stožer, Andraž
Perc, Matjaž
Marhl, Marko
author_facet Grubelnik, Vladimir
Markovič, Rene
Lipovšek, Saška
Leitinger, Gerd
Gosak, Marko
Dolenšek, Jurij
Valladolid-Acebes, Ismael
Berggren, Per-Olof
Stožer, Andraž
Perc, Matjaž
Marhl, Marko
author_sort Grubelnik, Vladimir
collection PubMed
description Type 2 diabetes mellitus (T2DM) has been associated with insulin resistance and the failure of β-cells to produce and secrete enough insulin as the disease progresses. However, clinical treatments based solely on insulin secretion and action have had limited success. The focus is therefore shifting towards α-cells, in particular to the dysregulated secretion of glucagon. Our qualitative electron-microscopy-based observations gave an indication that mitochondria in α-cells are altered in Western-diet-induced T2DM. In particular, α-cells extracted from mouse pancreatic tissue showed a lower density of mitochondria, a less expressed matrix and a lower number of cristae. These deformities in mitochondrial ultrastructure imply a decreased efficiency in mitochondrial ATP production, which prompted us to theoretically explore and clarify one of the most challenging problems associated with T2DM, namely the lack of glucagon secretion in hypoglycaemia and its oversecretion at high blood glucose concentrations. To this purpose, we constructed a novel computational model that links α-cell metabolism with their electrical activity and glucagon secretion. Our results show that defective mitochondrial metabolism in α-cells can account for dysregulated glucagon secretion in T2DM, thus improving our understanding of T2DM pathophysiology and indicating possibilities for new clinical treatments.
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spelling pubmed-70299332020-03-26 Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells Grubelnik, Vladimir Markovič, Rene Lipovšek, Saška Leitinger, Gerd Gosak, Marko Dolenšek, Jurij Valladolid-Acebes, Ismael Berggren, Per-Olof Stožer, Andraž Perc, Matjaž Marhl, Marko R Soc Open Sci Physics and Biophysics Type 2 diabetes mellitus (T2DM) has been associated with insulin resistance and the failure of β-cells to produce and secrete enough insulin as the disease progresses. However, clinical treatments based solely on insulin secretion and action have had limited success. The focus is therefore shifting towards α-cells, in particular to the dysregulated secretion of glucagon. Our qualitative electron-microscopy-based observations gave an indication that mitochondria in α-cells are altered in Western-diet-induced T2DM. In particular, α-cells extracted from mouse pancreatic tissue showed a lower density of mitochondria, a less expressed matrix and a lower number of cristae. These deformities in mitochondrial ultrastructure imply a decreased efficiency in mitochondrial ATP production, which prompted us to theoretically explore and clarify one of the most challenging problems associated with T2DM, namely the lack of glucagon secretion in hypoglycaemia and its oversecretion at high blood glucose concentrations. To this purpose, we constructed a novel computational model that links α-cell metabolism with their electrical activity and glucagon secretion. Our results show that defective mitochondrial metabolism in α-cells can account for dysregulated glucagon secretion in T2DM, thus improving our understanding of T2DM pathophysiology and indicating possibilities for new clinical treatments. The Royal Society 2020-01-22 /pmc/articles/PMC7029933/ /pubmed/32218947 http://dx.doi.org/10.1098/rsos.191171 Text en © 2020 The Authors. http://creativecommons.org/licenses/by/4.0/ Published by the Royal Society under the terms of the Creative Commons Attribution License http://creativecommons.org/licenses/by/4.0/, which permits unrestricted use, provided the original author and source are credited.
spellingShingle Physics and Biophysics
Grubelnik, Vladimir
Markovič, Rene
Lipovšek, Saška
Leitinger, Gerd
Gosak, Marko
Dolenšek, Jurij
Valladolid-Acebes, Ismael
Berggren, Per-Olof
Stožer, Andraž
Perc, Matjaž
Marhl, Marko
Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title_full Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title_fullStr Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title_full_unstemmed Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title_short Modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
title_sort modelling of dysregulated glucagon secretion in type 2 diabetes by considering mitochondrial alterations in pancreatic α-cells
topic Physics and Biophysics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7029933/
https://www.ncbi.nlm.nih.gov/pubmed/32218947
http://dx.doi.org/10.1098/rsos.191171
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