In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload

Alterations in the metabolism of substrates such as glucose are integrally linked to the structural and functional changes that occur in the remodeling heart. Assessment of such metabolic changes under in vivo conditions would provide important insights into this interrelationship. We aimed to inves...

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Autores principales: Schnelle, Moritz, Chong, Mei, Zoccarato, Anna, Elkenani, Manar, Sawyer, Greta Jane, Hasenfuss, Gerd, Ludwig, Christian, Shah, Ajay M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Physiological Society 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7473922/
https://www.ncbi.nlm.nih.gov/pubmed/32648823
http://dx.doi.org/10.1152/ajpheart.00219.2020
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author Schnelle, Moritz
Chong, Mei
Zoccarato, Anna
Elkenani, Manar
Sawyer, Greta Jane
Hasenfuss, Gerd
Ludwig, Christian
Shah, Ajay M.
author_facet Schnelle, Moritz
Chong, Mei
Zoccarato, Anna
Elkenani, Manar
Sawyer, Greta Jane
Hasenfuss, Gerd
Ludwig, Christian
Shah, Ajay M.
author_sort Schnelle, Moritz
collection PubMed
description Alterations in the metabolism of substrates such as glucose are integrally linked to the structural and functional changes that occur in the remodeling heart. Assessment of such metabolic changes under in vivo conditions would provide important insights into this interrelationship. We aimed to investigate glucose carbon metabolism in pressure-overload and volume-overload cardiac hypertrophy by using an in vivo [U-(13)C]glucose labeling strategy to enable analyses of the metabolic fates of glucose carbons in the mouse heart. Therefore, [U-(13)C]glucose was administered in anesthetized mice by tail vein infusion, and the optimal duration of infusion was established. Hearts were then excised for (13)C metabolite isotopomer analysis by NMR spectroscopy. [U-(13)C]glucose infusions were performed in mice 2 wk following transverse aortic constriction (TAC) or aortocaval fistula (Shunt) surgery. At this time point, there were similar increases in left ventricular (LV) mass in both groups, but TAC resulted in concentric hypertrophy with impaired LV function, whereas Shunt caused eccentric hypertrophy with preserved LV function. TAC was accompanied by significant changes in glycolysis, mitochondrial oxidative metabolism, glucose metabolism to anaplerotic substrates, and de novo glutamine synthesis. In contrast to TAC, hardly any metabolic changes could be observed in the Shunt group. Taken together, in vivo [U-(13)C]glucose labeling is a valuable method to investigate the fate of nutrients such as glucose in the remodeling heart. We find that concentric and eccentric cardiac remodeling are accompanied by distinct differences in glucose carbon metabolism. NEW & NOTEWORTHY This study implemented a method for assessing the fate of glucose carbons in the heart in vivo and used this to demonstrate that pressure and volume overload are associated with distinct changes. In contrast to volume overload, pressure overload-induced changes affect the tricarboxylic acid cycle, glycolytic pathways, and glutamine synthesis. A better understanding of cardiac glucose metabolism under pathological conditions in vivo may provide new therapeutic strategies specific for different types of hemodynamic overload. Listen to this article’s corresponding podcast at: https://ajpheart.podbean.com/e/u-13c-glucose-and-in-vivo-heart-metabolism/.
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spelling pubmed-74739222021-08-01 In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload Schnelle, Moritz Chong, Mei Zoccarato, Anna Elkenani, Manar Sawyer, Greta Jane Hasenfuss, Gerd Ludwig, Christian Shah, Ajay M. Am J Physiol Heart Circ Physiol Research Article Alterations in the metabolism of substrates such as glucose are integrally linked to the structural and functional changes that occur in the remodeling heart. Assessment of such metabolic changes under in vivo conditions would provide important insights into this interrelationship. We aimed to investigate glucose carbon metabolism in pressure-overload and volume-overload cardiac hypertrophy by using an in vivo [U-(13)C]glucose labeling strategy to enable analyses of the metabolic fates of glucose carbons in the mouse heart. Therefore, [U-(13)C]glucose was administered in anesthetized mice by tail vein infusion, and the optimal duration of infusion was established. Hearts were then excised for (13)C metabolite isotopomer analysis by NMR spectroscopy. [U-(13)C]glucose infusions were performed in mice 2 wk following transverse aortic constriction (TAC) or aortocaval fistula (Shunt) surgery. At this time point, there were similar increases in left ventricular (LV) mass in both groups, but TAC resulted in concentric hypertrophy with impaired LV function, whereas Shunt caused eccentric hypertrophy with preserved LV function. TAC was accompanied by significant changes in glycolysis, mitochondrial oxidative metabolism, glucose metabolism to anaplerotic substrates, and de novo glutamine synthesis. In contrast to TAC, hardly any metabolic changes could be observed in the Shunt group. Taken together, in vivo [U-(13)C]glucose labeling is a valuable method to investigate the fate of nutrients such as glucose in the remodeling heart. We find that concentric and eccentric cardiac remodeling are accompanied by distinct differences in glucose carbon metabolism. NEW & NOTEWORTHY This study implemented a method for assessing the fate of glucose carbons in the heart in vivo and used this to demonstrate that pressure and volume overload are associated with distinct changes. In contrast to volume overload, pressure overload-induced changes affect the tricarboxylic acid cycle, glycolytic pathways, and glutamine synthesis. A better understanding of cardiac glucose metabolism under pathological conditions in vivo may provide new therapeutic strategies specific for different types of hemodynamic overload. Listen to this article’s corresponding podcast at: https://ajpheart.podbean.com/e/u-13c-glucose-and-in-vivo-heart-metabolism/. American Physiological Society 2020-08-01 2020-07-10 /pmc/articles/PMC7473922/ /pubmed/32648823 http://dx.doi.org/10.1152/ajpheart.00219.2020 Text en Copyright © 2020 the American Physiological Society http://creativecommons.org/licenses/by/4.0/deed.en_US Licensed under Creative Commons Attribution CC-BY 4.0 (http://creativecommons.org/licenses/by/4.0/deed.en_US) : © the American Physiological Society.
spellingShingle Research Article
Schnelle, Moritz
Chong, Mei
Zoccarato, Anna
Elkenani, Manar
Sawyer, Greta Jane
Hasenfuss, Gerd
Ludwig, Christian
Shah, Ajay M.
In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title_full In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title_fullStr In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title_full_unstemmed In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title_short In vivo [U-(13)C]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
title_sort in vivo [u-(13)c]glucose labeling to assess heart metabolism in murine models of pressure and volume overload
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7473922/
https://www.ncbi.nlm.nih.gov/pubmed/32648823
http://dx.doi.org/10.1152/ajpheart.00219.2020
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