Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice

Destruction of the insulin-producing β-cells is the key determinant of diabetes mellitus regardless of their types. Due to their anatomical location within the islets of Langerhans scattered throughout the pancreas, it is difficult to monitor β-cell function and mass clinically. To this end, we prop...

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Autores principales: Brenner, Michael, Abadi, Sakineh Esmaeili Mohsen, Balouchzadeh, Ramin, Lee, H. Felix, Ko, Hoo Sang, Johns, Michael, Malik, Nehal, Lee, Joshua J., Kwon, Guim
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2017
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5463011/
https://www.ncbi.nlm.nih.gov/pubmed/28626803
http://dx.doi.org/10.1016/j.heliyon.2017.e00310
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author Brenner, Michael
Abadi, Sakineh Esmaeili Mohsen
Balouchzadeh, Ramin
Lee, H. Felix
Ko, Hoo Sang
Johns, Michael
Malik, Nehal
Lee, Joshua J.
Kwon, Guim
author_facet Brenner, Michael
Abadi, Sakineh Esmaeili Mohsen
Balouchzadeh, Ramin
Lee, H. Felix
Ko, Hoo Sang
Johns, Michael
Malik, Nehal
Lee, Joshua J.
Kwon, Guim
author_sort Brenner, Michael
collection PubMed
description Destruction of the insulin-producing β-cells is the key determinant of diabetes mellitus regardless of their types. Due to their anatomical location within the islets of Langerhans scattered throughout the pancreas, it is difficult to monitor β-cell function and mass clinically. To this end, we propose to use a mathematical model of glucose-insulin homeostasis to estimate insulin secretion, glucose uptake by tissues, and hepatic handling of glucose. We applied the mathematical model by Lombarte et al. (2013) to compare various rate constants representing glucose-insulin homeostasis between lean (11% fat)- and high fat diet (HFD; 45% fat)-fed mice. Mice fed HFD (n = 12) for 3 months showed significantly higher body weights (49.97 ± 0.52 g vs. 29.86 ± 0.46 g), fasting blood glucose levels (213.08 ± 10.35 mg/dl vs. 121.91 ± 2.26 mg/dl), and glucose intolerance compared to mice fed lean diet (n = 12). Mice were injected with 1 g/kg glucose intraperitoneally and blood glucose levels were measured at various intervals for 120 min. We performed simulation using Arena™ software based on the mathematical model and estimated the rate constants (9 parameters) for various terms in the differential equations using OptQuest™. The simulated data fit accurately to the observed data for both lean and obese mice, validating the use of the mathematical model in mice at different stages of diabetes progression. Among 9 parameters, 5 parameters including basal insulin, k(2) (rate constant for insulin-dependent glucose uptake to tissues), k(3) (rate constant for insulin-independent glucose uptake to tissues), k(4) (rate constant for liver glucose transfer), and I(pi) (rate constant for insulin concentration where liver switches from glucose release to uptake) were significantly different between lean- and HFD-fed mice. Basal blood insulin levels, k(3), and I(pi) were significantly elevated but k(2) and k(4) were reduced in mice fed a HFD compared to those fed a lean diet. Non-invasive assessment of the key components of glucose-insulin homeostasis including insulin secretion, glucose uptake by tissues, and hepatic handling of glucose may be helpful for individualized drug therapy and designing a customized control algorithm for the artificial pancreas.
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spelling pubmed-54630112017-06-16 Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice Brenner, Michael Abadi, Sakineh Esmaeili Mohsen Balouchzadeh, Ramin Lee, H. Felix Ko, Hoo Sang Johns, Michael Malik, Nehal Lee, Joshua J. Kwon, Guim Heliyon Article Destruction of the insulin-producing β-cells is the key determinant of diabetes mellitus regardless of their types. Due to their anatomical location within the islets of Langerhans scattered throughout the pancreas, it is difficult to monitor β-cell function and mass clinically. To this end, we propose to use a mathematical model of glucose-insulin homeostasis to estimate insulin secretion, glucose uptake by tissues, and hepatic handling of glucose. We applied the mathematical model by Lombarte et al. (2013) to compare various rate constants representing glucose-insulin homeostasis between lean (11% fat)- and high fat diet (HFD; 45% fat)-fed mice. Mice fed HFD (n = 12) for 3 months showed significantly higher body weights (49.97 ± 0.52 g vs. 29.86 ± 0.46 g), fasting blood glucose levels (213.08 ± 10.35 mg/dl vs. 121.91 ± 2.26 mg/dl), and glucose intolerance compared to mice fed lean diet (n = 12). Mice were injected with 1 g/kg glucose intraperitoneally and blood glucose levels were measured at various intervals for 120 min. We performed simulation using Arena™ software based on the mathematical model and estimated the rate constants (9 parameters) for various terms in the differential equations using OptQuest™. The simulated data fit accurately to the observed data for both lean and obese mice, validating the use of the mathematical model in mice at different stages of diabetes progression. Among 9 parameters, 5 parameters including basal insulin, k(2) (rate constant for insulin-dependent glucose uptake to tissues), k(3) (rate constant for insulin-independent glucose uptake to tissues), k(4) (rate constant for liver glucose transfer), and I(pi) (rate constant for insulin concentration where liver switches from glucose release to uptake) were significantly different between lean- and HFD-fed mice. Basal blood insulin levels, k(3), and I(pi) were significantly elevated but k(2) and k(4) were reduced in mice fed a HFD compared to those fed a lean diet. Non-invasive assessment of the key components of glucose-insulin homeostasis including insulin secretion, glucose uptake by tissues, and hepatic handling of glucose may be helpful for individualized drug therapy and designing a customized control algorithm for the artificial pancreas. Elsevier 2017-06-07 /pmc/articles/PMC5463011/ /pubmed/28626803 http://dx.doi.org/10.1016/j.heliyon.2017.e00310 Text en © 2017 Published by Elsevier Ltd. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Brenner, Michael
Abadi, Sakineh Esmaeili Mohsen
Balouchzadeh, Ramin
Lee, H. Felix
Ko, Hoo Sang
Johns, Michael
Malik, Nehal
Lee, Joshua J.
Kwon, Guim
Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title_full Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title_fullStr Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title_full_unstemmed Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title_short Estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
title_sort estimation of insulin secretion, glucose uptake by tissues, and liver handling of glucose using a mathematical model of glucose-insulin homeostasis in lean and obese mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5463011/
https://www.ncbi.nlm.nih.gov/pubmed/28626803
http://dx.doi.org/10.1016/j.heliyon.2017.e00310
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