Lenbury, Ruktamatakul, Amornsamarnkul, 2001
Model Status
Please note that this particular variant of the model is the basic core model which includes three main variables : plasma insulin concentration (x), glucose concentration (y), and the density of the pancreatic beta cells (z).
Model Structure
The secretion of insulin, and its biological effectiveness in reducing blood glucose levels, is mainly dependent on the number and functional efficiency of the pancreatic beta-cells, and also the degree of peripheral insulin resistance. Diabetes can arise from either a deficiency in insulin secretion or from a resistance to insulin. Several mathematical models have been proposed to try and describe the relationships between the plasma concentrations of glucose and insulin. However, these models are often too complex for the available clinical data; which is usually based on glucose alone and is only for a relatively short time period. The current model described here in CellML is based on the published model of Lenbury et al. (2001) and involves just four variables:
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Plasma insulin concentration;
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Plasma glucose concentration;
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Pancreatic beta-cell density; and
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A term to define gastrointestinal glucose absorption.
Schematic diagram of the pancreatic beta-cells. Glucose is taken up and produced in response to insulin secretion and clearance. Beta-cell formation and loss represent the rates at which beta-cells replicate and die. |
The complete original paper reference is cited below:
Modeling insulin kinetics: responses to a single oral glucose administration or ambulatory-fed conditions., Yongwimon Lenbury, Sitipong Ruktamatakul, and Somkid Amornsamarnkul, 2001, Mathematical Biosciences , 59, 15-25. (Full text (HTML) and PDF versions of the article are available on the BioSystems website.) PubMed ID: 11226623