A Computational Model of Liver Iron Metabolism
Simon Mitchell, Pedro Mendes

TL;DR
This paper presents a detailed computational model of human liver iron metabolism that accurately reproduces physiological responses and disease states, aiding understanding and potential treatment of iron-related disorders.
Contribution
A new mechanistic computational model of liver iron metabolism was developed and validated against experimental data, including disease simulation of haemochromatosis.
Findings
Model reproduces physiological iron regulation dynamics.
Simulation of haemochromatosis shows liver iron overload.
Model serves as a framework for drug target identification.
Abstract
Iron is essential for all known life due to its redox properties, however these same properties can also lead to its toxicity in overload through the production of reactive oxygen species. Robust systemic and cellular control are required to maintain safe levels of iron and the liver seems to be where this regulation is mainly located. Iron misregulation is implicated in many diseases and as our understanding of iron metabolism improves the list of iron-related disorders grows. Recent developments have resulted in greater knowledge of the fate of iron in the body and have led to a detailed map of its metabolism, however a quantitative understanding at the systems level of how its components interact to produce tight regulation remains elusive. A mechanistic computational model of human liver iron metabolism, which includes the core regulatory components, was constructed based on known…
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