DocumentCode :
2487529
Title :
Mechanistic modeling of drug elimination by the liver using local volume averaging method
Author :
Izadifar, M. ; Baik, O.D. ; Alcorn, J.
Author_Institution :
Div. of Biomed. Eng., Univ. of Saskatchewan, Saskatoon, SK, Canada
fYear :
2011
fDate :
Aug. 30 2011-Sept. 3 2011
Firstpage :
4314
Lastpage :
4317
Abstract :
Local volume averaging method and local mass (drug) equilibrium were used for developing a mathematical model for transient drug transport and elimination in the liver. Taking into account the liver porosity and tortuosity, physio-chemical properties of the drug, the drug effective diffusivity, dispersion, convection, local plasma-hepatocyte equilibrium and hepatocellular drug metabolism, the governing partial differential equation was developed and numerically solved to describe a transient drug transfer and elimination across the liver following intravenous (IV) administration. The predicted values of hepatic clearance and bioavailability had very good agreement with the reported observations for different drugs. Unlike the well-stirred, parallel tube and dispersion models of hepatic clearance, the proposed mechanistic model is able to predict the drug concentration gradient across the liver with time and position in very dynamic conditions associated with drug absorption process in the intestine.
Keywords :
biochemistry; biodiffusion; drugs; liver; partial differential equations; physiological models; bioavailability; drug convection; drug dispersion; drug effective diffusivity; drug physiochemical properties; hepatic clearance; hepatocellular drug metabolism; intravenous drug administration; liver drug elimination mechanistic modeling; liver porosity; liver tortuosity; liver transient drug transport; local drug equilibrium; local mass equilibrium; local plasma-hepatocyte equilibrium; local volume averaging method; mathematical model; partial differential equation; Biological system modeling; Blood; Dispersion; Drugs; Liver; Mathematical model; Predictive models; Humans; Liver; Models, Theoretical; Pharmacokinetics;
fLanguage :
English
Publisher :
ieee
Conference_Titel :
Engineering in Medicine and Biology Society, EMBC, 2011 Annual International Conference of the IEEE
Conference_Location :
Boston, MA
ISSN :
1557-170X
Print_ISBN :
978-1-4244-4121-1
Electronic_ISBN :
1557-170X
Type :
conf
DOI :
10.1109/IEMBS.2011.6091071
Filename :
6091071
Link To Document :
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