Resources
Pharmacokinetics
Author(s): Gretchen A. Koch
Goucher College
89 total view(s), 55 download(s)
- Pharmacokinetics_One_Compartment_Model_Longer_Time_Version_1_0.xls(XLS | 313 KB)
- Pharmacokinetics_One_Compartment_Model_Shorter_Time_Version_1_0.xls(XLS | 660 KB)
- Pharmacokinetics_Two_Compartment_Model_Longer_Time_Version_1_0.xls(XLS | 358 KB)
- Pharmacokinetics_Two_Compartment_Model_Shorter_Time_Version_1_0.xls(XLS | 1 MB)
- License terms
Overview
This Excel module explores how drugs are processed and absorbed in the human body. By entering the half-lives of any drug, selecting the dosage amount, choosing the frequency of the dose, and choosing whether doses are missed, the user can visually interpret whether or not the drug remains in a therapeutic range, or steady state.
This module consists of four files; there are two files for each type of model. For each model, there is a short time module that simulated the process for less than a month, and there is a longer time module, where several months are simulated. The differences in the file types are noted in the titles of the files.
The first model is a one-compartment pharmacokinetics model. This model can be used to explore injected drugs, or drugs that are administered directly into the action site, such as eye drops. The second model is a two-compartment pharmacokinetics model. This type of model would be used to explore drugs that are taken orally, and must go through the gut before being distributed through the body by the blood. This model could be used to explore any drug that must go through one organ before entering the blood.
Popular Text Citations
Begg, E. J. Instant Clinical Pharmacology. Blackwell Publishing Ltd.: Oxford. 2003.
Gibaldi, M. and D. Perrier. Pharmacokinetics. 2nd ed. Marcel Dekker: New York. 1982.
Gabrielsson, J. and D. Weiner. Pharmacokinetic and Pharmacodynamic Data Analysis: Concepts and Applications. Swedish Pharmaceutical Society: Stockholm. 2007.
Washington, N., Washington, C., and C. Wilson. Physiological Pharmaceutics: Barriers to Drug Absorption. 2nd ed. Taylor and Francis (CRC Press): London. 2001.
Research Articles
Austen, D. J., White, N. J., and R. M. Anderson. ''The dynamics of drug actions on the within-host population growth of infectious agents.'' J. Theor. Biol. 7 Oct 1998. 194(3): 313-39.
Paixão, P., Gouveia L. F., and J. A. G. Morais. ''Prediction of drug distribution within blood.'' Eur. J. Pharm. Sci. 2 March 2009. 36(4-5): 544-54.
Sheiner, L. B. and S. L. Beal. ''Bayesian individualization of pharmacokinetics: simple implementation and comparison with non-Bayesian methods.'' J. Pharm. Sci. Dec 1982. 71(12): 1344-48.
Funatogawa, T. and I. Funatogawa. ''The Bayesian bias correction method of first-order approximation of nonlinear mixed-effects models for population pharmacokinetics.'' J. Biopharm. Stat. 2007. 17(3): 381-92.
Data Sources
2022 Phish-Pharm Database of Pharmacokinetics Data in Fish
The Complete Pharmacokinetic Database [Broken link: http://pbpk.org//component/option,com%20weblinks/Itemid,23/]
U. S. Food and Drug Administration - Drugs@FDA
Education Research & Pedagogical Materials
Koch, G. A. ''Drugs in the Classroom: Using Pharmacokinetics to Introduce Biomathematical Modeling.'' Math. Model. Nat. Phen. Accepted January 2011. In-press.
Cornell College of Veterinary Medicine: Department of Pharmacology
PPlane Java Applet (Phase Plane Analysis Software) [In-browser version]
Tutorial & Background Materials
Thomson, A. ''Back to basics: pharmacokinetics.'' Society. June 2004. 272: 769-71.
Pub: Springer Netherlands. ''Pharmacokinetics and biopharmaceutics: a definition of terms.'' J. Pharmacokinet. Phar. 21 Feb 1973. 1(1): 3-4.
Citation
Researchers should cite this work as follows:
- Koch, G. A. (2024). Pharmacokinetics. ESTEEM, QUBES Educational Resources. doi:10.25334/94VG-8R46
Fundamental Mathematical Concepts
Developed By
Primary Reference
Spitznagel, E. ''Two-Compartment Pharmacokinetics Models.'' C-ODE-E. Harvey Mudd College, Fall 1992.