Abstract
Liver disease changes the disposition properties of drugs, complicating drug therapy management. We present normal and “diseased” versions of an abstract, agent-oriented In Silico Livers (ISLs), and validate their mechanisms against disposition data from perfused normal and diseased rat livers. Dynamic tracing features enabled spatiotemporal tracing of differences in dispositional events for diltiazem and sucrose across five levels, including interactions with representations of lobular microarchitectural features, cells, and intracellular factors that sequester and metabolize. Differences in attributes map to measures of histopathology. We measured disease-causing differences in local, intralobular ISL effects, obtaining until now unavailable views of how and where hepatic drug disposition may differ in normal and diseased rat livers from diltiazem's perspective. Exploration of disposition in less and more advanced stages of disease is feasible. The approach and technology represent an important step toward unraveling the complex changes from normal to disease states and their influences on drug disposition.
Footnotes
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This work was supported by CDH Research Foundation [Grants CDHRP-06/07, -0014, -0023]; and by Australian National Health and Medical Research Council [Grant 252871/9937600].
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C.A.H. is a trustee of CDH Research Foundation
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Article, publication date, and citation information can be found at http://jpet.aspetjournals.org.
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doi:10.1124/jpet.108.142497.
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ABBREVIATIONS: ISL, In Silico Liver; CCl4, carbon tetrachloride; PK, pharmacokinetic; PV, terminal portal vein tract; CV, central hepatic vein; SS, sinusoidal segment; SM, similarity measure; PCP, physicochemical property; CA, cellular automaton; OOP, object-oriented program(ming); ABS, agent-based system.
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↵ The online version of this article (available at http://jpet.aspetjournals.org) contains supplemental material.
- Received June 17, 2008.
- Accepted October 14, 2008.
- The American Society for Pharmacology and Experimental Therapeutics
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