Abstract

The long-term goal of the research proposal is to provide a thorough understanding of the space- and time-related changes associated with drug disappearance and metabolite formation in the liver, the major drug metabolizing organ. Methods for probing zonal metabolic heterogeneities: single pass prograde [P, inflow into portal vein (PV)] and retrograde [R, inflow into hepatic vein (HV)] and hepatic artery-portal vein, hepatic artery-hepatic vein [HAPV-HAHV, dual inflow system with substrates given to HA] perfusion and the multiple indicator dilution (MID) technique will be used to examine mechanisms of elimination and transport across hepatocyte membranes for several precursor-metabolite pairs. An injection of a mixture of vascular [51Cr-labeled red blood cells, 125I-labeled albumin, 58CoEDTA (similar to [14C]sucrose)] and cellular (D2O) reference noneliminated indicators and 14C- and 3H-labeled precursor and product will be given, during steady-state bulk perfusion by PR or HAPV-HAHV. The outflow profiles thus obtained will be appropriately analyzed and referenced with respect to the noneliminated reference indicators. Modeling is able to account for the binding effects due to red cells, plasma, or tissue proteins, provide the physiological volumes and the influx, efflux, and sequestration coefficients for both precursor and metabolite, and identify the rate-controlling step.
For Aim 1, the hepatic processing of benzoic acid, hippuric acid, taurolithocholic acid 3- sulfate, tracer salicylamide and phenacetin, morphine, morphine-3beta- and 6beta- glucuronides, 4-methyl-umbelliferone (4MU), 4MU glucuronide, harmol, harmol sulfate and glucuronide conjugates, estrone sulfate, estrone, and estradiol (with and without inhibitors of sulfation/desulfation) will be examined. The sulfate conjugate of the bile acid, and of estrone, 4-MU or harmol will be given simultaneously to test for interactions in transport and removal.
For Aim 2, the micro-mixing of the hepatic artery and portal vein will be investigated with a full set of noneliminated references with HA or PV injections, then with HA or PV infusion of carrier-mediated [bromosulfophthalein (BSP) and its glutathione conjugate (BSP-GSH)] and flow-limited (salicylamide) substrates at varying HA:PV flow ratios. Events underlying single, parallel, and sequential pathways, futile cycling, enzyme zonation, and competition in uptake will be provided in the above studies. The permeability of the peribiliary capillary plexus to solutes and the potential reduction in liver mass with the probes infused into the HA will be delineated. These studies should lend important insight into mechanisms of drug-metabolite processing of pharmacologically important sulfate and glucuronide conjugates, and differences in preformed vs. generated metabolite removal due to the differing origins.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM038250-07A1
Application #
2179234
Study Section
Pharmacology A Study Section (PHRA)
Project Start
1991-02-01
Project End
1998-01-31
Budget Start
1995-02-06
Budget End
1996-01-31
Support Year
7
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Toronto
Department
Type
DUNS #
259999779
City
Toronto
State
ON
Country
Canada
Zip Code
M5 1-S8

  Publications

Pang, K S; Schwab, A J; Goresky, C A et al. (1994) Transport, binding, and metabolism of sulfate conjugates in the liver. Chem Biol Interact 92:179-207
Xu, X; Schwab, A J; Barker 3rd, F et al. (1994) Salicylamide sulfate cell entry in perfused rat liver: a multiple-indicator dilution study. Hepatology 19:229-44
Pang, K S; Sherman, I A; Schwab, A J et al. (1994) Role of the hepatic artery in the metabolism of phenacetin and acetaminophen: intravital microscopic and multiple-indicator dilution study in perfused rat liver. Hepatology 20:672-83
Chiba, M; Poon, K; Hollands, J et al. (1994) Glycine conjugation activity of benzoic acid and its acinar localization in the perfused rat liver. J Pharmacol Exp Ther 268:409-16
Pang, K S; Barker 3rd, F; Schwab, A J et al. (1994) Demonstration of rapid entry and a cellular binding space for salicylamide in perfused rat liver: a multiple indicator dilution study. J Pharmacol Exp Ther 270:285-95
Ratna, S; Chiba, M; Bandyopadhyay, L et al. (1993) Futile cycling between 4-methylumbelliferone and its conjugates in perfused rat liver. Hepatology 17:838-53
Chiba, M; Pang, K S (1993) Effect of protein binding on 4-methylumbelliferyl sulfate desulfation kinetics in perfused rat liver. J Pharmacol Exp Ther 266:492-9
Pang, K S; Xu, X; St-Pierre, M V (1992) Determinants of metabolite disposition. Annu Rev Pharmacol Toxicol 32:623-69
Goresky, C A; Pang, K S; Schwab, A J et al. (1992) Uptake of a protein-bound polar compound, acetaminophen sulfate, by perfused rat liver. Hepatology 16:173-90
St-Pierre, M V; Lee, P I; Pang, K S (1992) A comparative investigation of hepatic clearance models: predictions of metabolite formation and elimination. J Pharmacokinet Biopharm 20:105-45

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