THE PHARMACOKINETICS AND PHARMACODYNAMICS OF THE ANGIOTENSIN-II RECEPTOR ANTAGONIST LOSARTAN POTASSIUM (DUP 753/MK 954) IN THE DOG

被引:0
|
作者
CHRIST, DD
WONG, PC
WONG, YN
HART, SD
QUON, CY
LAM, GN
机构
[1] DUPONT MERCK PHARMACEUT CO,DRUG METAB & PHARMACOKINET SECT,WILMINGTON,DE
[2] DUPONT MERCK PHARMACEUT CO,CARDIOVASC DIS RES GRP,WILMINGTON,DE
来源
JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS | 1994年 / 268卷 / 03期
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中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The pharmacokinetics and plasma concentration-effect relationship for the nonpeptide angiotensin II (Ang II) receptor antagonist losartan potassium (losartan) have been determined with conscious and anesthetized dogs. The p.o. bioavailability of single doses of 5 to 20 mg/kg was low, 23 to 33%, and independent of the dose. Absorption was rapid, with peak plasma levels observed within 1 hr, and the C-max and area under the concentration vs. time curve to infinity were proportional to the dose, P < .05. The elimination half-life, 108 to 153 min, was longer than that observed after a single i.v. dose, 41 min, and may reflect both continuous absorption and enterohepatic recirculation because the major route of excretion was via the bile. Single i.v. doses were eliminated rapidly, with a systemic plasma clearance of 22.2 ml/min/kg. When corrected for the blood:plasma distribution ratio, 0.66 to 0.72, the systemic clearance approximates hepatic blood flow, suggesting that clearance is primarily via hepatic metabolism and biliary excretion. Losartan was not distributed extensively to tissues; apparent volume of distribution at steady-state of 0.30 liters/kg and was highly but not extensively bound to plasma proteins; 2.7 to 2.9% unbound (free). The plasma concentration vs. blockade of exogenous Ang II-induced vasopressor response was also determined after a single 3-mg/kg i.v. dose of losartan with a sigmoidal E(max) model. Blockade of the presser response was rapid, 89% at 5 min, and declined to 11% at 240 min postdose. The relationship between concentration and effect was highly significant (r = 0.922, P < .01), with an IC50 (total) of 96 ng/ml. When corrected for plasma protein binding, the IC50 (free) was approximately 3 ng/ml or 6 nM, a value coincident with the IC50 for the blockade by losartan of Ang II binding in vitro in the absence of albumin, 5 nM. These studies have described the disposition of losartan in the dog, and should allow more rational design and interpretation of studies of this agent in this animal model.
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页码:1199 / 1205
页数:7
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