SENSITIVITY OF PROPRANOLOL ELIMINATION TO HYPOXIA IN THE ISOLATED PERFUSED-RAT-LIVER PREPARATION

被引：9

作者：

ELLIOTT, SL

MORGAN, DJ

ANGUS, PW

GHABRIAL, H

SMALLWOOD, RA

机构：

[1] UNIV MELBOURNE,REPATRIAT HOSP,DEPT MED,HEIDELBERG,VIC 3084,AUSTRALIA

[2] VICTORIAN COLL PHARM,MELBOURNE,VIC,AUSTRALIA

来源：

CLINICAL AND EXPERIMENTAL PHARMACOLOGY AND PHYSIOLOGY | 1993年 / 20卷 / 01期

关键词：

HEPATIC OXYGEN DELIVERY; HYPOXIA; ISOLATED PERFUSED RAT LIVER; PHARMACOKINETICS; PROPRANOLOL;

D O I：

10.1111/j.1440-1681.1993.tb01499.x

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

1. The relationship between the hepatic elimination of propranolol and hepatic oxygen delivery was examined in the single-pass isolated perfused rat liver preparation. Varying rates of oxygen delivery were produced (1.35-8.10 mumol/min per g liver) by equilibrating the perfusate with O2/N2 mixtures. 2. In two experiments, in which the rate of oxygen delivery was increased or decreased within the hypoxic range (<4-5 mumol/min per g liver) every 5 min for 120 min, propranolol clearance responded very rapidly in the same direction as the change in oxygen delivery. 3. In five experiments, propranolol clearance, measured at steady state during an initial 30 min normoxia phase and three subsequent 30 min hypoxia phases (oxygen delivery in the range 1.35-5.89 mumol/min per g liver), was linearly related to hepatic oxygen delivery and consumption (r = 0.92+/-0.07). 4. These data, combined with those from six further experiments that used one normoxia phase followed by one hypoxia phase, showed that there was a threshold for oxygen delivery of about 6 mumol/ min per g liver, below which propranolol clearance decreased with decreasing oxygenation. 5. This study shows that in the intact liver propranolol elimination is very sensitive to hepatic oxygen supply, with impairment in clearance occurring at the lower limit of what is considered normal hepatic oxygenation in the rat.

引用

页码：27 / 33

页数：7

共 50 条

[31] Effects of hypoxia/reperfusion injury on propranolol disposition in the rat isolated perfused liver
Arab, HA
Kadkhodaee, M
Roberts, MS
NAUNYN-SCHMIEDEBERGS ARCHIVES OF PHARMACOLOGY, 1998, 358 (01) : R407 - R407
[32] INFLUENCE OF OXYGEN-SUPPLY ON LIVER CONDITION AND ELIMINATION OF DIMETHYLACETAMIDE IN THE ISOLATED PERFUSED-RAT-LIVER
PALMEN, NGM
EVELO, CTA
BORM, PJA
HENDERSON, PT
TOXICOLOGY IN VITRO, 1992, 6 (04) : 357 - 365
[33] CADMIUM TOXICITY IN THE ISOLATED PERFUSED-RAT-LIVER
LUPO, S
HEWITT, WR
RUSH, GF
TOXICOLOGY LETTERS, 1986, 34 (01) : 5 - 11
[34] SYNTHESIS OF FIBRONECTIN BY THE ISOLATED PERFUSED-RAT-LIVER
OWENS, MR
CIMINO, CD
BLOOD, 1982, 59 (06) : 1305 - 1309
[35] URIDINE CATABOLISM BY THE ISOLATED PERFUSED-RAT-LIVER
HOLSTEGE, A
GENGENBACHER, HM
JEHLE, L
GEROK, W
JOURNAL OF HEPATOLOGY, 1992, 14 (2-3) : 335 - 341
[36] ERYTHROPOIETIN METABOLISM IN THE ISOLATED PERFUSED-RAT-LIVER
NIELSEN, OJ
EGFJORD, M
HIRTH, P
ERYTHROPOIETIN : FROM MOLECULAR STRUCTURE TO CLINICAL APPLICATION, 1989, 76 : 90 - 97
[37] MITOXANTRONE METABOLISM IN THE ISOLATED PERFUSED-RAT-LIVER
EHNINGER, G
PROKSCH, B
HARTMANN, F
GARTNER, HV
WILMS, K
CANCER CHEMOTHERAPY AND PHARMACOLOGY, 1984, 12 (01) : 50 - 52
[38] THE ISOLATED PERFUSED-RAT-LIVER - PERFUSATES REVISITED
GROSS, JB
KOST, LJ
TIETZ, PS
LARUSSO, NF
GASTROENTEROLOGY, 1983, 84 (05) : 1373 - 1373
[39] THE DISPOSITION OF MEFLOQUINE IN THE ISOLATED PERFUSED-RAT-LIVER
COLEMAN, ND
FLECKENSTEIN, EL
SHIPLEY, LA
HEIFFER, MH
FEDERATION PROCEEDINGS, 1987, 46 (03) : 867 - 867
[40] EFFECT OF HYPERTHERMIA ON ISOLATED PERFUSED-RAT-LIVER
ZAVAGNO, G
VESPA, D
MOSCHIN, N
BELLUCO, C
CECCHETTO, A
BERTOCCO, E
RAIMONDO, A
LISE, M
EUROPEAN SURGICAL RESEARCH, 1989, 21 (05) : 243 - 250

← 1 2 3 4 5 →