2007
DOI: 10.1248/bpb.30.552
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Pharmacokinetics and Hepatic Extraction of Metoprolol in Rats with Glycerol-Induced Acute Renal Failure

Abstract: The intestinal absorption of orally administered propranolol is essentially complete, with no metabolism of this drug occurring in the gut.1,2) After the oral administration of propranolol, the liver is the principal site of extensive presystemic and systemic metabolism, and less than 1% of the intact drug is found in urine.1,3) However, Bianchetti et al. 4) showed that the area under the concentration-time curve for orally administered propranolol in renal failure patients not on hemodialysis is 7-to 8-fold h… Show more

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Cited by 18 publications
(12 citation statements)
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“…In fact, it was demonstrated that the hepatic function of metabolizing therapeutic compounds is changed in rats with experimental renal failure, markedly altering their pharmacokinetics (5,6). In the intestine, the barrier function preventing xenobiotic absorption is decreased in renal failure, resulting in an increase in their intestinal absorption (7,8). These functional changes of the liver and intestine seem to be related to the fact that the expressions of drug-metabolizing enzymes and drug-transporting proteins are significantly altered in renal failure (9)(10)(11)(12).…”
Section: Introductionmentioning
confidence: 99%
“…In fact, it was demonstrated that the hepatic function of metabolizing therapeutic compounds is changed in rats with experimental renal failure, markedly altering their pharmacokinetics (5,6). In the intestine, the barrier function preventing xenobiotic absorption is decreased in renal failure, resulting in an increase in their intestinal absorption (7,8). These functional changes of the liver and intestine seem to be related to the fact that the expressions of drug-metabolizing enzymes and drug-transporting proteins are significantly altered in renal failure (9)(10)(11)(12).…”
Section: Introductionmentioning
confidence: 99%
“…was increased more than 10-fold in rats with pretreatment of cyclosporine (50 mg/kg, i.p.) [17]. The effect of 7-day BDL on BBC was also very significant; that is, the mean BBC values in BDL rats were 8.0-and 6.1-fold higher than those in normal rats at infusion rates of 24 and 60 mg/min/ kg, respectively (Figure 1).…”
Section: Effect Of Cyclosporine and Bdl On The Pharmacokinetics Of Bomentioning
confidence: 89%
“…Briefly, whole blood samples (0.1 ml) were mixed with 0.4 ml of distilled water to hemolyse blood cells [16,17]. After acidification with 1.2 ml of 1 M citrate buffer (pH 4.0), the samples were extracted with 5 ml of a mixture of n-butyl chloride and dichloromethane (4: 1, v/v).…”
Section: Assay Of Bosentanmentioning
confidence: 99%
“…Although reports relating toaltered absorption haven ot been extensivelydocumented in ARF ratmodels,there areafewinstancest od atethats uggest altered absorption:c yclosporine,Y JA-20379-8,diltiazem (CAS 42399-41-7),propranolol,metoprolol (CAS 83-43-2),oltipraz (CAS 64224-21-1),DA-7867,azosemide (CAS 27589-33-9) etc [ 21,25,30,40,41,46,53,55,56].Inthe caseo fcyclosporine in cisplatin,gentamicin,a nd glycerol induced ARF models (Table 2),therewasasignificantr eduction in the rateo fo ralabsorption and itw asalso attributed tothe diminished bile secretion whicho therwisem ayhavecontributed toani mproved solubility of cyclosporine in the intestinalfluids.Thisphenonmenon Glycerol (56-81-5) induced ARF The AUC values of tolbutamide were nearly 40 % lower in ARF rats relative to control rats. This was accompanied by moderate increase in the body clearance of tolbutamide in ARF rats.…”
Section: Absorption Related Changesmentioning
confidence: 99%
“…Interestingly,in the uranyln itratem odel,the extentof absorption of cyclosporine afterorald osing was comparable between ARF rats and control rats suggesting thatt hismodel behaved differentlyt hanthe other three ARF models.Anothercompound,Y JA-20379-8,a proton pump inhibitor,wass howntoh aveadecreased absorption ratei nauranyln itratei nduced ARF model [41].Inthe caseo fd iltiazem,itw ass uggested thatan improperoralabsorption mayhaveadditionallycontributed in the uranyln itratei nduced ARF model. In caseo fp ropranol,thereappeared tobetwocontrasting reports toaccountforits enhanced bioavailability in ARF rats.However,the twostudiesu sed differentARF models; the earliers tudyt hatu sed auranyln itrateARF suggested apossible reduction in presystemichepatic elimination [58]and the laterstudythatused acisplatin ARF model indicated ane nhanced intestinalabsorption rateofpropranolol from the gastrointestinaltractof ARF rats [56].Inthe caseo fanotherbeta-blocker,metoprolol,therewasasuggestion thatt he absorption ratewas initiallyincreased followed bys aturation of first-pass elimination [21].Inthe caseo fo ltipraz,therewasadecreased oralabsorption of the compound in ARF rats [30].Inthe caseo fDA-7867,aminordecreased absorption mayhavecontributed tothe reduced exposure [25]. Inthe caseo fazosemide,therewaspronounced intestinalabsorption of the drugi nARF rats [40], contrary to the reduced gastricemptying time reported forcyclosporine in ARF rats [55,56].…”
Section: Referencementioning
confidence: 99%