PHARMACOKINETICS OF NIPRADILOL (K-351), A NEW ANTIHYPERTENSIVE AGENT. II. INFLUENCE OF THE ROUTE OF ADMINISTRATION ON BIOAVAILABILITY IN DOGS
スポンサーリンク
概要
- 論文の詳細を見る
The pharmacokinetic parameters of nipradilol (NIP), a new potent antihypertensive and antianginal agent, and propranolol were determined after oral, intravenous and intraportal administration to the beagle dog implanted with cannula in portal vein at a dose of 1 mg/kg. Orally administered NIP underwent extensive first-pass metabolism leading to low bioavailability (11%), despite of complete gastrointestinal absorption. On the constant infusion for 30 min into the portal vein, hepatic extraction ratio was 0.71. The reduction in the systemic availability of orally administered NIP could partly be attributed to the fact that denitration and glucuronidation of NIP occur primarily in the intestinal tract and liver, respectively. Following oral administration of NIP, smaller amount of unchanged drug (1.9%) was excreted into the urine than that of intravenous administration (5.8%). However, in the qualitative and the quantitative aspects on urinary metabolic patterns, there was no appreciable influence of the route of administration. On the other hand, the systemic availability and the hepatic extraction ratio of propranolol were 11% and 0.86,respectively, suggesting that the first-pass metabolism through the liver actually contributes to the reduced availability.
- 公益社団法人日本薬学会の論文
著者
-
FUJII Mikio
Tokyo Research Laboratories, Pharmaceutical Division, Kowa Company Ltd
-
Fujii M
Tokyo Research Laboratories Kowa Co. Ltd.
-
Yoshimura Mitsuo
Tokyo Research Laboratories Kowa Co. Ltd.
-
Fujii Mikio
Tokyo Research Laboratories Kowa Co. Ltd.
-
Kojima Junji
Tokyo New Drug Research Laboratories Kowa Company Ltd.
-
Kojima Junji
Tokyo Research Laboratories Kowa Co. Ltd.
-
ITO TERUFUMI
Tokyo Research Laboratories, Kowa Co., Ltd.
-
SUZUKI JUNNOSUKE
Tokyo Research Laboratories, Kowa Co., Ltd.
-
Ito Terufumi
Tokyo Research Laboratories Kowa Co. Ltd.
-
Suzuki J
Department Of Chemical Pharmacology Faculty Of Pharmaceutical Sciences Toyama Medical And Pharmaceut
関連論文
- Effect of Protease-Activated Receptor-2 Deficiency on Allergic Dermatitis in the Mouse Ear
- INVOLVEMENT OF GLUCOCORTICOID IN INSULIN-INDUCED ANGIOGENESIS OF ADJUVANT POUCH GRANULOMA IN DIABETIC MICE
- QUANTITATIVE METHOD FOR MEASURING ADJUVANT-INDUCED GRANULOMA ANGIOGENESIS IN INSULIN-TREATED DIABETIC MICE
- MOUSE GRANULOMA POUCH INDUCED BY FREUND'S COMPLETE ADJUVANT WITH CROTON OIL
- Effect of Biliary Excretion on the Pharmacokinetics of Pitavastatin (NK-104) in Dogs
- Uptake Mechanism of Pitavastatin, a New Inhibitor of HMG-CoA Reductase, in Rat Hepatocytes
- Metabolic Fate of Pitavastatin, a New Inhibitor of HMG-CoA Reductase : Effect of cMOAT Deficiency on Hepatobiliary Excretion in Rats and of mdr1a/b Gene Disruption on Tissue Distribution in Mice
- Simultaneous determination of NK-104 and its lactone in biological samples by column-switching high-performance liquid chromatography with ultraviolet detection
- Identification of Metabolites of NK-104,an HMG-CoA Reductase Inhibitor, in Rat, Rabbit and Dog Bile
- PHARMACOKINETICS OF NIPRADILOL (K-351), A NEW ANTIHYPERTENSIVE AGENT. I. STUDIES ON INTERSPECIES VARIATION IN LABORATORY ANIMALS
- PHARMACOKINETICS OF NIPRADILOL (K-351), A NEW ANTIHYPERTENSIVE AGENT. II. INFLUENCE OF THE ROUTE OF ADMINISTRATION ON BIOAVAILABILITY IN DOGS
- A Genetically Diabetic Model “KK-CAy Mice” for a Pharmacological Assay
- PLACENTAL PASSAGE AND DUCTUS-CONSTRICTING EFFECT OF ACEMETACIN IN RATS
- Venodilating action of nipradilol (K-351) in the pithed rat pretreated with dihydroergotamine.
- Pharmacokinetics of nipradilol (K-351), a new antihypertensive agent, in human.
- Venous Distensibility in Stroke-Prone SHR at 6 and 15 Weeks of Age---Comparison with Age-Matched WKY---