Pharmacokinetics of bambuterol in healthy subjects

Autor:	L, Nyberg, J, Rosenborg, E, Weibull, S, Jönsson, B M, Kennedy, M, Nilsson
Rok vydání:	1998
Předmět:	Adult Male Metabolic Clearance Rate Administration Oral Biological Availability Original Articles Middle Aged Gas Chromatography-Mass Spectrometry Bronchodilator Agents Area Under Curve Injections Intravenous Terbutaline Cholinesterases Humans Female Prodrugs Half-Life
Zdroj:	British journal of clinical pharmacology. 45(5)
ISSN:	0306-5251
Popis:	To study the pharmacokinetics and bioavailability of the prodrug bambuterol and its bronchodilator moiety terbutaline in healthy subjects.Eight healthy subjects (four women) received intravenous doses of bambuterol and terbutaline. On a third occasion, they, plus another four subjects, ingested oral bambuterol as a single dose followed by repeated doses once daily for 7 days. Plasma concentrations and urinary excretion of bambuterol and terbutaline were measured.After intravenous administration, renal clearances of bambuterol and terbutaline were similar (about 140 ml min(-1)), but there was a five-fold difference in total clearance (bambuterol 1.25 l min(-1), terbutaline 0.23 l min(-1)). Volume of distribution (Vss) was 1.6 l kg(-1) b.w. for both substances. A similar renal clearance of bambuterol was found during oral administration but that of terbutaline decreased (to about 120 ml min(-1)). Mean terminal half-life of bambuterol was 2.6 h after intravenous and 12 h after oral administration, implying that uptake was rate-limiting. Mean residence time of terbutaline generated from oral bambuterol was 34 h compared with 8.0 h when terbutaline as such was infused. Generated terbutaline had a bioavailability of 36% (28-46) after intravenous and 10.2% (6.1-13.2) after oral administration of the prodrug. Bambuterol was well tolerated. The mean activity of plasma cholinesterase, an enzyme catalyzing bambuterol metabolism, was inhibited between 30-60% during repeated oral dosing. It virtually regained original activity within 48 h after the last dose.The plasma concentration ofterbutaline fluctuated little during repeated oral administration (mean peak: trough ratio 1.9), as a result of prolonged absorption of bambuterol and slow formation of terbutaline. Thus, the pharmacokinetic properties of bambuterol make it suitable for oral once-daily dosage.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=pmid________::53fef07ef1ac26496da18fce3cfbad02 https://pubmed.ncbi.nlm.nih.gov/9643620 Zobrazit plný text záznamu Plný text