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Pharmacokinetics of methyldopa in healthy man
Authors:Ø Stenbæk  E Myhre  H Erik Rugstad  Elisabeth Arnold  T Hansen
Institution:(1) Medical Department B and Division of Clinical Pharmacology, Institute of Surgical Research, University Hospital, Rikshospitalet, Oslo, Norway;(2) Department of Biology, Dumex Ltd., Copenhagen, Denmark
Abstract:Summary The pharmacokinetics of 2-14C-L-agr-methyldopa have been investigated in five healthy volunteers following intravenous and oral administration. In the intravenous study a bi-phasic plasma concentration curve was found both for chemically determined agr-methyldopa and for radioactivity. The plasma level of radioactivity differed significantly from chemically determined drug, a pattern which was also found in urine. This suggests the presence of unidentified metabolite(s). The difference between plasma disappearance and urine recovery of agr-methyldopa and radioactivity during the first 4 h after injection suggests distribution to an extravascular compartment. Plasma half-lives of total radioactivity and of unchanged drug were calculated. In three subjects, pharmacokinetic parameters for a two-compartment open body model were calculated from urine and plasma data. Urinary recovery of radioactivity was almost complete within 48 h after intravenous administration. After oral administration, however, only about 40 per cent of the radioactive dose was recovered in the urine, and it contained approximately equal amounts of unconjugated methyldopa, acid-labile conjugated methyldopa and unidentified metabolite(s). The acid-labile conjugate was found only after oral administration, which supports the theory of a mucosal conjugation process. The lack of acid-labile conjugated drug either in the plasma or urine after intravenous injection indicates that there is no enterohepatic circulation of this drug.
Keywords:Methyldopa  radioactive label  pharmacokinetics  metabolism  healthy volunteers  intravenous and oral administration
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