ABSORPTION OF QUINIDINE FROM AN ENTERIC-COATED PREPARATION

被引:7
作者
FREMSTAD, D
NILSEN, OG
AMLIE, J
STORSTEIN, L
OLSSON, B
JACOBSEN, S
机构
[1] RIKSHOSP,MED DEPT B,OSLO,NORWAY
[2] UNIV OSLO,INST PHARMACOL,OSLO,NORWAY
[3] AS FARMACEUT IND,OSLO,NORWAY
关键词
bioavailability; enteric-coated tablets; gastric emptying; pH; quinidine;
D O I
10.1007/BF00563116
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The absorption of quinidine from single and multiple doses of an enteric-coated preparation (Systodin®) was studied in seven healthy subjects, and was compared with the pharmacokinetics of intravenously administered quinidine and the results of in vitro dissolution tests of the tablets. Absorption of quinidine began after a variable delay, 2-8 h (mean 4.8) after fasting and 3-10 h (mean 6.1) after food. The rate of absorption varied both in and between individuals. It appeared to be lower when the drug was administered after food. Multiple doses after food gave a pattern of plasma concentration-time curves similar to that found on administration of single doses after food. The delay prior to absorption was prolonged at night. The ratio between the maximum and minimum concentration of quinidine during a dose interval varied from 1.3 to 3.2 (mean 2.0). Bioavailability of quinidine in fasting subjects ranged from 69 to 95% (mean 83); variation was greater when doses were administered after food. The release of quinidine from the enteric-coated preparation was pH dependent and was sustained at low pHs as may be found in the intestines. The results indicate that the absorption of quinidine from the enteric-coated formulation was dependent on the highly variable rate of gastric emptying and the pH of intestinal fluid, and it varied greatly both within and between individuals. © 1979 Springer-Verlag.
引用
收藏
页码:107 / 112
页数:6
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