通过特定的高效液相色谱法测定的三种口服制剂中地高辛的生物利用度。
The bioavailability of digoxin from three oral formulations measured by a specific h.p.l.c. assay.
作者信息
Cohen A F, Kroon R, Schoemaker H C, Breimer D D, Van Vliet-Verbeek A, Brandenburg H C
机构信息
Centre for Human Drug Research, Leiden University Hospital, The Netherlands.
出版信息
Br J Clin Pharmacol. 1993 Feb;35(2):136-42. doi: 10.1111/j.1365-2125.1993.tb05679.x.
Abstract
- We have studied the absolute bioavailability of three oral formulations of digoxin, 1.0 mg, in 12 young healthy volunteers in a four way randomised cross-over study using an intravenous control. 2. Digoxin tablets (250 micrograms), liquid filled digoxin capsules (100 micrograms) and an experimental enteric-coated capsule (100 micrograms) were evaluated. In vitro dissolution at pH 1 demonstrated extensive hydrolytic breakdown of digoxin from the tablets and capsules but not from the enteric-coated capsules. 3. Serum 'digoxin' concentrations were measured by fluorescence polarization immunoassay (FPI). The systemic availability (+/- s.d.) of the capsules was 70.5 +/- 11.3%, and that of the tablets 71.5 +/- 8.6%. Drug was less available from the enteric-coated capsules (62.1 +/- 10.3%) measured with FPI. These results were reflected in the urinary drug recoveries measured by FPI. 4. By contrast, there were no differences in urinary recovery of unchanged digoxin between any of the oral treatments, when this was measured by h.p.l.c. The cross-reactivity of immunoassays for metabolites of digoxin may produce artefactual results and the optimal pharmaceutical formulation for digoxin remains to be determined.
摘要
- 我们在一项使用静脉注射对照的四路随机交叉研究中,对12名年轻健康志愿者进行了1.0毫克地高辛三种口服制剂的绝对生物利用度研究。2. 对250微克地高辛片剂、100微克液填地高辛胶囊和一种实验性肠溶胶囊(100微克)进行了评估。在pH值为1时的体外溶出度显示,地高辛从片剂和胶囊中发生了广泛的水解分解,但肠溶胶囊未出现这种情况。3. 通过荧光偏振免疫测定法(FPI)测量血清“地高辛”浓度。胶囊的全身利用率(±标准差)为70.5±11.3%,片剂为71.5±8.6%。用FPI测量时,肠溶胶囊的药物利用率较低(62.1±10.3%)。这些结果反映在用FPI测量的尿药回收率中。4. 相比之下,当通过高效液相色谱法测量时,任何口服治疗之间未改变的地高辛尿回收率没有差异。地高辛代谢物免疫测定的交叉反应性可能会产生人为结果,地高辛的最佳药物制剂仍有待确定。
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