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Pharmacokinetic study of beta-methyldigoxin by enzyme immunoassay using a novel specific antiserum in rats.

机译:使用新型特异性抗血清通过酶免疫法在大鼠中进行β-甲基地高辛的药代动力学研究。

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摘要

We previously showed that enzyme immunoassay (EIA) of beta-methyldigoxin (MDx3) using anti-MDx3 3'-hemisuccinate-bovine serum albumin antiserum (Antiserum-I) was superior to that using commercial anti-digoxin antiserum (Antiserum-II) in terms of specificity and that pretreatment of human serum with phenyl boric acid (PBA) column was effective. In the present study, we examined the precision of EIA using Antiserum-I and the recovery of MDx3 after PBA column treatment in rat serum, and also investigated pharmacokinetic changes of MDx3 in rats. The intra- and inter-assay variations and recovery tests using Antiserum-I were good. The PBA column was effective in selectively separating MDx3 from rat serum containing MDx3 and its metabolites. The recovery tests using Antiserum-I with PBA column showed about 110% and the interference of metabolites of MDx3 was negligible. Serum concentration-time courses of MDx3 by EIA using Antiserum-I with PBA column and Antiserum-I were lower than that using Antiserum-II. The distribution volume at steady state and total body clearance values of MDx3 in these conditions were significantly higher than those using Antiserum-II. The usefulness of PBA column was ascertained, while effects of PBA column on these parameters were not significant. In addition, rapid absorption of MDx3 was observed by EIA using Antiserum-I with PBA column. These results suggest that EIA using Antiserum-I with PBA column for the pretreatment of serum samples should be a more useful and valuable system in therapeutic drug monitoring and pharmacokinetic studies of the unchanged type of MDx3 than Antiserum-II.
机译:我们先前显示,使用抗MDx3 3'-半琥珀酸-牛血清白蛋白抗血清(Antiserum-I)进行的β-甲基地高辛(MDx3)酶免疫分析(EIA)优于使用商业抗地高辛抗血清(Antiserum-II)在特异性方面以及用苯基硼酸(PBA)柱预处理人血清是有效的。在本研究中,我们检查了使用抗血清I进行EIA的精度以及大鼠血清中PBA柱处理后MDx3的回收率,还研究了MDx3在大鼠中的药代动力学变化。使用Antiserum-I进行的测定内和测定间变异和回收率测试很好。 PBA色谱柱可有效地从含有MDx3及其代谢物的大鼠血清中选择性分离MDx3。使用具有PBA的Antiserum-I进行的回收率测试显示约110%,MDx3代谢物的干扰可忽略不计。 EIA使用PBA色谱柱的Antiserum-I和Antiserum-I进行的MDx3血清浓度-时间进程低于使用Antiserum-II的血清浓度-时间进程。在这些条件下,MDx3在稳态下的分布体积和全身清除率值明显高于使用Antiserum-II的分布量。确定了PBA柱的有用性,而PBA柱对这些参数的影响不显着。此外,使用带有PBA柱的Antiserum-I通过EIA观察到MDx3的快速吸收。这些结果表明,与Antiserum-II相比,使用抗血清-I和PBA柱进行血清样品预处理的EIA在MDx3不变类型的治疗药物监测和药代动力学研究中应该是更有用和有价值的系统。

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