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在母羊和胎羊稳态输注雷尼替丁期间雷尼替丁的胎盘转运。

Placental transfer of ranitidine during steady-state infusions of maternal and fetal sheep.

作者信息

Mihaly G W, Morgan D J, Marshall A W, Smallwood R A, Cockbain S, MacLellan D, Hardy K J

出版信息

J Pharm Sci. 1982 Sep;71(9):1008-10. doi: 10.1002/jps.2600710913.

DOI:10.1002/jps.2600710913
PMID:6127399
Abstract

The placental transfer of ranitidine was studied at pharmacokinetic steady state in anesthetized, full-term, pregnant sheep. Ranitidine was administered to the ewe in three preparations and to the fetus in three other sheep. In all experiments, dose size was based on the combined maternal-fetal weight. Steady-state plasma levels were reached within 4 hr by using an initial intravenous bolus dose followed by continuous infusion. Following maternal dosage, the mean maternal (jugular vein) steady-state concentration (CMss) at 4 hr was 842 +/- 66 ng/ml (SEM), the mean fetal (carotid artery) steady-state concentration (CFss) was 26.5 +/- 4.2 ng/ml, and the mean fetal umbilical venous steady-state concentration was 28.9 +/- 3.5 ng/ml. Both the fetal and umbilical plasma concentrations were significantly less than the maternal plasma concentrations (p less than 0.01). With fetal dosage, mean CMss was 414 +/- 42 ng/ml at 4 hr and was significantly less than the mean CFss value at the same time, which was 6890 +/- 360 ng/ml (p less than 0.005). Ranitidine was not bound extensively to plasma proteins in the ewe or the fetus (range 12-55% bound). The reversal of the CMss/CFss gradient with the change from maternal to fetal administration and the low binding of the drug shows that the gradient following maternal dosage cannot be explained by ion-trapping or differential plasma protein binding. As active placental transport is considered unlikely, the low fetal plasma concentrations are probably due to the presence of significant fetal elimination of ranitidine. Furthermore, the substantial gradient between maternal and umbilical venous plasma concentrations suggests that placental elimination of ranitidine should also be considered.

摘要

在麻醉的足月妊娠绵羊中,于药代动力学稳态时研究了雷尼替丁的胎盘转运情况。对母羊以三种制剂给药,对另外三只羊的胎儿给药。在所有实验中,给药剂量基于母胎体重之和。通过先静脉推注初始剂量然后持续输注,4小时内达到稳态血浆水平。母体给药后,4小时时母体(颈静脉)稳态浓度(CMss)的平均值为842±66纳克/毫升(标准误),胎儿(颈动脉)稳态浓度(CFss)的平均值为26.5±4.2纳克/毫升,胎儿脐静脉稳态浓度的平均值为28.9±3.5纳克/毫升。胎儿和脐血浆浓度均显著低于母体血浆浓度(p<0.01)。胎儿给药时,4小时时CMss的平均值为414±42纳克/毫升,显著低于同时期CFss的平均值,后者为6890±360纳克/毫升(p<0.005)。雷尼替丁在母羊或胎儿体内与血浆蛋白的结合并不广泛(结合率范围为12% - 55%)。从母体给药改为胎儿给药时CMss/CFss梯度的逆转以及药物的低结合率表明,母体给药后的梯度不能用离子捕获或血浆蛋白结合差异来解释。由于不太可能存在活跃的胎盘转运,胎儿血浆浓度低可能是由于雷尼替丁在胎儿体内有显著消除。此外,母体和脐静脉血浆浓度之间的显著梯度表明,也应考虑雷尼替丁的胎盘消除。

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引用本文的文献

1
Human placental transport of cimetidine.西咪替丁的人体胎盘转运
J Clin Invest. 1987 Nov;80(5):1428-34. doi: 10.1172/JCI113222.