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苯妥英在原位灌注的大鼠足月胎盘的转运。

Phenytoin transfer across the in situ perfused rat term placenta.

作者信息

Staud F, Fendrich Z, Jindrová O, Láznícek M

机构信息

Department of Pharmacology and Toxicology, Faculty of Pharmacy, Charles University, Hradec Králové, Czech Republic.

出版信息

Pharmazie. 1997 Nov;52(11):871-4.

PMID:9399343
Abstract

Transfer of phenytoin (PHT) across the rat term placenta perfused in situ was investigated and compared with that of antipyrine (AP) as a marker of passive diffusion. PHT was shown to cross the placenta with similar kinetics as AP did. Both the first order transfer constant (ktr = 0.070 min-1) and the first order equilibration constant (keq = 0.027 min-1) of PHT were comparable to those of AP (ktr = 0.046 min-1, keq = 0.022 min-1). Similarly, there were significant differences between PHT and AP in the foeto-maternal concentration ratio at equilibrium (FMCReq = 1.01 and 1.09, respectively). The present data indicate that the transfer of PHT through the rat placenta is governed by the same principles as that of AP, i.e. by the mechanism of passive diffusion. Surprisingly, maternal plasma protein binding of PHT (60.5%) did not seem to influence either its rate of transfer or its eventual foeto-maternal concentration ratio.

摘要

研究了苯妥英(PHT)在原位灌注的大鼠足月胎盘的转运情况,并与作为被动扩散标志物的安替比林(AP)进行了比较。结果表明,PHT穿过胎盘的动力学与AP相似。PHT的一级转运常数(ktr = 0.070 min-1)和一级平衡常数(keq = 0.027 min-1)与AP的相当(ktr = 0.046 min-1,keq = 0.022 min-1)。同样,平衡时PHT和AP的胎儿-母体浓度比也存在显著差异(分别为FMCReq = 1.01和1.09)。目前的数据表明,PHT通过大鼠胎盘的转运遵循与AP相同的原则,即通过被动扩散机制。令人惊讶的是,PHT的母体血浆蛋白结合率(60.5%)似乎既不影响其转运速率,也不影响其最终的胎儿-母体浓度比。

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