Assessment of biotransformation during transfer of propoxyphene and acetaminophen across the isolated perfused human placenta.

U W Weigand, R C Chou, D Maulik, G Levy
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Abstract

The purpose of this investigation was to assess the extent of biotransformation of drugs by the human placenta during their transfer from the maternal to the fetal circulation. Propoxyphene was used to determine N-demethylation, and acetaminophen served as a substrate for glucuronide and sulfate conjugation. Human full-term placentae were dually perfused in vitro, with one or the other drug being added to the maternal circulation. Propoxyphene and acetaminophen concentrations reached an essentially constant fetal/maternal ratio within 1 hour, with a half-time of about 20 minutes. The concentrations of both drugs in the placental tissues were higher than in the perfusion fluids; this accumulation was particularly pronounced in the case of propoxyphene. No metabolites of either drug were found in the maternal or fetal circulations, but norporpoxyphene, the N-demethylated metabolite of propoxyphene, was detected in placental tissue.

丙氧苯和对乙酰氨基酚通过离体灌注人胎盘转移过程中生物转化的评估。
本研究的目的是评估药物从母体到胎儿循环转移过程中,人胎盘对药物的生物转化程度。用丙氧基苯测定n -去甲基化,对乙酰氨基酚作为葡萄糖醛酸和硫酸盐偶联的底物。人类足月胎盘在体外双灌注,其中一种或另一种药物被添加到母体循环。丙氧苯和对乙酰氨基酚浓度在1小时内达到基本恒定的胎母比,中间时间约为20分钟。两种药物在胎盘组织中的浓度均高于灌注液;这种积累在丙氧苯的情况下尤其明显。在母体和胎儿循环中均未发现这两种药物的代谢物,但在胎盘组织中检测到丙氧芬的n -去甲基化代谢物去甲氧芬。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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