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Bupivacaine transfer across the human term placenta. A study using the dual perfused human placental model.

作者信息

Johnson R F, Herman N, Arney T L, Gonzalez H, Johnson H V, Downing J W

机构信息

Department of Anesthesiology, Vanderbilt University School of Medicine, Nashville, Tennessee 37232.

出版信息

Anesthesiology. 1995 Feb;82(2):459-68. doi: 10.1097/00000542-199502000-00016.

DOI:10.1097/00000542-199502000-00016
PMID:7856904
Abstract

BACKGROUND

Bupivacaine is widely used for obstetric analgesia, yet published information on the mechanism of human placental bupivacaine transfer is sparse. The dual perfused human placental model was used to elucidate the factors governing the placental transfer of bupivacaine.

METHODS

Bupivacaine transfer was studied using the recirculating (closed) model and the single pass (open) model. Single placental cotyledons were perfused with either heparinized Krebs-Ringer's buffer (KRB) supplemented with human albumin (fetal and maternal circuits) or 100% fresh frozen plasma (maternal circuit) to control the bupivacaine protein binding in those circuits. In the open model, bupivacaine clearance was compared before and after being subjected to either increasing concentrations of bupivacaine or its structural analog, mepivacaine.

RESULTS

For those studies in which the maternal and fetal protein binding was equal, the maternal to fetal (M-->F) transfer was significantly greater (P < 0.05) than that in the fetal to maternal (F-->M) direction. When the perfusates were modified to simulate actual in vivo plasma protein concentrations, bupivacaine transfer was shown to be related to the degree of protein binding found in the two circuits. In the open studies, bupivacaine transfer was similar at all concentrations investigated, unaffected by mepivacaine, and related to the pH of the fetal perfusate. A concentration effect was seen within the placental tissue at the end of the experiment.

CONCLUSIONS

Bupivacaine placental transfer characteristics suggest passive diffusion rather than active drug transport and appear to be influenced by the maternal and fetal plasma protein binding, fetal pH, and placental uptake.

摘要

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