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母体向胎儿转移及分布研究。

Transplacental transfer and distribution of pravastatin.

机构信息

Department of Obstetrics and Gynecology, University of Texas Medical Branch, Galveston, TX.

出版信息

Am J Obstet Gynecol. 2013 Oct;209(4):373.e1-5. doi: 10.1016/j.ajog.2013.05.038.

Abstract

OBJECTIVE

The objective of the study was to determine the bidirectional transfer of pravastatin across the dually perfused term human placental lobule and its distribution between the tissue and maternal and fetal circuits.

STUDY DESIGN

The transfer of pravastatin was determined in the maternal-to-fetal (n = 11) and fetal-to-maternal (n = 10) directions. Pravastatin was coperfused with its [(3)H]-isotope and the marker compound antipyrine (20 μg/mL) and its [(14)C]-isotope. The concentration of pravastatin in the perfused tissue and the maternal and fetal circuits was determined using liquid scintillation spectrometry. Inside-out vesicles prepared from placental brush border membranes were utilized to investigate the role of efflux transporters in the transplacental transfer of pravastatin.

RESULTS

Pravastatin was transferred from the maternal to the fetal circuit and vice versa. In the maternal-to-fetal direction, the distribution of pravastatin at the end of experiment was as follows: 14 ± 5% of the drug was retained by the tissue, 68 ± 5% remained in the maternal circuit, and 18 ± 4% was transferred to the fetal circuit. The normalized transfer of pravastatin (clearance index) to antipyrine in the fetal-to-maternal direction (0.48 ± 0.07) was higher than its transfer in the maternal-to-fetal direction (0.36 ± 0.07, P < .01). Furthermore, pravastatin inhibited the adenosine triphosphate (ATP)-dependent uptake of the paclitaxel and estrone sulfate.

CONCLUSION

The transfer of pravastatin across the dually perfused placental lobule suggests that fetal exposure to pravastatin is plausible. The higher transfer of pravastatin in the fetal-to-maternal direction than the reverse as well as its inhibition of the ATP-dependent uptake of [(3)H]-paclitaxel and [(3)H]-estrone sulfate strongly suggest the involvement of efflux transporters in decreasing its transfer across the placenta and support pravastatin's favorable pharmacokinetic profile in pregnancy.

摘要

目的

本研究旨在确定普伐他汀在双灌流人体胎盘小叶中的双向转运及其在组织与母胎循环之间的分布。

研究设计

在母体向胎儿(n=11)和胎儿向母体(n=10)方向测定普伐他汀的转运。普伐他汀与其[3H]-同位素和标记化合物安替比林(20μg/ml)及其[14C]-同位素共灌流。通过液体闪烁谱法测定灌流组织及母胎循环中普伐他汀的浓度。利用胎盘刷状缘膜制备的外翻囊泡,研究外排转运体在普伐他汀跨胎盘转运中的作用。

结果

普伐他汀从母体向胎儿循环转移,反之亦然。在母体向胎儿方向,实验结束时普伐他汀的分布如下:14±5%的药物保留在组织中,68±5%的药物保留在母胎循环中,18±4%的药物转移到胎儿循环中。与普伐他汀在母胎向胎儿方向的转运(0.36±0.07)相比,其在胎儿向母胎方向的转运(0.48±0.07)的标准化转移(清除指数)更高(P<.01)。此外,普伐他汀抑制了三磷酸腺苷(ATP)依赖性紫杉醇和雌酮硫酸的摄取。

结论

普伐他汀在双灌流胎盘小叶中的转运表明胎儿接触普伐他汀是合理的。与反向相比,普伐他汀在胎儿向母胎方向的转运更高,以及其对[3H]-紫杉醇和[3H]-雌酮硫酸的 ATP 依赖性摄取的抑制作用强烈表明外排转运体参与降低其在胎盘内的转运,并支持普伐他汀在妊娠期间良好的药代动力学特征。

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