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地高辛 - 环孢素A相互作用:对肾脏中多药转运蛋白P - 糖蛋白的调节

Digoxin-cyclosporin A interaction: modulation of the multidrug transporter P-glycoprotein in the kidney.

作者信息

Okamura N, Hirai M, Tanigawara Y, Tanaka K, Yasuhara M, Ueda K, Komano T, Hori R

机构信息

Department of Pharmacy, Kyoto University Hospital, Faculty of Medicine, Japan.

出版信息

J Pharmacol Exp Ther. 1993 Sep;266(3):1614-9.

PMID:8103797
Abstract

The mechanism of a renal tubular digoxin-cyclosporin A interaction was elucidated using a kidney epithelial cell line and the isolated perfused rat kidney. The cells expressed an excess amount of human P-glycoprotein on the apical membranes by transfection with MDR1 cDNA. Cyclosporin A inhibited the transepithelial transport of digoxin mediated by human P-glycoprotein; net basal-to-apical transport across the cell monolayer was 22.8, 21.2, 6.61 and 0.91 pmol/mg of protein/3 hr in the presence of 0, 1, 5 and 10 microM cyclosporin A, respectively. Cyclosporin A also reduced the renal tubular secretion of digoxin by the kidney. The ratio of fractional excretion/filtration fraction for digoxin was 2.88 +/- 0.71 (mean +/- S.D.) in the control, and this was decreased to 1.21 +/- 0.09 and 1.05 +/- 0.13 in the presence of 1 and 5 microM cyclosporin A, respectively. Because no signs of acute nephrotoxicity were observed, a direct effect of cyclosporin A accounted for the reduced secretion. On the other hand, digoxin did not affect cyclosporin A transport by P-glycoprotein. These findings indicate that serum concentrations of digoxin in patients should be carefully monitored when administered concurrently with cyclosporin A. The present transepithelial transport system using the transfectant cells is a simple and useful screening system for predicting drug interactions that can occur in a clinical situation.

摘要

利用肾上皮细胞系和分离灌注的大鼠肾脏,阐明了肾小管地高辛 - 环孢素A相互作用的机制。通过用MDR1 cDNA转染,细胞在顶膜上表达过量的人P - 糖蛋白。环孢素A抑制人P - 糖蛋白介导的地高辛跨上皮转运;在存在0、1、5和10 microM环孢素A的情况下,跨细胞单层从基底到顶端的净转运分别为22.8、21.2、6.61和0.91 pmol/mg蛋白质/3小时。环孢素A还减少了肾脏对地高辛的肾小管分泌。地高辛的排泄分数/滤过分数比值在对照组中为2.88±0.71(平均值±标准差),在存在1 microM和5 microM环孢素A时分别降至1.21±0.09和1.05±0.13。由于未观察到急性肾毒性迹象,环孢素A的直接作用导致了分泌减少。另一方面,地高辛不影响P - 糖蛋白对环孢素A的转运。这些发现表明,当与环孢素A同时给药时,应仔细监测患者的地高辛血清浓度。目前使用转染细胞的跨上皮转运系统是一种简单且有用的筛选系统,用于预测临床情况下可能发生的药物相互作用。

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