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伊拉地平与达罗地平与不同血浆蛋白结合对其透过大鼠血脑屏障的影响。药物与脂蛋白的结合并不限制药物的转运。

Effect of the binding of isradipine and darodipine to different plasma proteins on their transfer through the rat blood-brain barrier. Drug binding to lipoproteins does not limit the transfer of drug.

作者信息

Urien S, Pinquier J L, Paquette B, Chaumet-Riffaud P, Kiechel J R, Tillement J P

出版信息

J Pharmacol Exp Ther. 1987 Jul;242(1):349-53.

PMID:2956411
Abstract

Brain extraction of two calcium channel antagonists, isradipine (PN 200-110) and darodipine (PY 108-068) was investigated using the carotid injection technique in rats. An inhibitor effect of binding to plasma proteins on the brain extraction was also investigated. Equilibrium dialysis at 37 degrees C showed that both drugs were highly bound to human serum proteins, including albumin, alpha-1 acid glycoprotein and lipoproteins. The free dialyzable drug fraction was inversely related to the protein concentration. The brain extraction of the drugs in the presence of either albumin or alpha-1 acid glycoprotein was inversely related to the protein concentrations in the presence of either albumin or alpha-1 acid glycoprotein, but it was higher than expected from the in vitro measurement of the dialyzable fraction. Despite a significant degree of binding to lipoproteins, no significant reduction in the brain extraction of the drugs was observed, regardless of the class or the concentration of lipoproteins. These data indicate that the amount of circulating darodipine or isradipine available for entry in a peripheral tissue such as brain exceeds the dialyzable fraction of drug. However, the in vivo exchangeable drug fraction still parallels the dialyzable fraction, except if the drug is lipoprotein bound.

摘要

采用颈动脉注射技术在大鼠中研究了两种钙通道拮抗剂伊拉地平(PN 200 - 110)和达罗地平(PY 108 - 068)的脑摄取情况。还研究了与血浆蛋白结合对脑摄取的抑制作用。37℃下的平衡透析表明,两种药物都与包括白蛋白、α-1酸性糖蛋白和脂蛋白在内的人血清蛋白高度结合。可透析的游离药物分数与蛋白质浓度呈负相关。在白蛋白或α-1酸性糖蛋白存在下,药物的脑摄取与白蛋白或α-1酸性糖蛋白存在时的蛋白质浓度呈负相关,但高于体外可透析分数测量的预期值。尽管与脂蛋白有显著程度的结合,但无论脂蛋白的类别或浓度如何,均未观察到药物脑摄取的显著降低。这些数据表明,可进入外周组织如脑的循环中的达罗地平或伊拉地平的量超过了药物的可透析分数。然而,体内可交换的药物分数仍与可透析分数平行,除非药物与脂蛋白结合。

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