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毛细管电泳法研究药物对映体与血清白蛋白的相互作用

Study of interaction between drug enantiomers and serum albumin by capillary electrophoresis.

作者信息

Ding Y, Zhu X, Lin B

机构信息

Dalian Institute of Chemical Physics, Chinese Academy of Sciences, PR China.

出版信息

Electrophoresis. 1999 Jul;20(9):1890-4. doi: 10.1002/(SICI)1522-2683(19990701)20:9<1890::AID-ELPS1890>3.0.CO;2-E.

Abstract

The interaction between drugs and human serum albumin (HSA) was investigated by capillary electrophoresis (CE). It involves stereoselectivity, drug displacement and synergism effects. Under protein-drug binding equilibrium, the unbound concentrations of drug enantiomers were measured by frontal analysis (FA). The stereoselectivity of verapamil (VER) binding to HSA was proved by the different free fractions of two enantiomers. In physiological pH (7.4, ionic strength 0.17 phosphate buffer) when 300 microM (+/-) VER were equilibrated with 500 microM HSA, the concentration of unbound S-VER was about 1.7 times its antipode. The binding constants of two enantiomers, K(R-VER) and K(S-VER), were 2670 and 850 M(-1), respectively. However, no obvious stereoselective binding of propranolol (PRO) to HSA was observed. Trimethyl-beta-cyclodextrin (45 mM) was used as a chiral selector in pH 2.5 phosphate buffer. Several drug systems were studied by the method. When ibuprofen (IBU) was added into VER-HSA solution. R-VER was partially displaced while S-VER was not displaced at all. A binding synergism effect between bupivacaine (BUP) and verapamil was observed and further study suggested that verapamil and bupivacaine occupy different binding site of HSA (site II and site III, respectively).

摘要

采用毛细管电泳(CE)研究了药物与人血清白蛋白(HSA)之间的相互作用。这涉及立体选择性、药物置换和协同效应。在蛋白质 - 药物结合平衡状态下,通过前沿分析(FA)测定药物对映体的未结合浓度。维拉帕米(VER)与HSA结合的立体选择性通过两种对映体不同的游离分数得以证明。在生理pH值(7.4,离子强度0.17的磷酸盐缓冲液)下,当300微摩尔(±)VER与500微摩尔HSA平衡时,未结合的S - VER浓度约为其对映体的1.7倍。两种对映体的结合常数K(R - VER)和K(S - VER)分别为2670和850 M⁻¹。然而,未观察到普萘洛尔(PRO)与HSA有明显的立体选择性结合。在pH 2.5的磷酸盐缓冲液中,使用三甲基 - β - 环糊精(45 mM)作为手性选择剂。用该方法研究了几种药物体系。当将布洛芬(IBU)加入VER - HSA溶液中时,R - VER被部分置换,而S - VER完全未被置换。观察到布比卡因(BUP)与维拉帕米之间存在结合协同效应,进一步研究表明维拉帕米和布比卡因分别占据HSA的不同结合位点(分别为位点II和位点III)。

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