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对从斯普拉格-道利大鼠、Wistar大鼠和多药耐药相关蛋白2缺陷型Wistar(TR(-))大鼠分离的培养肝细胞中5(6)-羧基-2',7'-二氯荧光素(CDF)的胆汁排泄和窦状隙排泄进行定量分析。

Quantification of biliary excretion and sinusoidal excretion of 5(6)-carboxy-2',7'-dichlorofluorescein (CDF) in cultured hepatocytes isolated from Sprague Dawley, Wistar and Mrp2-deficient Wistar (TR(-)) rats.

作者信息

Ellis L C J, Grant M H, Hawksworth G M, Weaver R J

机构信息

Section of Translational Medicine, Division of Applied Medicine, Polwarth Building, Foresterhill, Aberdeen AB25 2ZD, UK.

Department of Biomedical Engineering, Bioengineering Unit, University of Strathclyde, Glasgow G4 0NW, UK.

出版信息

Toxicol In Vitro. 2014 Sep;28(6):1165-75. doi: 10.1016/j.tiv.2014.05.010. Epub 2014 Jun 4.

Abstract

Hepatic efflux of drug candidates is an important issue in pre-clinical drug development. Here we utilise a method which quantifies and distinguishes efflux of drugs at the canalicular and sinusoidal membranes in rat hepatocyte cultures. Bi-phasic kinetics of transport of 5(6)-carboxydichlorofluorescein (CDF) at the canalicular membrane was demonstrated in Sprague Dawley (SD) and Wistar (W) rat hepatocytes. The high affinity component (Km=3.2±0.8μM (SD), 9.0±3.1μM (W)) was attributed to Mrp2-mediated transport, the low affinity component (Km=192.1±291.5μM (SD), 69.2±36.2μM (W)) may be attributed to transport involving a separate Mrp2 binding site. Data from membranes (Hill coefficient (h)=2.0±0.5) and vesicles (h=1.6±0.2) expressing Mrp2 and from SD (h=1.6±0.4) and Wistar (h=4.0±0.6) hepatocytes suggests transport involves more than one binding site. In TR(-) hepatocytes, CDF efflux was predominantly over the sinusoidal membrane (Km=100.7±36.0μM), consistent with low abcc2 (Mrp2) expression and compensatory increase in abcc3 (Mrp3) expression. This report shows the potential of using this in vitro method to model changes in biliary excretion due to alterations in transporter expression.

摘要

在临床前药物开发中,候选药物的肝脏外排是一个重要问题。在此,我们采用了一种方法,该方法可对大鼠肝细胞培养物中胆小管和窦状隙膜处药物的外排进行定量和区分。在斯普拉格-道利(SD)大鼠和Wistar(W)大鼠肝细胞中,证明了5(6)-羧基二氯荧光素(CDF)在胆小管膜处的双相转运动力学。高亲和力组分(Km = 3.2±0.8μM(SD),9.0±3.1μM(W))归因于Mrp2介导的转运,低亲和力组分(Km = 192.1±291.5μM(SD),69.2±36.2μM(W))可能归因于涉及单独Mrp2结合位点的转运。来自表达Mrp2的膜(希尔系数(h)= 2.0±0.5)和囊泡(h = 1.6±0.2)以及来自SD(h = 1.6±0.4)和Wistar(h = 4.0±0.6)肝细胞的数据表明,转运涉及多个结合位点。在TR(-)肝细胞中,CDF外排主要发生在窦状隙膜上(Km = 100.7±36.0μM),这与低abcc2(Mrp2)表达和abcc3(Mrp3)表达的代偿性增加一致。本报告显示了使用这种体外方法模拟由于转运体表达改变而导致的胆汁排泄变化的潜力。

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