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首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Uptake and glutathione conjugation of ethacrynic acid and efflux of the glutathione adduct by periportal and perivenous rat hepatocytes.
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Uptake and glutathione conjugation of ethacrynic acid and efflux of the glutathione adduct by periportal and perivenous rat hepatocytes.

机译:肝细胞的摄取和谷胱甘肽的共轭以及谷胱甘肽加合物的流出由大鼠的门静脉和静脉周围的肝细胞引起。

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摘要

We assessed the impact of zonal factors on the hepatic reduced glutathione (GSH) conjugation of ethacrynic acid (EA). Uptake of EA by enriched periportal (PP) and perivenous (PV) rat hepatocytes was characterized by both saturable (V(max)(uptake) = 3.4 +/- 1.7 and 3. 2 +/- 0.8 nmol/min/mg protein and K(m)(uptake) = 51 +/- 13 and 44 +/- 15 microM) and nonsaturable (12 +/- 5 and 12 +/- 3 microl/min/mg protein) components. Values for the overall GSH conjugation rates of EA (200 microM) were similar among the zonal hepatocytes and resembled those for the influx transport rates. In the absence of the hepatocyte membrane, GSH conjugation in PV and PP hepatocyte cytosol was similar, but a higher perivenous GSH conjugation activity toward EA (PV/PP of 2.4) that mirrored the higher PV/PP ratios of immunodetectable GSTs Ya (1.7) and Yb2 (2.5) was found in cell lysates obtained by the dual-digitonin-pulse perfusion technique. The GSH conjugation rates in the subcellular fragments were, however, much greater than those observed for intact hepatocytes. Efflux rates of the glutathione conjugate EA-SG from zonal hepatocytes were similar, as were levels of the immunodetectable multidrug-resistance protein 2/canalicular multispecific organic anion transporter (Mrp2/cMoat) in the 100,000g pellets. The composite results suggest that the GSTs responsible for EA metabolism are more abundant in the PV region, albeit that the gradient of enzymatic activities is shallow. Despite the existence of zonal metabolic activity, the overall GSH conjugation rate of EA is homogeneous among cells because the reaction is rate limited by uptake, which occurs evenly. Results on EA-SG efflux suggest the acinar homogeneity in Mrp2/cMoat function for canalicular transport.
机译:我们评估了区域性因素对乙炔酸(EA)肝脏还原型谷胱甘肽(GSH)结合的影响。丰富的门静脉(PP)和静脉(PV)大鼠肝细胞对EA的摄取均以可饱和(V(max)(摄取)= 3.4 +/- 1.7和3. 2 +/- 0.8 nmol / min / mg蛋白质和K(m)(摄取)= 51 +/- 13和44 +/- 15 microM)和不饱和的(12 +/- 5和12 +/- 3 microl / min / mg蛋白质)成分。区域性肝细胞中EA的总GSH结合率(200 microM)值相似,与内流转运率相似。在没有肝细胞膜的情况下,PV和PP肝细胞胞浆中的GSH缀合相似,但是对EA的较高静脉GSH缀合活性(PV / PP为2.4)反映了免疫检测GST Ya(1.7)的较高PV / PP比。在通过双洋地黄皂苷脉冲灌注技术获得的细胞裂解物中发现了Yb2(2.5)。然而,亚细胞片段中的GSH结合率比完整肝细胞中观察到的要高得多。谷胱甘肽结合物EA-SG从区域肝细胞中的流出速率与100,000g沉淀物中免疫检测的多药耐药蛋白2 /小管多特异性有机阴离子转运蛋白(Mrp2 / cMoat)的水平相似。综合结果表明,尽管酶活性的梯度很浅,但负责PV区域中EA代谢的GST却更为丰富。尽管存在区域性代谢活性,但由于反应受吸收速率限制(均匀发生),因此EA在细胞之间的总GSH偶联率是均匀的。 EA-SG外排的结果表明,Mrp2 / cMoat功能在腺泡运输中具有腺泡均匀性。

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