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原代培养大鼠肝细胞对谷胱甘肽结合物的排泄

Excretion of glutathione conjugates by primary cultured rat hepatocytes.

作者信息

Lindwall G, Boyer T D

出版信息

J Biol Chem. 1987 Apr 15;262(11):5151-8.

PMID:3558387
Abstract

Conjugation of xenobiotics with glutathione occurs commonly within the liver, and these glutathione conjugates are then preferentially excreted into bile. We have characterized this excretory process using primary cultured hepatocytes (24 h). 1-Chloro-2,4-dinitrobenzene rapidly entered the cells and formed a glutathione conjugate, S-(dinitrophenyl)glutathione, irrespective of the temperature of incubation. In contrast, the efflux of the glutathione conjugate was essentially absent in the cold but recovered rapidly upon rewarming of the cells. Therefore, initial rates of efflux of the conjugate at 37 degrees C were measured from cells preloaded biosynthetically at 10 degrees C. Efflux was a saturable process with respect to intracellular S-(dinitrophenyl)glutathione with an apparent Km of 0.58 +/- 0.12 mM and Vmax of 0.15 +/- 0.05 nmol/min/mg of protein. The excretion of S-(dinitrophenyl)glutathione had an energy of activation of 15.3 kcal/mol. The glutathione conjugate of p-nitrobenzylchloride when formed within the hepatocytes acted as a competitive inhibitor of S-(dinitrophenyl)glutathione efflux. Cultured hepatocytes, therefore, appeared to have a specific transport process for the excretion of glutathione conjugates. The addition of S-(dinitrophenyl)glutathione, but not GSH, GSSG, or methionine, to the medium caused a decrease in the rate of efflux of radiolabeled S-(dinitrophenyl)glutathione. The hepatocytes were able, however, to excrete the glutathione conjugate against an excess of extracellular S-(dinitrophenyl)glutathione. This observation suggested that extracellular S-(dinitrophenyl)glutathione, although capable of binding to the carrier, entered the hepatocytes quite slowly relative to rates of efflux. This carrier may function in a manner that would minimize the reuptake by hepatocytes of conjugates that have been excreted into the bile.

摘要

异生素与谷胱甘肽的结合通常发生在肝脏内,然后这些谷胱甘肽结合物会优先排泄到胆汁中。我们使用原代培养的肝细胞(培养24小时)对这一排泄过程进行了表征。1-氯-2,4-二硝基苯迅速进入细胞并形成谷胱甘肽结合物S-(二硝基苯基)谷胱甘肽,无论孵育温度如何。相比之下,谷胱甘肽结合物的外排在低温下基本不存在,但细胞复温后迅速恢复。因此,在37℃下,从在10℃下生物合成预加载的细胞中测量结合物的初始外排速率。外排是一个关于细胞内S-(二硝基苯基)谷胱甘肽的饱和过程,表观Km为0.58±0.12 mM,Vmax为0.15±0.05 nmol/分钟/毫克蛋白质。S-(二硝基苯基)谷胱甘肽的排泄具有15.3千卡/摩尔的活化能。对硝基苄基氯在肝细胞内形成的谷胱甘肽结合物可作为S-(二硝基苯基)谷胱甘肽外排的竞争性抑制剂。因此,培养的肝细胞似乎具有排泄谷胱甘肽结合物的特定转运过程。向培养基中添加S-(二硝基苯基)谷胱甘肽,但不添加谷胱甘肽、氧化型谷胱甘肽或蛋氨酸,会导致放射性标记的S-(二硝基苯基)谷胱甘肽外排速率降低。然而,肝细胞能够逆着过量的细胞外S-(二硝基苯基)谷胱甘肽排泄谷胱甘肽结合物。这一观察结果表明,细胞外S-(二硝基苯基)谷胱甘肽虽然能够与载体结合,但相对于外排速率而言,进入肝细胞的速度相当缓慢。这种载体的作用方式可能是将已排泄到胆汁中的结合物被肝细胞重新摄取的情况降至最低。

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