HEP G2 CELL-LINE AS A HUMAN-MODEL FOR SULFATE CONJUGATION OF DRUGS

被引:31
|
作者
SHWED, JA
WALLE, UK
WALLE, T
机构
[1] MED UNIV S CAROLINA,DEPT HOSP PHARM,171 ASHLEY AVE,CHARLESTON,SC 29425
[2] MED UNIV S CAROLINA,DEPT CELL & MOLEC PHARMACOL,CHARLESTON,SC 29425
[3] MED UNIV S CAROLINA,DEPT EXPTL THERAPEUT,CHARLESTON,SC 29425
来源
XENOBIOTICA | 1992年 / 22卷 / 08期
关键词
D O I
10.3109/00498259209049903
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
1. The objective of this study was to examine the usefulness of the hepatoma cell line Hep G2 as a model for human sulphoconjugation of drugs, in particular stereoselective conjugation. 2. Using the substrates p-nitrophenol and dopamine, we found sulphation activities consistent with the presence of both the phenol (P) and the monoamine (M) form of the human phenolsulphotransferases in these cells. 3. The K(mapp) was 3.0 muM for the sulphation of p-nitrophenol. This activity was inhibited selectively by 2,6-dichloro-4-nitrophenol, IC50 6 muM. The K(mapp) was 39 muM for the sulphation of dopamine. This activity was selectively inhibited by elevated temperature. 4. The chiral adrenergic drugs (+/-)-terbutaline and (+/-)-4-hydroxypropranolol were both sulphated stereoselectively with K(mapp) and V(maxapp) values for each enantiomer virtually identical to previous observations with human liver cytosol. 5. In a direct comparison, the estimated activity of the P form of phenolsulphotransferase in the Hep G2 cell line was 30% of that in human liver, whereas, surprisingly, the activity of the M form of phenolsulphotransferase was 4.5 times higher in the Hep G2 cells than in the liver.
引用
收藏
页码:973 / 982
页数:10
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