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首页> 外文期刊>Journal of pharmaceutical sciences. >Relative quantities of catalytically active CYP 2C9 and 2C19 in human liver microsomes: application of the relative activity factor approach.
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Relative quantities of catalytically active CYP 2C9 and 2C19 in human liver microsomes: application of the relative activity factor approach.

机译:人肝微粒体中催化活性CYP 2C9和2C19的相对量:相对活性因子方法的应用。

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The relative catalytic activities of CYP2C9 and CYP2C19 in human liver microsomes has been determined using the approach of relative activity factors (RAFs). Tolbutamide methylhydroxylation and S-mephenytoin 4'-hydroxylation were used as measures of CYP2C9 and CYP2C19 activity, respectively. The kinetics of these reactions were studied in human liver microsomes, in microsomes from human lymphoblastoid cells, and in insect cells expressing CYP2C9 and CYP2C19. RAFs were calculated as the ratio of Vmax (reaction velocity at saturating substrate concentrations) in human liver microsomes of the isoform-specific index reaction divided by the Vmax of the reaction catalyzed by the cDNA expressed isoform. RAFs were also determined for SUPERMIX, a commercially available mixture of cDNA expressed human drug metabolizing CYPs formulated to achieve a balance of enzyme activities similar to that found in human liver microsomes. Lymphoblast RAF2C9 in human liver microsomes ranged from 54 to 145 pmol CYP/mg protein (mean value: 87), while a value of 251 pmol CYP/mg protein was obtained for SUPERMIX. Insect cell RAF2C9 in human liver microsomes ranged from 1.6 to 143 pmol CYP/mg protein (mean value: 49), while a value of 201 pmol CYP/mg protein was obtained for SUPERMIX. Both lymphoblast and insect cell RAF2C19 in human liver microsomes ranged from 4 to 45 pmol CYP/mg protein (mean values: 29 and 28, respectively), while a value of 29 pmol CYP/mg protein was obtained for SUPERMIX. The nature of the cDNA expression system used had no effect on the kinetic parameters of CYP2C9 as a tolbutamide methylhydroxylase, or of CYP2C19 as a S-mephenytoin hydroxylase. However insect cell expressed CYP2C19 (which includes oxidoreductase) had substantially greater activity as a tolbutamide methylhydroxylase when compared to lymphoblast expressed CYP2C19. The ratio of mean lymphoblast-determined RAF2C9 to RAF2C19 in human livers was 3.0 (range 1.6-17.9; n = 10), while this ratio for SUPERMIX was 8.6. The ratio of mean insect cell-determined RAF2C9 to RAF2C19 in human livers was 1.7 (range 0.04-16.2; n = 10), while this ratio for SUPERMIX was 7.0. Neither ratio is in agreement with the 20:1 ratio of immunoquantified levels of CYP2C9 and 2C19 in human liver microsomes reported in previous studies. SUPERMIX may contain catalytically active CYP2C9 in levels higher than those in human liver microsomes.
机译:CYP2C9和CYP2C19在人肝微粒体中的相对催化活性已使用相对活性因子(RAFs)的方法进行了测定。甲苯磺丁酰胺甲基羟化和S-美芬妥英4'-羟化分别用作CYP2C9和CYP2C19活性的量度。在人肝微粒体,人淋巴母细胞样微粒体和表达CYP2C9和CYP2C19的昆虫细胞中研究了这些反应的动力学。 RAF计算为同种型特异性指数反应的人肝微粒体中Vmax(饱和底物浓度下的反应速度)除以cDNA表达的同种型所催化的反应的Vmax之比。还确定了RAF的SUPERMIX,SUPERMIX是cDNA表达的人类药物代谢CYP的可商购混合物,其配方旨在实现类似于人肝微粒体中酶活性的平衡。人肝微粒体中的淋巴母细胞RAF2C9的CYP / mg蛋白范围为54至145 pmol CYP / mg蛋白(平均值:87),而SUPERMIX的蛋白值为251 pmol CYP / mg蛋白。人肝微粒体中的昆虫细胞RAF2C9的CYP / mg蛋白为1.6至143 pmol CYP / mg蛋白,而SUPERMIX获得的CYP / mg蛋白值为201 pmol CYP / mg蛋白。人肝微粒体中的淋巴母细胞和昆虫细胞RAF2C19的浓度范围为4至45 pmol CYP / mg蛋白(平均值分别为29和28),而SUPERMIX的值为29 pmol CYP / mg蛋白。所使用的cDNA表达系统的性质对CYP2C9的动力学参数(作为甲苯磺丁酰胺甲基羟化酶)或CYP2C19的动力学参数(作为S-甲吩妥英羟化酶)没有影响。然而,与淋巴母细胞表达的CYP2C19相比,昆虫细胞表达的CYP2C19(包括氧化还原酶)作为甲苯磺丁酰胺甲基羟化酶的活性明显更高。人肝中平均由淋巴母细胞测定的RAF2C9与RAF2C19的比率为3.0(范围1.6-17.9; n = 10),而SUPERMIX的比率为8.6。人肝脏中昆虫细胞确定的RAF2C9与RAF2C19的平均比例为1.7(范围0.04-16.2; n = 10),而SUPERMIX的比例为7.0。这两个比例均与先前研究中报道的人肝微粒体中CYP2C9和2C19的免疫定量水平的20:1比例不一致。 SUPERMIX可能含有的催化活性CYP2C9的含量高于人肝微粒体中的含量。

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