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药物和化学物质对肝酶及蛋白质的影响。II. 各种巴比妥类药物对肝细胞质有机阴离子结合蛋白诱导和减少的影响。

Influence of drugs and chemicals upon hepatic enzymes and proteins. II. The effects of various barbiturates on the induction and reduction of hepatic cytoplasmic organic anion-binding proteins.

作者信息

Adachi Y, Yamamoto T

出版信息

Gastroenterol Jpn. 1976;11(1):23-30. doi: 10.1007/BF02775447.

Abstract

The effects of seven barbiturates (phenobarbital, three N-phenylbarbiturates and three N-cyclohexylbarbiturates) on the hepatic cytoplasmic organic anion-binding proteins, Y and Z, were investigated in an attempt to observe the structure-activity relationship of baributrates to induction and reduction of these two proteins. Sulfobromophthalein (BSP) was fully bound by the Y and Z proteins at ten minutes of mixing with the 10,5000 X g supernate. In low concentrations of BSP, saturation of binding of BSP by the Z protein was very low, and with increasing concentration, BSP-binding by the Z protein increased rapidly. The Y protein bound BSP sufficiently even in low concentrations of the dye. BSP-binding capacity of the Yprotein was increased by phenobarbital, phetharbital and bucolome, and decreased by one of the N-phenylbarbiturates. BSP-binding capacity of the Zprotein tended to be decreased by phenobarbital and phetharbital, but to be increased by bucolome. The other N-phenyl- and N-cyclohexylbarbiturates had no effect on the binding capacities of the two proteins. From these results it was concluded that the regulation by the barbiturates of cytoplasmic proteins is different from that of the microsomal enzymes, and that both type and structural relation are important in the induction and reduction of the Y and Z proteins.

摘要

研究了七种巴比妥酸盐(苯巴比妥、三种N-苯基巴比妥酸盐和三种N-环己基巴比妥酸盐)对肝细胞质有机阴离子结合蛋白Y和Z的影响,以观察巴比妥酸盐与这两种蛋白诱导和减少之间的构效关系。磺溴酞钠(BSP)与105000×g上清液混合10分钟时,可被Y和Z蛋白完全结合。在低浓度的BSP中,Z蛋白对BSP的结合饱和度很低,随着浓度增加,Z蛋白对BSP的结合迅速增加。即使在低浓度染料情况下,Y蛋白也能充分结合BSP。苯巴比妥、苯乙巴比妥和布可隆可增加Y蛋白的BSP结合能力,而一种N-苯基巴比妥酸盐则使其降低。苯巴比妥和苯乙巴比妥倾向于降低Z蛋白的BSP结合能力,而布可隆则使其增加。其他N-苯基和N-环己基巴比妥酸盐对这两种蛋白的结合能力没有影响。从这些结果得出结论,巴比妥酸盐对细胞质蛋白的调节与微粒体酶不同,而且类型和结构关系在Y和Z蛋白的诱导和减少中都很重要。

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