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低剂量苯巴比妥对肝微粒体UDP-葡萄糖醛酸转移酶活性的影响。

Effect of low-dose phenobarbital on hepatic microsomal UDP-glucuronyl transferase activity.

作者信息

Tavoloni N, Wittman R, Jones M J, Berk P D

出版信息

Biochem Pharmacol. 1983 Jul 15;32(14):2143-7. doi: 10.1016/0006-2952(83)90219-8.

Abstract

To determine whether hepatic microsomal enzyme induction occurs in rats following administration of phenobarbital at doses similar to those used in humans (0.5 to 7.5 mg/kg), UDP-glucuronyl transferase (UDPGT) and cytochrome P-450 activities were measured in liver homogenate and microsomal preparations from control rats and rats treated for 6 days with phenobarbital at 1 and 3 mg per kg per day. While no significant increases in liver weight and protein content of homogenate and microsomal preparations were observed with either dose of the drug, both UDPGT and P-450 activities were enhanced significantly following administration of phenobarbital at 3 mg per kg per day. The activity of P-450 was increased by approximately 30% and that of UDPGT by 15-24 and 45-66%, respectively, employing bilirubin and p-nitrophenol as the acceptor substrate. The extent of induction of bilirubin or p-nitrophenol UDPGT was similar when measured with "native" enzyme or with enzyme activated by UDP-N-acetyl glucosamine, digitonin or deoxycholate. These data suggest that the discordant effects of phenobarbital on UDPGT and cytochrome P-450 previously reported in humans and rats may not be attributable solely to differences in the drug doses employed.

摘要

为了确定给予大鼠类似于人类所用剂量(0.5至7.5毫克/千克)的苯巴比妥后是否会发生肝微粒体酶诱导,在来自对照大鼠以及每天按1毫克/千克和3毫克/千克给予苯巴比妥处理6天的大鼠的肝脏匀浆和微粒体制剂中测量了尿苷二磷酸葡萄糖醛酸基转移酶(UDPGT)和细胞色素P - 450活性。虽然两种剂量的药物均未观察到肝脏重量以及匀浆和微粒体制剂的蛋白质含量有显著增加,但每天按3毫克/千克给予苯巴比妥后,UDPGT和P - 450活性均显著增强。以胆红素和对硝基苯酚作为受体底物时,P - 450的活性分别增加了约30%,UDPGT的活性分别增加了15 - 24%和45 - 66%。用“天然”酶或用经UDP - N - 乙酰葡糖胺、洋地黄皂苷或脱氧胆酸盐激活的酶测量时,胆红素或对硝基苯酚UDPGT的诱导程度相似。这些数据表明,先前在人类和大鼠中报道的苯巴比妥对UDPGT和细胞色素P - 450的不一致影响可能并非仅归因于所用药物剂量的差异。

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