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模拟皮质类固醇对大鼠肝脏酪氨酸转氨酶动力学的受体/基因介导效应:内源性和外源性皮质类固醇的双重调节

Modeling receptor/gene-mediated effects of corticosteroids on hepatic tyrosine aminotransferase dynamics in rats: dual regulation by endogenous and exogenous corticosteroids.

作者信息

Hazra Anasuya, Pyszczynski Nancy, DuBois Debra C, Almon Richard R, Jusko William J

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy and Pharmaceutical Sciences, State University of New York at Buffalo, Buffalo, NY 14260, USA.

出版信息

J Pharmacokinet Pharmacodyn. 2007 Oct;34(5):643-67. doi: 10.1007/s10928-007-9063-3. Epub 2007 Jun 26.

Abstract

Receptor/gene-mediated effects of corticosteroids on hepatic tyrosine aminotransferase (TAT) were evaluated in normal rats. A group of normal male Wistar rats were injected with 50 mg/kg methylprednisolone (MPL) intramuscularly at the nadir of their plasma corticosterone (CST) rhythm (early light cycle) and sacrificed at various time points up to 96 h post-treatment. Blood and livers were collected to measure plasma MPL, CST, hepatic glucocorticoid receptor (GR) mRNA, cytosolic GR density, TAT mRNA, and TAT activity. The pharmacokinetics of MPL showed bi-exponential disposition with two first-order absorption components from the injection site and bioavailability was 21%. Plasma CST was reduced after MPL dosing, but resumed its daily circadian pattern within 36 h. Cytosolic receptor density was significantly suppressed (90%) and returned to baseline by 72 h resuming its biphasic pattern. Hepatic GR mRNA follows a circadian pattern which was disrupted by MPL and did not return during the study. MPL caused significant down-regulation (50%) in GR mRNA which was followed by a delayed rebound phase (60-70 h). Hepatic TAT mRNA and activity showed up-regulation as a consequence of MPL, and returned to their circadian baseline within 72 and 24 h of treatment. A mechanistic receptor/gene-mediated pharmacokinetic/pharmacodynamic model was able to satisfactorily describe the complex interplay of exogenous and endogenous corticosteroid effects on hepatic GR mRNA, cytosolic free GR, TAT mRNA, and TAT activity in normal rats.

摘要

在正常大鼠中评估了皮质类固醇对肝酪氨酸转氨酶(TAT)的受体/基因介导作用。一组正常雄性Wistar大鼠在其血浆皮质酮(CST)节律的最低点(早光照周期)肌肉注射50mg/kg甲泼尼龙(MPL),并在治疗后长达96小时的不同时间点处死。收集血液和肝脏以测量血浆MPL、CST、肝糖皮质激素受体(GR)mRNA、胞浆GR密度、TAT mRNA和TAT活性。MPL的药代动力学显示为双指数分布,有两个来自注射部位的一级吸收成分,生物利用度为21%。MPL给药后血浆CST降低,但在36小时内恢复其每日昼夜节律模式。胞浆受体密度显著受抑制(90%),并在72小时恢复到基线,恢复其双相模式。肝GR mRNA遵循昼夜节律模式,被MPL破坏,在研究期间未恢复。MPL导致GR mRNA显著下调(50%),随后是延迟的反弹期(60 - 70小时)。肝TAT mRNA和活性因MPL而出现上调,并在治疗后72小时和24小时内恢复到昼夜节律基线。一个受体/基因介导的药代动力学/药效学机制模型能够令人满意地描述外源性和内源性皮质类固醇对正常大鼠肝GR mRNA、胞浆游离GR、TAT mRNA和TAT活性的复杂相互作用。

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