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甲泼尼龙对葡萄糖调节的药效学。II. 正常大鼠

Pharmacodynamics of glucose regulation by methylprednisolone. II. normal rats.

作者信息

Jin Jin Y, Jusko William J

机构信息

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

出版信息

Biopharm Drug Dispos. 2009 Jan;30(1):35-48. doi: 10.1002/bdd.642.

Abstract

A physiologic pharmacodynamic model was developed to jointly describe the effects of methylprednisolone (MPL) on adrenal suppression and glycemic control in normal rats. Six groups of animals were given MPL intravenously at 0, 10 and 50 mg/kg, or by subcutaneous 7 day infusion at rates of 0, 0.1 and 0.3 mg/kg/h. Plasma concentrations of MPL, corticosterone (CST), glucose and insulin were determined at various times up to 72 h after injection and 336 h after infusion. The pharmacokinetics of MPL was described by a two-compartment model. A circadian rhythm for CST was found in untreated rats with a stress-altered baseline caused by handling, which was captured by a circadian harmonic secretion rate with an increasing mesor. All drug treatments caused CST suppression. Injection of MPL caused temporary increases in glucose over 4 h. Insulin secretion was thereby stimulated yielding a later peak around 6 h. In turn, insulin can normalize glucose. However, long-term dosing caused continuous hyperglycemia during and after infusion. Hyperinsulinemia was achieved during infusion, but diminished immediately after dosing despite the high glucose concentration. The effects of CST and MPL on glucose production were described with a competitive stimulation function. A disease progression model incorporating reduced endogenous glucose uptake/utilization was used to describe glucose metabolism under different treatments. The results exemplify the roles of endogenous and exogenous hormones in mediating glucose dynamics. The pharmacokinetic/pharmacodynamic model is valuable for quantitating diabetogenic effects of corticosteroid treatments and provides mechanistic insights into the hormonal control of the metabolic system.

摘要

建立了一个生理药代动力学模型,以联合描述甲基强的松龙(MPL)对正常大鼠肾上腺抑制和血糖控制的影响。六组动物分别静脉注射0、10和50mg/kg的MPL,或皮下7天输注,速率分别为0、0.1和0.3mg/kg/h。在注射后长达72小时和输注后336小时的不同时间点测定MPL、皮质酮(CST)、葡萄糖和胰岛素的血浆浓度。MPL的药代动力学用二室模型描述。在未处理的大鼠中发现CST存在昼夜节律,处理引起的应激改变了基线,通过具有增加中值的昼夜谐波分泌率来捕捉。所有药物治疗均导致CST抑制。注射MPL导致4小时内葡萄糖暂时升高。从而刺激胰岛素分泌,在6小时左右出现后期峰值。反过来,胰岛素可以使葡萄糖正常化。然而,长期给药导致输注期间和之后持续高血糖。输注期间实现了高胰岛素血症,但给药后尽管葡萄糖浓度很高,高胰岛素血症立即减弱。用竞争性刺激函数描述CST和MPL对葡萄糖生成的影响。使用包含内源性葡萄糖摄取/利用减少的疾病进展模型来描述不同治疗下的葡萄糖代谢。结果例证了内源性和外源性激素在介导葡萄糖动态变化中的作用。该药代动力学/药效学模型对于定量皮质类固醇治疗的致糖尿病作用具有重要价值,并为代谢系统的激素控制提供了机制性见解。

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