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一种捕捉大鼠体温、心率和血压不对称昼夜基线的药效学周转模型:耐受性和动物处理效应方面的挑战。

A pharmacodynamic turnover model capturing asymmetric circadian baselines of body temperature, heart rate and blood pressure in rats: challenges in terms of tolerance and animal-handling effects.

作者信息

Sällström Björn, Visser Sandra A G, Forsberg Tomas, Peletier Lambertus A, Ericson Ann-Christine, Gabrielsson Johan

机构信息

PKPD section, Local Discovery Research Area CNS & Pain Control, AstraZeneca R&D Södertälje, B231, SE-151 85, Södertälje, Sweden.

出版信息

J Pharmacokinet Pharmacodyn. 2005 Dec;32(5-6):835-59. doi: 10.1007/s10928-005-0087-2.

Abstract

This study presents development and behaviour of a feedback turnover model that mimics asymmetric circadian oscillations of body temperature, blood pressure and heart rate in rats. The study also includes an application to drug-induced hypothermia, tolerance and handling effects. Data were collected inn normotensive Sprague-Dawley rats, housed at 25 degrees C with a 12:12 hr light dark cycle (light on at 06:00 am) and with free access of food and water. The model consisted of two intertwined parallel compartments which captured a free-running rhythm with a period close to but not exactly 24 hrs. The free-running rhythm was synchronised to exactly 24 hrs by the environmental timekeeper (12:12 hr light on/off cycle) in experimental settings. The baseline model was fitted to a standardised 24-hr period derived from mean data of six animals over a period of nine consecutive days. The first-order rate constants related to the turnover of the baseline temperature, alpha and beta, were 0.026 min(-1) (+/-5%) and 0.0037 min(-1) (+/-3%). The alpha and beta parameters are approximately 2/transition time between day and night and 2/night time, respectively. The day:night timekeeper g(t), reference point T(ref) and amplitude were 0.053(+/-2%), 37.3(+/-0.02%) and 3.3% (+/-2%), respectively. Simulations with the baseline model revealed stable oscillations (free-running rhythm) in the absence of the timekeeper. This temperature-time profile was then symmetric and had a smaller amplitude, with a slightly shorter period and less pronounced temperature shift as compared to the profile in the presence of an external Timekeeper. Fitting the model to 96 hr mean profiles of blood pressure and heart rate from 10 control animals demonstrated the usefulness of the model. Simulations of the integrated temperature model succeeded in mimicking other modes of administration such as oral dosing.

摘要

本研究展示了一种反馈周转模型的发展及行为,该模型模拟了大鼠体温、血压和心率的不对称昼夜节律振荡。该研究还包括其在药物诱导的体温过低、耐受性及处理效应方面的应用。数据收集于正常血压的斯普拉格 - 道利大鼠,饲养在25摄氏度环境中,光照 - 黑暗周期为12:12小时(早上6点开灯),可自由获取食物和水。该模型由两个相互交织的平行隔室组成,其捕捉到一个接近但不完全为24小时的自由运行节律。在实验环境中,该自由运行节律通过环境计时装置(12:12小时光照开/关周期)同步至精确的24小时。基线模型拟合至从六只动物连续九天的平均数据得出的标准化24小时周期。与基线温度周转相关的一级速率常数α和β分别为0.026分钟⁻¹(±5%)和0.0037分钟⁻¹(±3%)。α和β参数分别约为昼夜转换时间的2倍和夜间时间的2倍。昼夜计时装置g(t)、参考点T(ref)和振幅分别为0.053(±2%)、37.3(±0.02%)和3.3%(±2%)。基线模型的模拟显示在没有计时装置的情况下存在稳定振荡(自由运行节律)。该温度 - 时间曲线随后是对称的,且振幅较小,与存在外部计时装置时的曲线相比,周期略短且温度变化不太明显。将该模型拟合至10只对照动物的96小时血压和心率平均曲线证明了该模型的实用性。整合温度模型的模拟成功地模拟了其他给药方式,如口服给药。

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