首页> 外文期刊>Journal of Veterinary Pharmacology and Therapeutics >External validation of pharmacokinetic and pharmacodynamic models of microemulsion and long-chain triglyceride emulsion propofol in beagle dogs.
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External validation of pharmacokinetic and pharmacodynamic models of microemulsion and long-chain triglyceride emulsion propofol in beagle dogs.

机译:外部验证比格犬中微乳和长链甘油三酸酯乳化丙泊酚的药代动力学和药效学模型。

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摘要

This study aimed at assessing the predictive performance of a target-controlled infusion (TCI) system, which incorporates canine PK-PD models for microemulsion and long-chain triglyceride emulsion (LCT) propofol and at investigating time independency of propofol effect on the observed electroencephalographic approximate entropy (ApEn) in TCI. Using a crossover design with a 7-day washout period, 28 healthy beagle dogs were randomized to receive TCI of both formulations in a stepwise or constant manner. Plasma propofol concentrations and ApEn were measured at preset intervals. Pooled biases, inaccuracies, divergences, and wobbles in pharmacokinetic and pharmacodynamic predictions were 2.1% (95% CI: -0.8 to 4.9), 18.1% (15.6-20.5), 1.9%/h, 7.3% (5.4-9.3), and -0.5% (-2.6 to 1.6), 8.7% (7.3-10.1), 2.5%/h, 6.0% (4.1-7.2) for microemulsion propofol, and -9.3% (-11.6 to -6.9), 20.1% (18.2-22.0), 5.1%/h, 7.6% (6.1-9.1) and 5.6% (4.1-7.1), 8.0% (6.9-9.3), 4.7%/h, 4.1% (3.1-5.1) for LCT propofol. Observed ApEn values over time were statistically not different across all time points in a TCI with constant manner. Canine PK-PD model of microemulsion propofol showed good predictive performances. Propofol effect (ApEn) was time independent as long as time is allowed for equilibration.
机译:这项研究旨在评估目标控制输注(TCI)系统的预测性能,该系统结合了用于微乳和长链甘油三酸酯乳剂(LCT)丙泊酚的犬PK-PD模型,并研究了丙泊酚对观察到的脑电图的时间独立性TCI中的近似熵(ApEn)。使用具有7天清除期的交叉设计,随机将28只健康的比格犬以逐步或恒定的方式接受两种配方的TCI。以预设的时间间隔测量血浆丙泊酚浓度和ApEn。药代动力学和药效学预测中的偏见,不准确性,差异和摆动汇总为2.1%(95%CI:-0.8至4.9),18.1%(15.6-20.5),1.9%/ h,7.3%(5.4-9.3)和-0.5%(-2.6至1.6),8.7%(7.3-10.1),2.5%/ h,微乳液丙泊酚为6.0%(4.1-7.2)和-9.3%(-11.6至-6.9),20.1%(18.2) LCT异丙酚的-22.0),5.1%/ h,7.6%(6.1-9.1)和5.6%(4.1-7.1),8.0%(6.9-9.3),4.7%/ h,4.1%(3.1-5.1)。在TCI中,以恒定的方式在所有时间点上随时间观察到的ApEn值在统计上均无差异。微乳丙泊酚的犬PK-PD模型具有良好的预测性能。只要允许时间达到平衡,异丙酚​​效应(ApEn)就与时间无关。

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