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A Bayesian approach for estimating detection times in horses : exploring the pharmacokinetics of a urinary acepromazine metabolite

机译:一种估计马匹检测时间的贝叶斯方法:探索尿液中乙酰丙嗪代谢物的药代动力学

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摘要

We describe the population pharmacokinetics of an acepromazine (ACP) metabolite (2-(1-hydroxyethyl)promazine) (HEPS) in horses for the estimation of likely detection times in plasma and urine. Acepromazine (30 mg) was administered to 12 horses, and blood and urine samples were taken at frequent intervals for chemical analysis. A Bayesian hierarchical model was fitted to describe concentration-time data and cumulative urine amounts for HEPS. The metabolite HEPS was modelled separately from the parent ACP as the half-life of the parent was considerably less than that of the metabolite. The clearance ($Cl/F_{PM}$) and volume of distribution ($V/F_{PM}$), scaled by the fraction of parent converted to metabolite, were estimated as 769 L/h and 6874 L, respectively. For a typical horse in the study, after receiving 30 mg of ACP, the upper limit of the detection time was 35 hours in plasma and 100 hours in urine, assuming an arbitrary limit of detection of 1 $mu$g/L, and a small ($pprox 0.01$) probability of detection. The model derived allowed the probability of detection to be estimated at the population level. This analysis was conducted on data collected from only 12 horses, but we assume that this is representative of the wider population.
机译:我们描述了马匹中乙酰丙嗪(ACP)代谢产物(2-(1-羟乙基)丙嗪)(HEPS)的群体药代动力学,用于估计血浆和尿液中可能的检测时间。给12匹马服用Acepromazine(30 mg),并定期抽血和尿液进行化学分析。使用贝叶斯分层模型描述HEPS的浓度时间数据和累积尿量。代谢物HEPS与母体ACP分开进行建模,因为母体的半衰期明显小于代谢物的半衰期。清除率($ Cl / F_ {PM} $)和分布量($ V / F_ {PM} $),按转化为代谢物的母体比例换算,估计分别为769 L / h和6874L。对于本研究中的典型马,在接受30 mg的ACP后,假设任意检测极限为1μg/ g,则血浆中检测时间的上限为35小时,尿液中检测时间的上限为100小时,并且侦测的可能性很小($ 大约0.01 $)。导出的模型允许在总体水平上估计检测概率。这项分析是基于仅从12匹马中收集的数据进行的,但是我们假设这代表了更广泛的种群。

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