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通过优化剂量选择提高暴露-反应关系的精度。来自使用正电子发射断层扫描(PET)进行受体占有率研究以及神经性疼痛治疗剂量确定研究的实例。

Improved precision of exposure-response relationships by optimal dose-selection. Examples from studies of receptor occupancy using PET and dose finding for neuropathic pain treatment.

作者信息

Kågedal Matts, Karlsson Mats O, Hooker Andrew C

机构信息

Department of Pharmaceutical Biosciences, Uppsala University, Uppsala, Sweden,

出版信息

J Pharmacokinet Pharmacodyn. 2015 Jun;42(3):211-24. doi: 10.1007/s10928-015-9410-8. Epub 2015 Mar 20.

Abstract

An understanding of the relationship between drug exposure and response is a fundamental basis for any dosing recommendation. We investigate optimal dose-selection for two different types of studies, a receptor occupancy study assessed by positron emission tomography (PET) and a dose-finding study in neuropathic pain treatment. For the PET-study, an inhibitory E-max model describes the relationship between drug exposure and displacement of a radioligand from specific receptors in the brain. The model has a mechanistic basis in the law of mass action and the affinity parameter (Ki PL ) is of primary interest. For optimization of the neuropathic pain study, the model is empirical and the exposure response curve itself is of primary interest. An alternative parameterization of the sigmoid Emax model was therefore used where the plasma concentration corresponding to the minimum relevant efficacy was estimated as a parameter. Optimal design methodology was applied using the D-optimal criterion as well as the Ds-optimal criterion where parameters of interest were defined. For the PET-study it was shown that the precision of Ki PL can be improved by inclusion of brain regions with both high and low receptor density and that the need for high doses is reduced when a brain region with low receptor density is included in the analysis. In the case of the neuropathic pain study it was shown that a Ds-optimal study design using the reparameterized Emax model can improve the precision in the minimum effective dose compared to a D-optimal design.

摘要

了解药物暴露与反应之间的关系是任何给药建议的基本依据。我们针对两种不同类型的研究调查了最佳剂量选择,一种是通过正电子发射断层扫描(PET)评估的受体占有率研究,另一种是神经性疼痛治疗中的剂量探索研究。对于PET研究,抑制性E-max模型描述了药物暴露与放射性配体从大脑特定受体上的置换之间的关系。该模型基于质量作用定律具有机制基础,亲和参数(Ki PL)是主要关注对象。为了优化神经性疼痛研究,该模型是经验性的,暴露反应曲线本身是主要关注对象。因此,使用了S形Emax模型的另一种参数化方法,将对应于最小相关疗效的血浆浓度作为一个参数进行估计。采用D-最优准则以及Ds-最优准则应用最优设计方法,其中定义了感兴趣的参数。对于PET研究,结果表明,通过纳入高受体密度和低受体密度的脑区,可以提高Ki PL的精度,并且当分析中纳入低受体密度的脑区时,对高剂量的需求会降低。在神经性疼痛研究中,结果表明,与D-最优设计相比,使用重新参数化的Emax模型的Ds-最优研究设计可以提高最小有效剂量的精度。

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