首页> 外文期刊>Therapeutic Drug Monitoring >Achieving target goals most precisely using nonparametric compartmental models and 'multiple model' design of dosage regimens.
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Achieving target goals most precisely using nonparametric compartmental models and 'multiple model' design of dosage regimens.

机译:使用非参数隔室模型和剂量方案的“多个模型”设计,可以最精确地实现目标目标。

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摘要

Multiple model (MM) design and stochastic control of dosage regimens permit essentially full use of all the information contained in either a Bayesian prior nonparametric EM (NPEM) population pharmacokinetic model or in an MM Bayesian posterior updated parameter set, to achieve and maintain selected therapeutic goals with optimal precision (least predicted weighted squared error). The regimens are visibly more precise in the achievement of desired target goals than are current methods using mean or median population parameter values. Bayesian feedback has now also been incorporated into the MM software. An evaluation of MM dosage design using an NPEM population model versus dosage design based on conventional mean population parameter values is presented, using a population model of vancomycin. Further feedback control was also evaluated, incorporating realistic simulated uncertainties in the clinical environment such as those in the preparation and administration of doses.
机译:多种模型(MM)设计和剂量方案的随机控制,可以基本上充分利用贝叶斯先验非参数EM(NPEM)群体药代动力学模型或MM贝叶斯后验更新参数集中包含的所有信息,以实现并维持所选的治疗方法最佳精度的目标(最小预测加权平方误差)。与使用均值或中位数人口参数值的当前方法相比,该方案在实现预期目标方面明显更精确。贝叶斯反馈现在也已被合并到MM软件中。使用万古霉素的种群模型,提出了使用NPEM种群模型与基于常规平均种群参数值的剂量设计对MM剂量设计的评估。还评估了进一步的反馈控制,纳入了临床环境中现实的模拟不确定性,例如剂量的制备和给药中的不确定性。

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