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Sequential model-based A- and V-optimal design of experiments for building fundamental models of pharmaceutical production processes

机译:基于顺序模型的A和V最优实验设计,用于建立药品生产过程的基本模型

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Sequential model-based A-and V-optimal experimental designs are known to be effective for maximizing the information content of data, leading to reliable parameter estimates and model predictions. A- and V-optimal designs require inversion of the Fisher Information Matrix (FIM), which may be noninvertible especially for fundamental models with many parameters. In this study, two different methodologies for selecting sequential approximately A-and V-optimal experiments are compared for situations where the FIM is noninvertible. The first approach, called Leave Out (LO) approach, finds and leaves out problematic parameters that make the FIM noninvertible and the second approach, called Pseudoinverse (PI) approach, uses a Moore-Penrose pseudoinverse of the FIM. Comparisons are carried out using a Michaelis Menten reaction dynamic model for production of a pharmaceutical agent. Monte Carlo simulations indicate, for both A-and V-optimal situations, that designed experiments using the LO approach are superior to designs obtained by the PI approach. (C) 2019 Elsevier Ltd. All rights reserved.
机译:已知基于顺序模型的A和V最佳实验设计对于最大化数据的信息含量是有效的,从而导致可靠的参数估计和模型预测。 A和V最佳设计需要Fisher信息矩阵(FIM)的求逆,这可能是不可逆的,尤其是对于具有许多参数的基本模型而言。在这项研究中,比较了在FIM不可逆的情况下选择顺序近似A和V最佳实验的两种不同方法。第一种方法称为“离开”(LO)方法,查找并排除了使FIM不可逆的有问题的参数,第二种方法称为“伪逆”(PI)方法,它使用FIM的Moore-Penrose伪逆。使用Michaelis Menten反应动力学模型进行比较以生产药剂。蒙特卡洛仿真表明,对于A和V最优情况,使用LO方法设计的实验均优于通过PI方法获得的设计。 (C)2019 Elsevier Ltd.保留所有权利。

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