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Comparisons Between Hamiltonian Monte Carlo and Maximum A Posteriori For A Bayesian Model For Apixaban Induction DoseANDDose Personalization

机译:Hamiltonian Monte Carlo与Apixaban Incuction Dosanddose个性化的贝叶斯模型的最大探险模型的比较

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Precision medicine’s slogan is "right drug - right patient - right time." Implicit in the slogan is "right dose"; however, determining the right dose for any one patient can be challenging when dose-response data are limited. Bayesian methods, with their ability to explicitly incorporate prior information to supplement limited data, have been proposed as a solution to this problem. Although Hamiltonian Monte Carlo (HMC) is a leading methodology for inference in Bayesian models because of its ability to capture posterior distributions with high fidelity, dose personalization studies commonly use simpler Maximum A Posteriori (MAP) inference methods. The impact of the choice of inference engine on dose decision-making has not been explored. To better understand this issue, we perform a simulation study characterizing the differences between inferences made via MAP and HMC for personalized dosing strategies. The simulation study uses a new Bayesian pharmacokinetic model for apixaban pharmacokinetics written in an open source Bayesian language; the model code and posterior summaries of all parameters will be publicly available. We demonstrate that the differences between HMC and MAP are non-trivial and can greatly affect the choices surrounding dose selection for personalized medicine.
机译:精密医学的口号是“正确的药物 - 正确的患者 - 正确的时间”。在口号中隐含为“右剂量”;然而,当剂量响应数据有限时,确定任何一个患者的右剂量可能是挑战。贝叶斯方法,其能够明确地将事先信息纳入补充有限的数据,已提出对此问题的解决方案。虽然Hamiltonian Monte Carlo(HMC)是贝叶斯模型推理的主要方法,因为其能够捕获高保真的后分布,剂量个性化研究通常使用更简单的后验(MAP)推理方法。尚未探讨推理引擎选择对剂量决策的影响。为了更好地理解这个问题,我们执行一个仿真研究,其特征,其通过地图和HMC进行了个性化给药策略所做的推断之间的差异。仿真研究采用了一种新的贝叶斯药代动力学模型,用于在开源贝叶斯语中编写的Apixaban药代动力学;所有参数的模型代码和后序将是公开的。我们证明HMC和地图之间的差异是非微不足道的,并且可以极大地影响个性化药物围绕剂量选择的选择。

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