Isoherranen Nina
Department of Pharmaceutics, School of Pharmacy, University of Washington, Seattle, Washington.
Drug Metab Dispos. 2025 Jan;53(1):100013. doi: 10.1124/dmd.123.000960. Epub 2024 Nov 22.
Physiologically based pharmacokinetic (PBPK) models of small molecules have become mainstream in drug development and in academic research. The use of PBPK models is continuously expanding, with the majority of work now focusing on predictions of drug-drug interactions, drug-disease interactions, and changes in drug disposition across lifespan. Recently, publications that use PBPK modeling to predict drug disposition during pregnancy and in organ impairment have increased reflecting the advances in incorporating diverse physiologic changes into the models. Because of the expanding computational power and diversity of modeling platforms available, the complexity of PBPK models has also increased. Academic efforts have provided clear advances in better capturing human physiology in PBPK models and incorporating more complex mathematical concepts into PBPK models. Examples of such advances include the segregated gut model with a series of gut compartments allowing modeling of physiologic blood flow distribution within an organ and zonation of metabolic enzymes and series compartment liver models allowing simulations of hepatic clearance for high extraction drugs. Despite these advances in academic research, the progress in assessing model quality and defining model acceptance criteria based on the intended use of the models has not kept pace. This Minireview suggests that awareness of the need for predefined criteria for model acceptance has increased, but many manuscripts still lack description of scientific justification and/or rationale for chosen acceptance criteria. As artificial intelligence and machine learning approaches become more broadly accepted, these tools offer promise for development of comprehensive assessment for existing observed data and analysis of model performance. SIGNIFICANCE STATEMENT: Physiologically based pharmacokinetic (PBPK) modeling has become a mainstream application in academic literature and is broadly used for predictions, analysis, and evaluation of pharmacokinetic data. Significant progress has been made in developing advanced PBPK models that better capture human physiology, but oftentimes sufficient justification for the chosen model acceptance criterion and model structure is still missing. This Minireview provides a summary of the current landscape of PBPK applications used and highlights the need for advancing PBPK modeling science and training in academia.
小分子的基于生理的药代动力学(PBPK)模型已成为药物研发和学术研究的主流。PBPK模型的应用正在不断扩展,目前大部分工作集中在药物-药物相互作用、药物-疾病相互作用以及药物在整个生命周期内处置变化的预测上。最近,使用PBPK建模来预测孕期和器官损伤时药物处置的出版物有所增加,这反映了将各种生理变化纳入模型方面的进展。由于可用的计算能力不断增强以及建模平台的多样性,PBPK模型的复杂性也有所增加。学术研究在更好地在PBPK模型中捕捉人体生理学以及将更复杂的数学概念纳入PBPK模型方面取得了明显进展。这些进展的例子包括具有一系列肠道隔室的分离肠道模型,该模型允许对器官内的生理血流分布以及代谢酶的分区进行建模,还有串联隔室肝脏模型,该模型允许对高摄取药物的肝清除进行模拟。尽管学术研究取得了这些进展,但在根据模型的预期用途评估模型质量和定义模型接受标准方面的进展却未能跟上。这篇小型综述表明,对模型接受的预定义标准的需求意识有所提高,但许多手稿仍缺乏对所选接受标准的科学依据和/或基本原理的描述。随着人工智能和机器学习方法得到更广泛的接受,这些工具为对现有观测数据进行全面评估以及分析模型性能提供了希望。意义声明:基于生理的药代动力学(PBPK)建模已成为学术文献中的主流应用,并广泛用于药代动力学数据的预测、分析和评估。在开发能更好地捕捉人体生理学的先进PBPK模型方面已取得重大进展,但通常仍缺少对所选模型接受标准和模型结构的充分理由。这篇小型综述总结了当前使用的PBPK应用的现状,并强调了在学术界推进PBPK建模科学和培训的必要性。
