Note on importance of correct stoichiometric assumptions for modeling of monoclonal antibodies.

IF 2.2 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Leonid Gibiansky, Ekaterina Gibiansky
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Abstract

Pharmacokinetic modeling of monoclonal antibodies (mAbs) with non-linear binding is based on equations of the target-mediated drug disposition (Mager and Jusko, J Pharmacokinet Pharmacodyn 28:507-532, 2001). These equations demonstrated their utility in countless examples and drug development programs. The model assumes that the mAb drug and the target have only one binding site each while, in reality, most antibodies have two binding sites. Thus, the currently used model does not correspond to the biological process that it aims to describe. The correct mechanistic model should take into account both binding sites. We investigated, using simulations, whether this discrepancy is important and when it is advisable to use a model with correct stoichiometric 2-to-1 ratio. We show that for soluble targets when elimination rate of the drug-target complex is comparable with the elimination rate of the drug or lower, and when measurements of both total drug and total target concentrations are available, the model with 1-to-1 (monovalent) binding cannot describe data simulated from the model with 2-to-1 (bivalent) binding. In these cases, models with correct stoichiometric assumptions may be necessary for an adequate description of the observed data. Also, a model with allosteric binding that encompasses both 2-to-1 and 1-to-1 binding models as particular cases was proposed and applied. It was shown to be identifiable given the detailed concentration data of total drug and total target.

Abstract Image

关于单克隆抗体建模中正确计量假设重要性的说明。
具有非线性结合的单克隆抗体(mAbs)的药代动力学建模是基于靶向介导的药物处置方程(Mager 和 Jusko,J Pharmacokinet Pharmacodyn 28:507-532,2001 年)。这些方程在无数的实例和药物开发项目中证明了它们的实用性。该模型假设 mAb 药物和靶点各有一个结合位点,而实际上大多数抗体都有两个结合位点。因此,目前使用的模型并不符合它所要描述的生物过程。正确的机理模型应该考虑到两个结合位点。我们通过模拟研究了这种差异是否重要,以及何时应该使用具有正确的 2 比 1 比例的模型。我们的研究表明,对于可溶性靶点,当药物-靶点复合物的消除率与药物的消除率相当或更低时,当药物总浓度和靶点总浓度均可测量时,1-1(单价)结合模型无法描述 2-1(二价)结合模型模拟的数据。在这种情况下,为了充分描述观察到的数据,可能需要建立具有正确化学计量假设的模型。此外,我们还提出并应用了一种异生结合模型,该模型包括 2 对 1 和 1 对 1 两种特殊情况的结合模型。根据药物总量和目标物总量的详细浓度数据,该模型是可识别的。
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来源期刊
CiteScore
4.90
自引率
4.00%
发文量
39
审稿时长
6-12 weeks
期刊介绍: Broadly speaking, the Journal of Pharmacokinetics and Pharmacodynamics covers the area of pharmacometrics. The journal is devoted to illustrating the importance of pharmacokinetics, pharmacodynamics, and pharmacometrics in drug development, clinical care, and the understanding of drug action. The journal publishes on a variety of topics related to pharmacometrics, including, but not limited to, clinical, experimental, and theoretical papers examining the kinetics of drug disposition and effects of drug action in humans, animals, in vitro, or in silico; modeling and simulation methodology, including optimal design; precision medicine; systems pharmacology; and mathematical pharmacology (including computational biology, bioengineering, and biophysics related to pharmacology, pharmacokinetics, orpharmacodynamics). Clinical papers that include population pharmacokinetic-pharmacodynamic relationships are welcome. The journal actively invites and promotes up-and-coming areas of pharmacometric research, such as real-world evidence, quality of life analyses, and artificial intelligence. The Journal of Pharmacokinetics and Pharmacodynamics is an official journal of the International Society of Pharmacometrics.
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