Physiologically Based Pharmacokinetic Model of Brain Delivery of Plasma Protein Bound Drugs

体内 药代动力学 化学 游离分数 血脑屏障 血液蛋白质类 白蛋白 药理学 丙咪嗪 口粘液 基于生理学的药代动力学模型 药品 普萘洛尔 血浆蛋白结合 体外 生物化学 医学 内分泌学 中枢神经系统 糖蛋白 生物 病理 生物技术 替代医学
作者
William M. Pardridge
出处
期刊:Pharmaceutical Research [Springer Nature]
卷期号:40 (3): 661-674 被引量:4
标识
DOI:10.1007/s11095-023-03484-2
摘要

A physiologically based pharmacokinetic (PBPK) model is developed that focuses on the kinetic parameters of drug association and dissociation with albumin, alpha-1 acid glycoprotein (AGP), and brain tissue proteins, as well as drug permeability at the blood-brain barrier, drug metabolism, and brain blood flow.The model evaluates the extent to which plasma protein-mediated uptake (PMU) of drugs by brain influences the concentration of free drug both within the brain capillary compartment in vivo and the brain compartment. The model also studies the effect of drug binding to brain tissue proteins on the concentration of free drug in brain.The steady state and non-steady state PBPK models are comprised of 11-12 variables, and 18-23 parameters, respectively. Two model drugs are analyzed: propranolol, which undergoes modest PMU from the AGP-bound pool, and imipramine, which undergoes a high degree of PMU from both the albumin-bound and AGP-bound pools in plasma.The free propranolol concentration in brain is under-estimated 2- to fourfold by in vitro measurements of free plasma propranolol, and the free imipramine concentration in brain is under-estimated by 18- to 31-fold by in vitro measurements of free imipramine in plasma. The free drug concentration in brain in vivo is independent of drug binding to brain tissue proteins.In vitro measurement of free drug concentration in plasma under-estimates the free drug in brain in vivo if PMU in vivo from either the albumin and/or the AGP pools in plasma takes place at the BBB surface.
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