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Development of a Multicompartment Permeability-Limited Lung PBPK Model and Its Application in Predicting Pulmonary Pharmacokinetics of Antituberculosis Drugs

机译:限制多室通透性的肺PBPK模型的建立及其在抗结核药物的肺药代动力学预测中的应用

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摘要

Achieving sufficient concentrations of antituberculosis (TB) drugs in pulmonary tissue at the optimum time is still a challenge in developing therapeutic regimens for TB. A physiologically based pharmacokinetic model incorporating a multicompartment permeability-limited lung model was developed and used to simulate plasma and pulmonary concentrations of seven drugs. Passive permeability of drugs within the lung was predicted using an in vitro-in vivo extrapolation approach. Simulated epithelial lining fluid (ELF):plasma concentration ratios showed reasonable agreement with observed clinical data for rifampicin, isoniazid, ethambutol, and erythromycin. For clarithromycin, itraconazole and pyrazinamide the observed ELF:plasma ratios were significantly underpredicted. Sensitivity analyses showed that changing ELF pH or introducing efflux transporter activity between lung tissue and ELF can alter the ELF:plasma concentration ratios. The described model has shown utility in predicting the lung pharmacokinetics of anti-TB drugs and provides a framework for predicting pulmonary concentrations of novel anti-TB drugs.
机译:在最佳时间在肺组织中获得足够浓度的抗结核(TB)药物仍然是制定TB治疗方案的挑战。建立了基于生理学的药代动力学模型,该模型结合了多室渗透性受限的肺部模型,并用于模拟七种药物的血浆和肺部浓度。使用体外-体内外推法可预测药物在肺内的被动渗透性。模拟的上皮衬里液(ELF):血浆浓度比与观察到的利福平,异烟肼,乙胺丁醇和红霉素的临床数据合理吻合。对于克拉霉素,伊曲康唑和吡嗪酰胺,观察到的ELF:血浆比率被大大低估了。敏感性分析表明,改变ELF pH值或在肺组织和ELF之间引入外排转运蛋白活性可以改变ELF:血浆浓度比。所描述的模型已显示出可用于预测抗结核药物的肺药代动力学,并提供了预测新型抗结核药物的肺部浓度的框架。

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