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肺部沉积和体外通透性对预测吸入用布地奈德制剂的血浆水平的影响。

Effect of the pulmonary deposition and in vitro permeability on the prediction of plasma levels of inhaled budesonide formulation.

机构信息

Research Center Pharmaceutical Engineering, Graz, Austria.

Center for Medical Research, Medical University of Graz, Graz, Austria.

出版信息

Int J Pharm. 2017 Oct 30;532(1):337-344. doi: 10.1016/j.ijpharm.2017.08.124. Epub 2017 Sep 7.

Abstract

The growing interest in the inhalable pharmaceutical products requires advanced approaches to safe and fast product development, such as in silico tools that can be used for estimating the bioavailability and toxicity of developed formulation. GastroPlus™ is one of the few available software packages for in silico simulation of PBPK profile of inhalable products. It contains a complementary module for calculating the lung deposition, the permeability and the systemic absorption of inhalable products. Experimental values of lung deposition and permeability can also be used. This study aims to assess the efficiency of simulation by applying experimental permeability and deposition values, using budesonide as a model substance. The lung deposition values were obtained from the literature, the lung permeability data were experimentally determined by culturing Calu-3 cells under air-liquid interface and submersed conditions to morphologically resemble bronchial and alveolar epithelial cells, respectively. A two-compartment PK model was created for i.v. administration and used as a background for the in silico simulation of the plasma profile of budesonide after inhalation. The predicted plasma profile was compared with the in vivo data from the literature and the effects of experimental lung deposition and permeability on prediction were assessed. The developed model was significantly improved by using realistic lung deposition data combined with experimental data for peripheral permeability.

摘要

对可吸入药物产品日益增长的兴趣,需要先进的方法来安全、快速地进行产品开发,例如可用于估算开发制剂生物利用度和毒性的计算工具。GastroPlus™ 是少数可用于模拟可吸入产品 PBPK 特征的软件包之一。它包含一个用于计算可吸入产品肺部沉积、渗透性和全身吸收的补充模块。也可以使用实验获得的肺部沉积和渗透性值。本研究旨在通过应用实验获得的渗透性和沉积值来评估模拟的效率,以布地奈德作为模型物质。肺部沉积值从文献中获得,肺部渗透性数据通过在气液界面和浸没条件下培养 Calu-3 细胞获得,分别模拟支气管和肺泡上皮细胞。为静脉注射给药创建了一个两室 PK 模型,并用作模拟吸入后布地奈德血浆特征的计算基础。预测的血浆特征与文献中的体内数据进行了比较,并评估了实验性肺部沉积和渗透性对预测的影响。通过使用现实的肺部沉积数据和外周渗透性的实验数据相结合,所开发的模型得到了显著改进。

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