Mechanistic insights into effect of surfactants on oral bioavailability of amorphous solid dispersions

生物利用度 溶解 肺表面活性物质 赋形剂 化学 化学工程 药物输送 挤压 小泡 吸收(声学) 生物制药 过饱和度 剂型 材料科学 色谱法 有机化学 药理学 体外 生物化学 生物活性 工程类 复合材料 生药学 冶金 医学
作者
Andreas Schittny,S. Philipp-Bauer,Pascal Detampel,Jörg Huwyler,Maxim Puchkov
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:320: 214-225 被引量:50
标识
DOI:10.1016/j.jconrel.2020.01.031
摘要

Drug delivery of poorly soluble drugs in form amorphous solid dispersions (ASDs) is an appealing method to increase in vivo bioavailability. For rational formulation design, a mechanistic understanding of the impact of surfactants on the performance of ASD-based formulations is therefore of importance. In this study, we used hot-melt extrusion to prepare ASDs composed of the model drug substance efavirenz with hydroxypropyl methylcellulose phthalate (HPMCP) as the base polymer, and surfactants. Molecular dynamics simulations and in vitro dissolution studies were used to investigate formation and drug release from polymer vesicles, and their ability to maintain a supersaturation state as a function of surfactant composition. It was possible to identify main factors regulating particle formation and to modify dissolution profiles with different excipient compositions. Animal studies in the rat, in combination with physiologically based pharmacokinetic modeling, demonstrated enhanced drug absorption from formed vesicles. The surfactant composition in the ASD had a direct influence on the morphology of these vesicles, as well as kinetics of drug release, and, therefore, the oral bioavailability. ASDs, prepared by hot-melt extrusion method, were optimized for dissolution and adsorption rates increase. Our findings contribute to a better understanding of dissolution behavior of ASDs with respect to the function of surfactants, aiming to facilitate a rational formulation development and an accelerated transition from in vitro systems to in vivo applications.
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