Pharmacokinetic evaluation of poorly soluble compounds formulated as nano- or microcrystals after intraperitoneal injection to mice

生物利用度 药理学 药代动力学 化学 背景(考古学) 体内 药物输送 吸收(声学) 药品 溶解度 粒径 口服 溶解 医学 材料科学 有机化学 复合材料 古生物学 生物技术 物理化学 生物
作者
Krishna Aluri,Kalle Sigfridsson,Aixiang Xue,Niresh Hariparsad,Dermot F. McGinnity,Diane Ramsden
出处
期刊:International Journal of Pharmaceutics [Elsevier]
卷期号:636: 122787-122787 被引量:2
标识
DOI:10.1016/j.ijpharm.2023.122787
摘要

Intraperitonial (i.p.) delivery during initial stages of drug discovery can allow efficacy readouts for compounds which have suboptimal pharmacokinetics (PK) due to poor physiochemical properties and/or oral bioavailability. A major limitation for widespread use of i.p. administration is the paucity of published data and unclear mechanisms of absorption, particularly when using complex formulations. The aim of the present study was to investigate the PK of poorly soluble compounds with low oral bioavailability when administered i.p. as crystalline nano- and microsuspensions. Three compounds, with varying aqueous solubility (2, 7, and 38 µM, at 37 °C), were dosed to mice at 10 and 50 mg/kg. In vitro dissolution confirmed that nanocrystals dissolved faster than microcrystals and hence were expected to result in higher exposure after i.p. dosing. Surprisingly, the increase in dissolution rate with decrease in particle size did not result in higher in vivo exposure. In contrast, the microcrystals showed higher exposure. The potential of smaller particles to promote access to the lymphatic system is hypothesized and discussed as one plausible explanation. The present work demonstrates the importance of understanding physicochemical properties of drug formulations in the context of the microphysiology at the delivery site and how that knowledge can be leveraged to alter systemic PK.
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