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Merck

Oral delivery of sorafenib through spontaneous formation of ionic liquid nanocomplexes.

Journal of controlled release : official journal of the Controlled Release Society (2020-03-24)
Yujie Shi, Zongmin Zhao, Yongsheng Gao, Daniel C Pan, Alyssa K Salinas, Eden E L Tanner, Junling Guo, Samir Mitragotri
RESUMEN

Delivery of hydrophobic drugs is a significant challenge due to poor solubility and formulation difficulty. Here, we describe the potential of ionic liquids, in particular choline and geranic acid (CAGE), for oral delivery of a hydrophobic drug, sorafenib (SRF). CAGE provided excellent apparent solubility of SRF tosylate (> 500 mg/mL). Upon oral dosing in rats, CAGE increased peak blood concentrations of SRF by 2.2-fold. The elimination half-life of SRF was also increased by 2-fold and the mean absorption time was extended by 1.6-fold. Furthermore, SRF delivered by CAGE exhibited significantly different biodistribution compared to control formulations. Specifically, accumulation in lungs and kidneys improved 4.4-fold and 6.2-fold, respectively compared to control formulations. Mechanistic studies revealed that SRF-CAGE solution spontaneously formed a self-assembled structure (427 ± 41 nm), which is likely responsible for altered biodistribution in vivo. UPLC-MS studies confirmed the presence of choline-geranate species in blood indicative of micellar/emulsion structures which eventually dissociated into choline and geranic acid molecular species. These studies provide a simple, scalable strategy for oral delivery of hydrophobic drugs.

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Sigma-Aldrich
Choline bicarbonate, ~80% in H2O
Sigma-Aldrich
Geranic acid, technical grade, 85%