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A novel flunarizine hydrochloride-loaded organogel for intraocular drug delivery in situ: Design, physicochemical characteristics and inspection. | LitMetric

A novel flunarizine hydrochloride-loaded organogel for intraocular drug delivery in situ: Design, physicochemical characteristics and inspection.

Int J Pharm

Department of Pharmaceutics, College of Pharmacy, Anhui University of Chinese Medicine, Hefei 230012, People's Republic of China; Institute of Pharmaceutics, Anhui Academy of Chinese Medical Sciences, Hefei 230012, People's Republic of China; Engineering Technology Research Center of Modernized Pharmaceutics, Anhui Province, Hefei 230012, People's Republic of China; Anhui Province Key Laboratory of Chinese Medicinal Formula, Hefei 230012, People's Republic of China. Electronic address:

Published: February 2020

We developed a safe and efficacious drug delivery system for treatment of brain diseases. A novel in-situ gel system was prepared using soybean oil, stearic acid and N-methyl-2-pyrrolidinone (NMP) (10:1:3, v/w/v). This system had low viscosity as a sol in vitro and turned into a solid or semi-solid gel in situ after administration. The poorly water-soluble drug flunarizine hydrochloride (FNZ) was incorporated into this "organogel" system. Organogel-FNZ was characterized by light microscopy, differential scanning calorimetry (DSC) and rheology. Drug release in vitro was investigated. The initial "burst" effect did not occur in organogel-FNZ, which is different from other gels formed in situ. Pharmacokinetic studies were undertaken in rats using gel administration (14 mg kg), intravenous administration (5 mg kg) and administration using drops (14 mg kg). Organogel-FNZ could reduce the clearance rate and prolong the duration of action, in the plasma and brain tissues of rats. The peak serum concentration, area under the curve and absolute bioavailability of the organogel-FNZ group were higher than those of the intraocular- drops group. Organogel-FNZ is a promising drug-delivery system for treatment of brain diseases by intraocular administration.

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Source
http://dx.doi.org/10.1016/j.ijpharm.2020.119027DOI Listing

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