Consistent Intraocular Pressure Reduction by Solid Drug Nanoparticles in Fixed Combinations for Glaucoma Therapy

Author:

Huang Da12,Norat Pedro3,Qi Lin2,Chernatynskaya Anna2,Cole James D.3,Mani Vimalin Jeyalatha2,Xu Lei2,Liu Xiaorong345ORCID,Yang Hu2ORCID

Affiliation:

1. College of Biological Science and Engineering Fuzhou University Fuzhou Fujian 350108 China

2. Linda and Bipin Doshi Department of Chemical and Biochemical Engineering Missouri University of Science and Technology Rolla MO 65409 USA

3. Department of Biology University of Virginia Charlottesville VA 22904 USA

4. Department of Psychology University of Virginia Charlottesville VA 22904 USA

5. Program in Fundamental Neuroscience University of Virginia Charlottesville VA 22904 USA

Abstract

AbstractEfficient topical drug delivery remains a significant challenge in glaucoma management. Although nanoparticle formulations offer considerable promise, their complex preparation processes, co‐delivery issues, and batch consistency have hindered their potential. A scalable fabrication strategy is developed here for preparing solid drug nanoparticles (SDNs) with enhanced drug delivery efficiency. Utilizing hydrophobic antiglaucoma drugs brimonidine (BM) and betaxolol (BX), uniform fixed combination BM/BX SDNs are fabricated through a continuous process, improving batch‐to‐batch consistency for combined glaucoma treatment. With trehalose being used as a lyoprotectant, BM/BX SDNs can be stored as dry powder and easily reconstituted in phosphate buffered saline. Importantly, reconstituted BM/BX SDNs form clear, homogenous solutions, and exhibit negligible cytotoxicity and irritation, making them well‐suited for topical administration as eyedrops. Ex vivo and in vivo studies demonstrated that topically applied BM/BX SDNs permeate through the cornea significantly (about two fold to three fold) compared to their hydrophilic counterparts, i.e., brimonidine tartrate, and betaxolol hydrogen chloride. Notably, BM/BX SDNs displayed consistent intraocular pressure lowering effects in vivo in both normotensive rats and glaucoma mice. Collectively, this study demonstrates the potential of the scalable fabrication strategy and the resultant BM/BX SDNs for improving glaucoma management through eyedrops.

Funder

National Institutes of Health

Publisher

Wiley

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