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International Journal of Nanomedicine Volume 11, 2016 - Issue
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Original Research

Phytosome-hyaluronic acid systems for ocular delivery of L-carnosine

Hamdy Abdelkader1 Drug Discovery, Delivery and Patient Care (DDDPC) Theme, School of Life Sciences, Pharmacy and Chemistry, Kingston University London, Kingston Upon Thames, London, UK;2 Department of Pharmaceutics, Faculty of Pharmacy, Minia University, Mina, EgyptCorrespondence[email protected] [email protected]
,
Michael R Longman1 Drug Discovery, Delivery and Patient Care (DDDPC) Theme, School of Life Sciences, Pharmacy and Chemistry, Kingston University London, Kingston Upon Thames, London, UK
,
Raid G Alany1 Drug Discovery, Delivery and Patient Care (DDDPC) Theme, School of Life Sciences, Pharmacy and Chemistry, Kingston University London, Kingston Upon Thames, London, UK;3 School of Pharmacy, The University of Auckland, Auckland, New ZealandCorrespondence[email protected] [email protected]
&
Barbara Pierscionek4 Vision Cognition and Neuroscience Theme, Faculty of Science, Engineering and Computing, Kingston University London, Kingston Upon Thames, London, UK
Pages 2815-2827 | Published online: 14 Jun 2016
 
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Abstract

This study reports on L-carnosine phytosomes as an alternative for the prodrug N-acetyl-L-carnosine as a novel delivery system to the lens. L-carnosine was loaded into lipid-based phytosomes and hyaluronic acid (HA)-dispersed phytosomes. L-carnosine-phospholipid complexes (PC) of different molar ratios, 1:1 and 1:2, were prepared by the solvent evaporation method. These complexes were characterized with thermal and spectral analyses. PC were dispersed in either phosphate buffered saline pH 7.4 or HA (0.1% w/v) in phosphate buffered saline to form phytosomes PC1:1, PC1:2, and PC1:2 HA, respectively. These phytosomal formulations were studied for size, zeta potential, morphology, contact angle, spreading coefficient, viscosity, ex vivo transcorneal permeation, and cytotoxicity using primary human corneal cells. L-carnosine-phospholipid formed a complex at a 1:2 molar ratio and phytosomes were in the size range of 380–450 nm, polydispersity index of 0.12–0.2. The viscosity of PC1:2 HA increased by 2.4 to 5-fold compared with HA solution and PC 1:2, respectively; significantly lower surface tension, contact angle, and greater spreading ability for phytosomes were also recorded. Ex vivo transcorneal permeation parameters showed significantly controlled corneal permeation of L-carnosine with the novel carrier systems without any significant impact on primary human corneal cell viability. Ex vivo porcine lenses incubated in high sugar media without and with L-carnosine showed concentration-dependent marked inhibition of lens brunescence indicative of the potential for delaying changes that underlie cataractogenesis that may be linked to diabetic processes.

Acknowledgments

This work is partially funded by The Cultural Affairs and Missions Sector, Ministry of Higher Education, Cairo, Egypt, in the form of a postdoctoral grant for Dr Abdelkader. The authors acknowledge funding from the Leverhulme Trust and thank Lipoid GmbH, Ludwigshafen, Germany, for the gift of Lipoid S 75.

Disclosure

The authors report no conflicts of interest in this work.

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