Chitosan-coated liposomes to stabilize and enhance transdermal delivery of indocyanine green for photodynamic therapy of melanoma

•Indocyanine green is a photosensitizer approved for clinical use.•Anionic indocyanine green is unstable and hardly permeates through skin.•Topical photodynamic therapy is noninvasive strategy for melanoma treatment.•Chitosan-coating of liposomes can protect indocyanine green from degradation.•Chito...

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Bibliographic Details
Published in:Carbohydrate polymers 2019-11, Vol.224, p.115143-115143, Article 115143
Main Authors: Lee, Eun-Hye, Lim, Soo-Jeong, Lee, Mi-Kyung
Format: Article
Language:English
Subjects:
Administration, Cutaneous
Animals
Biological Transport
Chitosan
Chitosan - chemistry
Indocyanine green
Indocyanine Green - administration & dosage
Indocyanine Green - chemistry
Indocyanine Green - metabolism
Indocyanine Green - pharmacology
Liposomes
Liposomes - chemistry
Male
Melanoma
Melanoma, Experimental - drug therapy
Melanoma, Experimental - metabolism
Melanoma, Experimental - pathology
Mice
Permeability
Photochemotherapy
Skin - metabolism
Topical PDT
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Summary:•Indocyanine green is a photosensitizer approved for clinical use.•Anionic indocyanine green is unstable and hardly permeates through skin.•Topical photodynamic therapy is noninvasive strategy for melanoma treatment.•Chitosan-coating of liposomes can protect indocyanine green from degradation.•Chitosan-coated liposomes enhances skin permeation of indocyanine green. Indocyanine green (ICG) has been used clinically and noticed as a promising candidate for the topical melanoma photodynamic therapy (PDT). Despite its high potentials in topical PDT, the use of ICG has been hampered by the instability in aqueous solution. In the present study, chitosan-coated liposomes were adopted as a formulation strategy which could stabilize and enhance skin permeation of ICG. Chitosan-coating was verified by the significantly increased liposomal size and reversed zeta potential from negative to positive value by positive chitosan coating. Chitosan-coating liposomes protected ICG from degradation while uncoated liposomes did not. Moreover, they significantly increased cellular uptake and photocytotoxicity of ICG in B16-F10 melanoma cells in a chitosan-dependent manner. The skin permeation of ICG was also drastically improved by chitosan-coated liposomes. These findings emphasize the promising potential of ICG-loaded chitosan-coated liposomes for topical PDT of melanoma.
ISSN:0144-8617
1879-1344
DOI:10.1016/j.carbpol.2019.115143