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Photodynamic therapy using topically applied hypericin: comparative effect with methyl-aminolevulinic acid on UV induced skin tumours. | LitMetric

Photodynamic therapy using topically applied hypericin: comparative effect with methyl-aminolevulinic acid on UV induced skin tumours.

J Photochem Photobiol B

Faculty of Pharmaceutical Sciences, KU Leuven, Leuven, Belgium.

Published: February 2011

AI Article Synopsis

  • Photodynamic therapy (PDT) is effective for treating superficial skin lesions, and this study compared the effects of topical hypericin and methyl-aminolevulinic acid (Me-ALA) on actinic keratosis using a mouse model.
  • Despite both treatments leading to some tumor necrosis and replacement by normal cells, hypericin-PDT showed significantly lower efficiency (44% clearance) compared to Me-ALA-PDT (80% clearance).
  • Microscopic analysis revealed that hypericin had poor skin penetration and limited tumor selectivity, accumulating mostly in the outer skin layer, while Me-ALA had a more uniform distribution in the lesions.

Article Abstract

Photodynamic therapy (PDT) is a treatment option particularly well-suited for superficial (pre)malignant skin lesions due to the skin's accessibility to light. In the present study, the efficacy of topical hypericin-PDT was evaluated using a mouse model for actinic keratosis. For comparison, similar experiments were conducted with methyl-aminolevulinic acid (Me-ALA). Small skin tumours (1-2 mm) were induced in hairless mice by chronic UV irradiation. After topical application of hypericin (0.1% in gelcream for 24 h) or Me-ALA (Metvix® for 4 h), the lesional/non-lesional skin surface fluorescence ratio was determined and fluorescence microscopy was used to study the skin penetration of the photosensitizers. The antitumour activity of topical PDT (20 mW cm(-2), 40 J cm(-2)) was evaluated by measurement of the lesional diameters. Moreover, biopsies were taken at various time points after PDT for histological evaluation of the therapy. Our results demonstrate that after topical application of hypericin and Me-ALA, tumour selectivity is limited in mouse skin. The microscopic distribution of hypericin fluorescence showed an accumulation in the stratum corneum and low fluorescence levels in the rest of the lesions, whereas the distribution of PpIX in the skin was more homogenous. Topical hypericin-PDT was found to be less efficient (44% total lesional clearance) as compared to Me-ALA-PDT (80% total lesional clearance). Full lesional necrosis was observed in responsive lesions, and the atypical cells of actinic keratosis were replaced by normal keratinocytes 3 weeks later, both after hypericin-PDT and Me-ALA-PDT.

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Source
http://dx.doi.org/10.1016/j.jphotobiol.2010.09.012DOI Listing

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