Differential susceptibility of primary cultured human skin cells to hypericin PDT in an in vitro model

Differential susceptibility of primary cultured human skin cells to hypericin PDT in an in vitro model

•Hypericin (HYP)-PDT is an effective treatment option for skin cancer.•This paper aims at the effect of HYP-PDT on the 3 skin cell types around a tumor.•Significant differences exist in cell viability and morphology between the cells.•Higher ROS levels in fibroblasts than both melanocytes and kerati...

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Veröffentlicht in:Journal of photochemistry and photobiology. B, Biology Biology, 2015-08, Vol.149, p.249-256
Hauptverfasser: Popovic, A., Wiggins, T., Davids, L.M.
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Apoptosis
Apoptosis - drug effects
Apoptosis - radiation effects
Cell Survival - drug effects
Cell Survival - radiation effects
Human skin cells
Humans
Hypericin
Infant, Newborn
Intracellular Space - drug effects
Intracellular Space - metabolism
Intracellular Space - radiation effects
Perylene - analogs & derivatives
Perylene - pharmacology
Photochemotherapy
Photodynamic therapy
Photosensitizing Agents - pharmacology
Reactive Oxygen Species - metabolism
ROS
Skin - cytology
Skin - drug effects
Skin - radiation effects
Tumor Microenvironment - drug effects
Tumor Microenvironment - radiation effects
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Zusammenfassung:•Hypericin (HYP)-PDT is an effective treatment option for skin cancer.•This paper aims at the effect of HYP-PDT on the 3 skin cell types around a tumor.•Significant differences exist in cell viability and morphology between the cells.•Higher ROS levels in fibroblasts than both melanocytes and keratinocytes.•A differential response exists to HYP-PDT for each skin cell type. Skin cancer is the most common cancer worldwide, and its incidence rate in South Africa is increasing. Photodynamic therapy (PDT) has been shown to be an effective treatment modality, through topical administration, for treatment of non-melanoma skin cancers. Our group investigates hypericin-induced PDT (HYP-PDT) for the treatment of both non-melanoma and melanoma skin cancers. However, a prerequisite for effective cancer treatments is efficient and selective targeting of the tumoral cells with minimal collateral damage to the surrounding normal cells, as it is well established that cancer therapies have bystander effects on normal cells in the body, often causing undesirable side effects. The aim of this study was to investigate the cellular and molecular effects of HYP-PDT on normal primary human keratinocytes (Kc), melanocytes (Mc) and fibroblasts (Fb) in an in vitro tissue culture model which represented both the epidermal and dermal cellular compartments of human skin. Cell viability analysis revealed a differential cytotoxic response to a range of HYP-PDT doses in all the human skin cell types, showing that Fb (LD50=1.75μM) were the most susceptible to HYP-PDT, followed by Mc (LD50=3.5μM) and Kc (LD50>4μM HYP-PDT) These results correlated with the morphological analysis which displayed distinct morphological changes in Fb and Mc, 24h post treatment with non-lethal (1μM) and lethal (3μM) doses of HYP-PDT, but the highest HYP-PDT doses had no effect on Kc morphology. Fluorescent microscopy displayed cytoplasmic localization of HYP in all the 3 skin cell types and additionally, HYP was excluded from the nuclei in all the cell types. Intracellular ROS levels measured in Fb at 3μM HYP-PDT, displayed a significant 3.8 fold (p
ISSN:1011-1344
1873-2682
DOI:10.1016/j.jphotobiol.2015.06.009