Comparing the efficacy of photodynamic and sonodynamic therapy in non-melanoma and melanoma skin cancer |
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Affiliation: | 1. Biomedical Sciences Research Institute, University of Ulster, Coleraine BT52 1SA, Northern Ireland, UK;2. Oxford Institute of Biomedical Engineering, University of Oxford, Oxford, OX3 7DQ, UK;3. Department of Mechanical Engineering, University of Colorado, 1111 Engineering Drive, Boulder, CO 80309, USA;4. Division of Surgery & Interventional Science, Medical School, University College London, London W1W 7EJ, UK |
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Abstract: | Sonodynamic therapy (SDT) involves the activation of a non-toxic sensitiser drug using low-intensity ultrasound to produce cytotoxic reactive oxygen species (ROS). Given the low tissue attenuation of ultrasound, SDT provides a significant benefit over the more established photodynamic therapy (PDT) as it enables activation of sensitisers at a greater depth within human tissue. In this manuscript, we compare the efficacy of aminolevulinic acid (ALA) mediated PDT and SDT in a squamous cell carcinoma (A431) cell line as well as the ability of these treatments to reduce the size of A431 ectopic tumours in mice. Similarly, the relative cytotoxic ability of Rose Bengal mediated PDT and SDT was investigated in a B16-melanoma cell line and also in a B16 ectopic tumour model. The results reveal no statistically significant difference in efficacy between ALA mediated PDT or SDT in the non-melanoma model while Rose Bengal mediated SDT was significantly more efficacious than PDT in the melanoma model. This difference in efficacy was, at least in part, attributed to the dark pigmentation of the melanoma cells that effectively filtered the excitation light preventing it from activating the sensitiser while the use of ultrasound circumvented this problem. These results suggest SDT may provide a better outcome than PDT when treating highly pigmented cancerous skin lesions. |
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Keywords: | PDT SDT Melanoma Squamous cell carcinoma Ultrasound Light Melanin |
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