1. A potent nonporphyrin class of photodynamic therapeutic agent: cellular localisation, cytotoxic potential and influence of hypoxia
- Author
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Tony J. Kenna, John Killoran, Lorcan T. Allen, William M. Gallagher, Michael J. Hall, Donal F. O'Shea, Aoife Gorman, and Caroline O'Shea
- Subjects
Azadipyrromethene ,Cytoplasm ,Cancer Research ,Programmed cell death ,Pathology ,medicine.medical_specialty ,Porphyrins ,Light ,medicine.medical_treatment ,Apoptosis ,Photodynamic therapy ,cytotoxic potential ,Biology ,Endoplasmic Reticulum ,Flow cytometry ,chemistry.chemical_compound ,Cell Line, Tumor ,medicine ,Humans ,Pyrroles ,Viability assay ,Cytotoxicity ,photodynamic therapeutic agent ,Photosensitizing Agents ,Dose-Response Relationship, Drug ,cellular localisation ,medicine.diagnostic_test ,Endoplasmic reticulum ,Cell Hypoxia ,Photochemotherapy ,Oncology ,chemistry ,Cancer research ,Translational Therapeutics - Abstract
We have developed a totally new class of nonporphyrin photodynamic therapeutic agents with a specific focus on two lead candidates azadipyrromethene (ADPM)01 and ADPM06. Confocal laser scanning microscopy imaging showed that these compounds are exclusively localised to the cytosolic compartment, with specific accumulation in the endoplasmic reticulum and to a lesser extent in the mitochondria. Light-induced toxicity assays, carried out over a broad range of human tumour cell lines, displayed EC50 values in the micro-molar range for ADPM01 and nano-molar range for ADPM06, with no discernable activity bias for a specific cell type. Strikingly, the more active agent, ADPM06, even retained significant activity under hypoxic conditions. Both photosensitisers showed low to nondeterminable dark toxicity. Flow cytometric analysis revealed that ADPM01 and ADPM06 were highly effective at inducing apoptosis as a mode of cell death. The photophysical and biological characteristics of these PDT agents suggest that they have potential for the development of new anticancer therapeutics.
- Published
- 2005
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