Uptake and phototoxicity of meso-tetrahydroxyphenyl chlorine are highly variable in human biliary tract cancer cell lines and correlate with markers of differentiation and proliferation
Photodynamic therapy (PDT) using Photofrin® and, recently, Foscan® has gained broad acceptance for palliative treatment of non-resectable cholangiocarcinoma (CC). No information, however, is available whether the phenotype of CC tumour cells has an effect on the efficiency of the treatment. Using a...
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Veröffentlicht in: | Photochemical & photobiological sciences 2010-05, Vol.9 (5), p.734-743 |
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Sprache: | eng |
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Zusammenfassung: | Photodynamic therapy (PDT) using Photofrin® and, recently, Foscan® has gained broad acceptance for palliative treatment of non-resectable cholangiocarcinoma (CC). No information, however, is available whether the phenotype of CC tumour cells has an effect on the efficiency of the treatment. Using a well-characterised set of
n
= 9 biliary tract cancer cell lines this study investigated the uptake, phototoxicity, and release of
meso
-tetrahydroxyphenyl chlorine (mTHPC, Foscan®) after incubation with 200 or 400 ng ml
−1
mTHPC. For uptake of mTHPC we found great variations between the individual cell lines (up to a factor 2), resulting in even more pronounced differences in phototoxicity. Based on statistical classification by hierarchical cluster analysis, two groups of cell lines can be distinguished which are characterised by either high or low susceptibility towards mTHPC-based photodynamic treatment. Correlation analysis with previously established immunochemical parameters showed that cells with a low cytokeratin-19 (ductal differentiation), high vimentin (mesenchymal marker), and high proliferative phenotype preferentially show higher uptake of mTHPC and subsequent phototoxicity. These results demonstrate high variability of biliary tract cancer cells when subjected to mTHPC-based photodynamic treatment and identify possible markers that could be used in the clinical setting in order to predict the efficiency of PDT and adjust the dose for complete tumour elimination. |
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ISSN: | 1474-905X 1474-9092 |
DOI: | 10.1039/b9pp00201d |