The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells

Disagreement exists in the literature as to whether the successful antitumour agent cisplatin exhibits greater toxicity in hypoxia than in air. In this study, Chinese hamster ovary cells were incubated in clinically relevant concentrations of cisplatin for periods of up to three hours in aerobic and...

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Main Author: Matthews, Jeffrey Blair
Format: Others
Language:English
Published: 2009
Online Access:http://hdl.handle.net/2429/3371
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spelling ndltd-UBC-oai-circle.library.ubc.ca-2429-33712018-01-05T17:31:24Z The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells Matthews, Jeffrey Blair Disagreement exists in the literature as to whether the successful antitumour agent cisplatin exhibits greater toxicity in hypoxia than in air. In this study, Chinese hamster ovary cells were incubated in clinically relevant concentrations of cisplatin for periods of up to three hours in aerobic and hypoxic environments. For all incubation times studied, cells treated in hypoxia were more sensitive to cisplatin than those treated in air. Toxicity in hypoxic cells was up to two times greater than in aerobic cells. Detection of platinum using atomic absorption spectroscopy provided resolution fine enough to characterize whole cell uptake and DNA-binding of cisplatin at these concentrations. Cells treated in hypoxia showed consistently higher levels of platinum within the cells and bound to DNA than those treated in air. Furthermore, cells treated in hypoxia showed greater toxicity perplatinum-DNA adduct and per atom of platinum bound per cell than those treated in air. Two novel bis(platinum) compounds AN-38 and AN-36, of structural formula{[Pt(malonate)(NH₃)]₂H₂N(CH₂)ƞNH₂} (n=6 and 4, respectively), were also found to be preferentially toxic to hypoxic cells, up to four times as toxic as in air (for a four hour incubation), although there was little increase in platinum uptake levels. To date, this study represents the most thorough investigation of cisplatin properties in air versus hypoxia, given that survival, whole cell uptake and DNA binding in the same cell population each showed enhanced effects in hypoxia. Suggestions of possible mechanisms explaining these data could form the basis for future studies. Science, Faculty of Physics and Astronomy, Department of Graduate 2009-01-05T23:33:13Z 2009-01-05T23:33:13Z 1992 1992-05 Text Thesis/Dissertation http://hdl.handle.net/2429/3371 eng For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use. 3341303 bytes application/pdf
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description Disagreement exists in the literature as to whether the successful antitumour agent cisplatin exhibits greater toxicity in hypoxia than in air. In this study, Chinese hamster ovary cells were incubated in clinically relevant concentrations of cisplatin for periods of up to three hours in aerobic and hypoxic environments. For all incubation times studied, cells treated in hypoxia were more sensitive to cisplatin than those treated in air. Toxicity in hypoxic cells was up to two times greater than in aerobic cells. Detection of platinum using atomic absorption spectroscopy provided resolution fine enough to characterize whole cell uptake and DNA-binding of cisplatin at these concentrations. Cells treated in hypoxia showed consistently higher levels of platinum within the cells and bound to DNA than those treated in air. Furthermore, cells treated in hypoxia showed greater toxicity perplatinum-DNA adduct and per atom of platinum bound per cell than those treated in air. Two novel bis(platinum) compounds AN-38 and AN-36, of structural formula{[Pt(malonate)(NH₃)]₂H₂N(CH₂)ƞNH₂} (n=6 and 4, respectively), were also found to be preferentially toxic to hypoxic cells, up to four times as toxic as in air (for a four hour incubation), although there was little increase in platinum uptake levels. To date, this study represents the most thorough investigation of cisplatin properties in air versus hypoxia, given that survival, whole cell uptake and DNA binding in the same cell population each showed enhanced effects in hypoxia. Suggestions of possible mechanisms explaining these data could form the basis for future studies. === Science, Faculty of === Physics and Astronomy, Department of === Graduate
author Matthews, Jeffrey Blair
spellingShingle Matthews, Jeffrey Blair
The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
author_facet Matthews, Jeffrey Blair
author_sort Matthews, Jeffrey Blair
title The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
title_short The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
title_full The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
title_fullStr The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
title_full_unstemmed The effect of hypoxia on cytotoxicity, uptake and DNA binding of cisplatin and novel bis(platinum) complexes in Chinese hamster ovary cells
title_sort effect of hypoxia on cytotoxicity, uptake and dna binding of cisplatin and novel bis(platinum) complexes in chinese hamster ovary cells
publishDate 2009
url http://hdl.handle.net/2429/3371
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