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  5. Bioavailable copper modulates oxidative phosphorylation and growth of tumors

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Article
en
2013

Bioavailable copper modulates oxidative phosphorylation and growth of tumors

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en
2013
Vol 110 (48)
Vol. 110
DOI: 10.1073/pnas.1318431110

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Douglas Hanahan
Douglas Hanahan

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Seiko Ishida
Pénélope A. Andreux
Carole Poitry‐Yamate
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Abstract

Copper is an essential trace element, the imbalances of which are associated with various pathological conditions, including cancer, albeit via largely undefined molecular and cellular mechanisms. Here we provide evidence that levels of bioavailable copper modulate tumor growth. Chronic exposure to elevated levels of copper in drinking water, corresponding to the maximum allowed in public water supplies, stimulated proliferation of cancer cells and de novo pancreatic tumor growth in mice. Conversely, reducing systemic copper levels with a chelating drug, clinically used to treat copper disorders, impaired both. Under such copper limitation, tumors displayed decreased activity of the copper-binding mitochondrial enzyme cytochrome c oxidase and reduced ATP levels, despite enhanced glycolysis, which was not accompanied by increased invasiveness of tumors. The antiproliferative effect of copper chelation was enhanced when combined with inhibitors of glycolysis. Interestingly, larger tumors contained less copper than smaller tumors and exhibited comparatively lower activity of cytochrome c oxidase and increased glucose uptake. These results establish copper as a tumor promoter and reveal that varying levels of copper serves to regulate oxidative phosphorylation in rapidly proliferating cancer cells inside solid tumors. Thus, activation of glycolysis in tumors may in part reflect insufficient copper bioavailability in the tumor microenvironment.

How to cite this publication

Seiko Ishida, Pénélope A. Andreux, Carole Poitry‐Yamate, Johan Auwerx, Douglas Hanahan (2013). Bioavailable copper modulates oxidative phosphorylation and growth of tumors. , 110(48), DOI: https://doi.org/10.1073/pnas.1318431110.

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Publication Details

Type

Article

Year

2013

Authors

5

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1073/pnas.1318431110

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