Cadiou JL, et al. (2017)

Reference: Cadiou JL, et al. (2017) Copper transporters are responsible for copper isotopic fractionation in eukaryotic cells. Sci Rep 7:44533

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Abstract

Copper isotopic composition is altered in cancerous compared to healthy tissues. However, the rationale for this difference is yet unknown. As a model of Cu isotopic fractionation, we monitored Cu uptake in Saccharomyces cerevisiae, whose Cu import is similar to human. Wild type cells are enriched in ⁶³Cu relative to ⁶⁵Cu. Likewise, ⁶³Cu isotope enrichment in cells without high-affinity Cu transporters is of slightly lower magnitude. In cells with compromised Cu reductase activity, however, no isotope fractionation is observed and when Cu is provided solely in reduced form for this strain, copper is enriched in ⁶³Cu like in the case of the wild type. Our results demonstrate that Cu isotope fractionation is generated by membrane importers and that its amplitude is modulated by Cu reduction. Based on ab initio calculations, we propose that the fractionation may be due to Cu binding with sulfur-rich amino acids: methionine and cysteine. In hepatocellular carcinoma (HCC), lower expression of the STEAP3 copper reductase and heavy Cu isotope enrichment have been reported for the tumor mass, relative to the surrounding tissue. Our study suggests that copper isotope fractionation observed in HCC could be due to lower reductase activity in the tumor.

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Reference Type: Journal Article | Research Support, Non-U.S. Gov't
Authors: Cadiou JL, Pichat S, Bondanese VP, Soulard A, Fujii T, Albarède F, Oger P
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