Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells

Ceruloplasmin, the main copper binding protein in blood plasma, has been of particular interest for its role in efflux of iron from cells, but has additional functions. Here we tested the hypothesis that it releases its copper for cell uptake by interacting with a cell surface reductase and transpor...

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Autores principales: Ramos, Danny, Mar, David, Ishida, Michael, Vargas, Rebecca, Gaite, Michaella, Montgomery, Aaron, Linder, Maria C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4774968/
https://www.ncbi.nlm.nih.gov/pubmed/26934375
http://dx.doi.org/10.1371/journal.pone.0149516
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author Ramos, Danny
Mar, David
Ishida, Michael
Vargas, Rebecca
Gaite, Michaella
Montgomery, Aaron
Linder, Maria C.
author_facet Ramos, Danny
Mar, David
Ishida, Michael
Vargas, Rebecca
Gaite, Michaella
Montgomery, Aaron
Linder, Maria C.
author_sort Ramos, Danny
collection PubMed
description Ceruloplasmin, the main copper binding protein in blood plasma, has been of particular interest for its role in efflux of iron from cells, but has additional functions. Here we tested the hypothesis that it releases its copper for cell uptake by interacting with a cell surface reductase and transporters, producing apoceruloplasmin. Uptake and transepithelial transport of copper from ceruloplasmin was demonstrated with mammary epithelial cell monolayers (PMC42) with tight junctions grown in bicameral chambers, and purified human (64)Cu-labeled ceruloplasmin secreted by HepG2 cells. Monolayers took up virtually all the (64)Cu over 16h and secreted half into the apical (milk) fluid. This was partly inhibited by Ag(I). The (64)Cu in ceruloplasmin purified from plasma of (64)Cu-injected mice accumulated linearly in mouse embryonic fibroblasts (MEFs) over 3-6h. Rates were somewhat higher in Ctr1+/+ versus Ctr1-/- cells, and 3-fold lower at 2°C. The ceruloplasmin-derived (64)Cu could not be removed by extensive washing or trypsin treatment, and most was recovered in the cytosol. Actual cell copper (determined by furnace atomic absorption) increased markedly upon 24h exposure to holoceruloplasmin. This was accompanied by a conversion of holo to apoceruloplasmin in the culture medium and did not occur during incubation in the absence of cells. Four different endocytosis inhibitors failed to prevent (64)Cu uptake from ceruloplasmin. High concentrations of non-radioactive Cu(II)- or Fe(III)-NTA (substrates for cell surface reductases), or Cu(I)-NTA (to compete for transporter uptake) almost eliminated uptake of (64)Cu from ceruloplasmin. MEFs had cell surface reductase activity and expressed Steap 2 (but not Steaps 3 and 4 or dCytB). However, six-day siRNA treatment was insufficient to reduce activity or uptake. We conclude that ceruloplasmin is a circulating copper transport protein that may interact with Steap2 on the cell surface, forming apoceruloplasmin, and Cu(I) that enters cells through CTR1 and an unknown copper uptake transporter.
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spelling pubmed-47749682016-03-10 Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells Ramos, Danny Mar, David Ishida, Michael Vargas, Rebecca Gaite, Michaella Montgomery, Aaron Linder, Maria C. PLoS One Research Article Ceruloplasmin, the main copper binding protein in blood plasma, has been of particular interest for its role in efflux of iron from cells, but has additional functions. Here we tested the hypothesis that it releases its copper for cell uptake by interacting with a cell surface reductase and transporters, producing apoceruloplasmin. Uptake and transepithelial transport of copper from ceruloplasmin was demonstrated with mammary epithelial cell monolayers (PMC42) with tight junctions grown in bicameral chambers, and purified human (64)Cu-labeled ceruloplasmin secreted by HepG2 cells. Monolayers took up virtually all the (64)Cu over 16h and secreted half into the apical (milk) fluid. This was partly inhibited by Ag(I). The (64)Cu in ceruloplasmin purified from plasma of (64)Cu-injected mice accumulated linearly in mouse embryonic fibroblasts (MEFs) over 3-6h. Rates were somewhat higher in Ctr1+/+ versus Ctr1-/- cells, and 3-fold lower at 2°C. The ceruloplasmin-derived (64)Cu could not be removed by extensive washing or trypsin treatment, and most was recovered in the cytosol. Actual cell copper (determined by furnace atomic absorption) increased markedly upon 24h exposure to holoceruloplasmin. This was accompanied by a conversion of holo to apoceruloplasmin in the culture medium and did not occur during incubation in the absence of cells. Four different endocytosis inhibitors failed to prevent (64)Cu uptake from ceruloplasmin. High concentrations of non-radioactive Cu(II)- or Fe(III)-NTA (substrates for cell surface reductases), or Cu(I)-NTA (to compete for transporter uptake) almost eliminated uptake of (64)Cu from ceruloplasmin. MEFs had cell surface reductase activity and expressed Steap 2 (but not Steaps 3 and 4 or dCytB). However, six-day siRNA treatment was insufficient to reduce activity or uptake. We conclude that ceruloplasmin is a circulating copper transport protein that may interact with Steap2 on the cell surface, forming apoceruloplasmin, and Cu(I) that enters cells through CTR1 and an unknown copper uptake transporter. Public Library of Science 2016-03-02 /pmc/articles/PMC4774968/ /pubmed/26934375 http://dx.doi.org/10.1371/journal.pone.0149516 Text en © 2016 Ramos et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ramos, Danny
Mar, David
Ishida, Michael
Vargas, Rebecca
Gaite, Michaella
Montgomery, Aaron
Linder, Maria C.
Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title_full Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title_fullStr Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title_full_unstemmed Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title_short Mechanism of Copper Uptake from Blood Plasma Ceruloplasmin by Mammalian Cells
title_sort mechanism of copper uptake from blood plasma ceruloplasmin by mammalian cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4774968/
https://www.ncbi.nlm.nih.gov/pubmed/26934375
http://dx.doi.org/10.1371/journal.pone.0149516
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