Surface Characteristics, Copper Release, and Toxicity of Nano- and Micrometer-Sized Copper and Copper(II) Oxide Particles: A Cross-Disciplinary Study

An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano‐ and micrometer‐sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All...

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Vydané v:Small (Weinheim an der Bergstrasse, Germany) Ročník 5; číslo 3; s. 389 - 399
Hlavní autori: Midander, Klara, Cronholm, Pontus, Karlsson, Hanna L., Elihn, Karine, Möller, Lennart, Leygraf, Christofer, Wallinder, Inger Odnevall
Médium: Journal Article
Jazyk:English
Vydavateľské údaje: Weinheim WILEY-VCH Verlag 06.02.2009
WILEY‐VCH Verlag
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ISSN:1613-6810, 1613-6829, 1613-6829
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Abstract An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano‐ and micrometer‐sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All particles, except micrometer‐sized Cu, release more copper in serum‐containing cell medium (supplemented Dulbecco's minimal essential medium) compared to identical exposures in phosphate‐buffered saline. Sonication of particles for dispersion prior to exposure has a large effect on the initial copper release from Cu nanoparticles. A clear size‐dependent effect is observed from both a copper release and a toxicity perspective. In agreement with greater released amounts of copper per quantity of particles from the nanometer‐sized particles compared to the micrometer‐sized particles, the nanometer particles cause a higher degree of DNA damage (single‐strand breaks) and cause a significantly higher percentage of cell death compared to cytotoxicity induced by micrometer‐sized particles. Cytotoxic effects related to the released copper fraction are found to be significantly lower than the effects related to particles. No DNA damage is induced by the released copper fraction. Save your breath: A multianalytical approach is used to assess the toxicity to cultured lung cells of micro‐ and nanoparticles of oxidized Cu and CuO in relation to the particle characteristics (see picture). Larger amounts of copper per quantity of particles are released from nanoparticles than micrometer‐sized particles. The cytotoxic effects of nanoparticles are caused by the particles rather than the released copper fraction.
AbstractList An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano- and micrometer-sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All particles, except micrometer-sized Cu, release more copper in serum-containing cell medium (supplemented Dulbecco's minimal essential medium) compared to identical exposures in phosphate-buffered saline. Sonication of particles for dispersion prior to exposure has a large effect on the initial copper release from Cu nanoparticles. A clear size-dependent effect is observed from both a copper release and a toxicity perspective. In agreement with greater released amounts of copper per quantity of particles from the nanometer-sized particles compared to the micrometer-sized particles, the nanometer particles cause a higher degree of DNA damage (single-strand breaks) and cause a significantly higher percentage of cell death compared to cytotoxicity induced by micrometer-sized particles. Cytotoxic effects related to the released copper fraction are found to be significantly lower than the effects related to particles. No DNA damage is induced by the released copper fraction.An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano- and micrometer-sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All particles, except micrometer-sized Cu, release more copper in serum-containing cell medium (supplemented Dulbecco's minimal essential medium) compared to identical exposures in phosphate-buffered saline. Sonication of particles for dispersion prior to exposure has a large effect on the initial copper release from Cu nanoparticles. A clear size-dependent effect is observed from both a copper release and a toxicity perspective. In agreement with greater released amounts of copper per quantity of particles from the nanometer-sized particles compared to the micrometer-sized particles, the nanometer particles cause a higher degree of DNA damage (single-strand breaks) and cause a significantly higher percentage of cell death compared to cytotoxicity induced by micrometer-sized particles. Cytotoxic effects related to the released copper fraction are found to be significantly lower than the effects related to particles. No DNA damage is induced by the released copper fraction.
An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano‐ and micrometer‐sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All particles, except micrometer‐sized Cu, release more copper in serum‐containing cell medium (supplemented Dulbecco's minimal essential medium) compared to identical exposures in phosphate‐buffered saline. Sonication of particles for dispersion prior to exposure has a large effect on the initial copper release from Cu nanoparticles. A clear size‐dependent effect is observed from both a copper release and a toxicity perspective. In agreement with greater released amounts of copper per quantity of particles from the nanometer‐sized particles compared to the micrometer‐sized particles, the nanometer particles cause a higher degree of DNA damage (single‐strand breaks) and cause a significantly higher percentage of cell death compared to cytotoxicity induced by micrometer‐sized particles. Cytotoxic effects related to the released copper fraction are found to be significantly lower than the effects related to particles. No DNA damage is induced by the released copper fraction. Save your breath: A multianalytical approach is used to assess the toxicity to cultured lung cells of micro‐ and nanoparticles of oxidized Cu and CuO in relation to the particle characteristics (see picture). Larger amounts of copper per quantity of particles are released from nanoparticles than micrometer‐sized particles. The cytotoxic effects of nanoparticles are caused by the particles rather than the released copper fraction.
An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano- and micrometer-sized particles of oxidized metallic copper and copper(II) oxide in contact with cultivated lung cells, as well as copper release in relevant media. All particles, except micrometer-sized Cu, release more copper in serum-containing cell medium (supplemented Dulbecco's minimal essential medium) compared to identical exposures in phosphate-buffered saline. Sonication of particles for dispersion prior to exposure has a large effect on the initial copper release from Cu nanoparticles. A clear size-dependent effect is observed from both a copper release and a toxicity perspective. In agreement with greater released amounts of copper per quantity of particles from the nanometer-sized particles compared to the micrometer-sized particles, the nanometer particles cause a higher degree of DNA damage (single-strand breaks) and cause a significantly higher percentage of cell death compared to cytotoxicity induced by micrometer-sized particles. Cytotoxic effects related to the released copper fraction are found to be significantly lower than the effects related to particles. No DNA damage is induced by the released copper fraction.
Author Elihn, Karine
Cronholm, Pontus
Möller, Lennart
Wallinder, Inger Odnevall
Leygraf, Christofer
Karlsson, Hanna L.
Midander, Klara
Author_xml – sequence: 1
  givenname: Klara
  surname: Midander
  fullname: Midander, Klara
  organization: Division of Corrosion Science, Department of Chemistry School of Chemical Science and Engineering Royal Institute of Technology Drottning Kristinas väg 51, 100 44 Stockholm (Sweden)
– sequence: 2
  givenname: Pontus
  surname: Cronholm
  fullname: Cronholm, Pontus
  organization: Unit for Analytical Toxicology, Department of Biosciences at Novum Karolinska Institutet, 141 57 Huddinge, Stockholm (Sweden)
– sequence: 3
  givenname: Hanna L.
  surname: Karlsson
  fullname: Karlsson, Hanna L.
  organization: Unit for Analytical Toxicology, Department of Biosciences at Novum Karolinska Institutet, 141 57 Huddinge, Stockholm (Sweden)
– sequence: 4
  givenname: Karine
  surname: Elihn
  fullname: Elihn, Karine
  organization: Atmospheric Science Unit Department of Applied Environmental Science Stockholm University, 106 91 Stockholm (Sweden)
– sequence: 5
  givenname: Lennart
  surname: Möller
  fullname: Möller, Lennart
  organization: Unit for Analytical Toxicology, Department of Biosciences at Novum Karolinska Institutet, 141 57 Huddinge, Stockholm (Sweden)
– sequence: 6
  givenname: Christofer
  surname: Leygraf
  fullname: Leygraf, Christofer
  organization: Division of Corrosion Science, Department of Chemistry School of Chemical Science and Engineering Royal Institute of Technology Drottning Kristinas väg 51, 100 44 Stockholm (Sweden)
– sequence: 7
  givenname: Inger Odnevall
  surname: Wallinder
  fullname: Wallinder, Inger Odnevall
  email: ingero@kth.se
  organization: Division of Corrosion Science, Department of Chemistry School of Chemical Science and Engineering Royal Institute of Technology Drottning Kristinas väg 51, 100 44 Stockholm (Sweden)
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crossref_primary_10_1016_j_etap_2009_12_002
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References_xml – reference: D. B. Warheit, T. R. Webb, C. M. Sayes, V. L. Colvin, K. L. Reed, Toxicol. Sci. 2006, 91, 227-236.
– reference: K. Midander, I. O. Wallinder, C. Leygraf, Environ. Pollut. 2007, 145, 51.
– reference: D. B. Warheit, T. R. Webb, V. L. Colvin, K. L. Reed, C. M. Sayes, Toxicol. Sci. 2007, 95, 270-280.
– reference: N. Lewinski, V. Colvin, R. Drezek, Small 2008, 4, 26-49.
– reference: M. P. Holsapple, W. H. Farland, T. D. Landry, N. A. Monteiro-Riviere, J. M. Carter, N. J. Walker, K. V. Thomas, Toxicol. Sci. 2005, 88, 12-17.
– reference: Z. Chen, H. Meng, G. Xing, C. Chen, Y. Zhao, G. Jia, T. Wang, H. Yuan, C. Ye, F. Zhao, Z. Chai, C. Zhu, X. Fang, B. Ma, L. Wan, Toxicol. Lett. 2006, 163, 109-120.
– reference: N. P. Singh, M. T. McCoy, R. R. Tice, E. L. Schneider, Exp. Cell Res. 1988, 175, 184.
– reference: R. Colognato, A. Bonelli, J. Ponti, M. Farina, E. Bergamaschi, E. Sabbioni, L. Migliore, Mutagenesis 2008, 23, 377-382.
– reference: S. K. Chawla, N. Sankarraman, J. H. Payer, J. Electron Spectrosc. Relat. Phenom. 1992, 61, 1-18.
– reference: C. A. Pope, III, R. T. Burnett, M. J. Thun, E. E. Calle, D. Krewski, K. Ito, G. D. Thurston, JAMA 2003, 287, 1132-1141.
– reference: R. J. Griffitt, R. Weil, K. A. Hyndman, N. D. Denslow, K. Powers, D. Taylor, D. S. Barber, Environ. Sci. Technol. 2007, 41, 8178-8186.
– reference: K. Donaldson, D. Brown, A. Clouter, R. Duffin, W. MacNee, L. Renwick, L. Tran, V. Stone, J. Aerosol Med. 2002, 15, 213-220.
– reference: A. J. Cohen, C. A. Pope, III, Environ. Health Perspect. 1995, 103, 219-224.
– reference: R. C. Murdock, L. Braydich-Stolle, A. M. Schrand, J. J. Schlager, S. M. Hussain, Toxicol. Sci. 2007, 239-253.
– reference: L. K. Limbach, Y. Li, R. N. Grass, T. J. Brunner, M. A. Hintermann, M. Muller, D. Gunther, W. J. Stark, Environ. Sci. Technol. 2005, 39, 9370-9376.
– reference: G. Oberdorster, E. Oberdorster, J. Oberdorster, Environ. Health Perspect. 2005, 113, 823-839.
– reference: C. D. Taylor, M. Neurock, J. R. Scully, J. Electrochem. Soc. 2008, 155, C407-C414.
– reference: J. Gabbay, G. Borkow, J. Mishal, E. Magen, R. Zatcoff, Y. Shemer-Avni, J. Ind. Textiles 2006, 35, 323-335.
– reference: P. Borm, D. Robbins, S. Haubold, T. Kuhlbusch, H. Fissan, K. Donaldson, R. Schins, V. Stone, W. Kreyling, J. Lademann, J. Krutmann, D. Warheit, E. Oberdorster, Part. Fibre Toxicol. 2006, 3, 11.
– reference: M. Heinlaan, A. Ivask, I. Blinova, H.-C. Dubourguier, A. Kahru, Chemosphere 2008, 71, 1308-1316.
– reference: A. M. Knaapen, P. J. A. Borm, C. Albrecht, R. P. F. Schins, Int. J. Cancer 2004, 109, 799-809.
– reference: Y. C. Zhang, J. Y. Tang, G. L. Wang, M. Zhang, X. Y. Hu, J. Cryst. Growth 2006, 294, 278-282.
– reference: N. Cioffi, N. Ditaranto, L. Torsi, R. A. Picca, L. Sabbatini, A. Valentini, L. Novello, G. Tantillo, T. Bleve-Zacheo, P. G. Zambonin, Anal. Bioanal. Chem. 2005, 381, 607-616.
– reference: M. Caicedo, J. J. Jacobs, A. Reddy, N. J. Hallab, J. Biomed. Mater. Res. Part A 2008, 86, 905-913.
– reference: Y. T. He, J. Wan, T. Tokunaga, J. Nanoparticle Res. 2008, 10, 321.
– reference: A. Jagminas, J. Kuzmarskyte, G. Niaura, Appl. Surf. Sci. 2002, 201, 129-137.
– reference: A. Nel, T. Xia, L. Madler, N. Li, Science 2006, 311, 622-627.
– reference: C. Monteiller, L. Tran, W. MacNee, S. Faux, A. Jones, B. Miller, K. Donaldson, Occup. Environ. Med. 2007, 64, 609-615.
– reference: W. T. Yao, S. H. Yu, Y. Zhou, J. Jiang, Q. S. Wu, L. Zhang, J. Jiang, J. Phys. Chem. B 2005, 109, 14011-14016.
– reference: G. Oberdorster, A. Maynard, K. Donaldson, V. Castranova, J. Fitzpatrick, K. Ausman, J. Carter, B. Karn, W. Kreyling, D. Lai, S. Olin, N. Monteiro-Riviere, D. Warheit, H. Yang, Part. Fibre Toxicol. 2005, 2, 8.
– reference: E. Roduner, Chem. Soc. Rev. 2006, 35, 583-592.
– reference: J. Ghijsen, L. H. Tjeng, J. van Elp, H. Eskes, J. Westerink, G. A. Sawatzky, M. T. Czyzyk, Phys. Rev. B 1988, 38, 11322-11330.
– reference: A. Russkikh, R. Baksht, A. Labetski, P. Levashov, S. Tkachenko, K. Khishchenko, A. Shishlov, A. Fedyunin, S. Chakovski, Plasma Phys. Rep. 2006, 32, 823-835.
– reference: W. Kim, J.-S. Park, C.-Y. Suh, H. Chang, J.-C. Lee, Mater. Lett. 2007, 61, 4259-4261.
– reference: L. K. Limbach, P. Wick, P. Manser, R. N. Grass, A. Bruinink, W. J. Stark, Environ. Sci. Technol. 2007, 41, 4158-4163.
– reference: T. Stoeger, C. Reinhard, S. Takenaka, A. Schroeppel, E. Karg, B. Ritter, J. Heyder, H. Schulz, Environ. Health Perspect. 2006, 114, 328-333.
– reference: H. Meng, Z. Chen, G. Xing, H. Yuan, C. Chen, F. Zhao, C. Zhang, Y. Zhao, Toxicol. Lett. 2007, 175, 102-110.
– reference: M. Parhizkar, S. Singh, P. K. Nayak, N. Kumar, K. P. Muthe, S. K. Gupta, R. S. Srinivasa, S. S. Talwar, S. S. Major, Colloids Surf. A: Physicochem. Eng. Asp. 2005, 277-282.
– volume: 381
  start-page: 607
  year: 2005
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Snippet An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano‐ and micrometer‐sized...
An interdisciplinary and multianalytical research effort is undertaken to assess the toxic aspects of thoroughly characterized nano- and micrometer-sized...
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SubjectTerms Cell Line
Chemical engineering
Chemical process and manufacturing engineering
copper
Copper - chemistry
Copper - toxicity
cytotoxicity
DNA Damage
Kemisk process- och produktionsteknik
Kemiteknik
Metal Nanoparticles - chemistry
Metal Nanoparticles - toxicity
Metal Nanoparticles - ultrastructure
Microscopy, Electron, Scanning
nanoparticles
particle characterization
Spectrophotometry, Atomic
Surface and colloid chemistry
Surface Properties
TECHNOLOGY
TEKNIKVETENSKAP
Yt- och kolloidkemi
Title Surface Characteristics, Copper Release, and Toxicity of Nano- and Micrometer-Sized Copper and Copper(II) Oxide Particles: A Cross-Disciplinary Study
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https://onlinelibrary.wiley.com/doi/abs/10.1002%2Fsmll.200801220
https://www.ncbi.nlm.nih.gov/pubmed/19148889
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https://www.proquest.com/docview/66889343
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Volume 5
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