The exceptional sensitivity of brain mitochondria to copper

Sabine Borchard, Francesca Bork, Tamara Rieder, Carola Eberhagen, Bastian Popper, Josef Lichtmannegger, Sabine Schmitt, Jerzy Adamski, Martin Klingenspor, Karl Heinz Weiss, Hans Zischka

Research output: Contribution to journalArticlepeer-review

52 Scopus citations

Abstract

Wilson disease (WD) is characterized by a disrupted copper homeostasis resulting in dramatically increased copper levels, mainly in liver and brain. While copper damage to mitochondria is an established feature in WD livers, much less is known about such detrimental copper effects in other organs. We therefore assessed the mitochondrial sensitivity to copper in a tissue specific manner, namely of isolated rat liver, kidney, heart, and brain mitochondria. Brain mitochondria presented with exceptional copper sensitivity, as evidenced by a comparatively early membrane potential loss, profound structural changes already at low copper dose, and a dose-dependent reduced capacity to produce ATP. This sensitivity was likely due to a copper-dependent attack on free protein thiols and due to a decreased copper reactive defense system, as further evidenced in neuroblastoma SHSY5Y cells. In contrast, an increased production of reactive oxygen species was found to be a late-stage event, only occurring in destroyed mitochondria. We therefore propose mitochondrial protein thiols as major targets of mitochondrial copper toxicity.

Original languageEnglish
Pages (from-to)11-22
Number of pages12
JournalToxicology in Vitro
Volume51
DOIs
StatePublished - Sep 2018

Keywords

  • Brain
  • Copper
  • Liver
  • Mitochondria
  • Protein oxidation
  • Wilson disease

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