Acta Neuropathologica Communications (Jun 2025)

Copper supplementation mitigates Parkinson-like wild-type SOD1 pathology and nigrostriatal degeneration in a novel mouse model

  • Benjamin D. Rowlands,
  • Benjamin G. Trist,
  • Connor Karozis,
  • Greta Schaffer,
  • David Mor,
  • Richard Harwood,
  • Sarah A. Rosolen,
  • Veronica Cottam,
  • Freyja Persson-Carboni,
  • Miriam Richardson,
  • Anne A. Li,
  • Michael P. Gotsbacher,
  • Amr H. Abdeen,
  • Rachel Codd,
  • Kay L. Double

DOI
https://doi.org/10.1186/s40478-025-02048-2
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 23

Abstract

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Abstract Misfolded wild-type superoxide dismutase 1 (disSOD1) protein is implicated in the death of substantia nigra (SN) dopamine neurons in Parkinson disease. Regionally reduced copper availability, and subsequent reduced copper binding to SOD1, is a key factor driving the development of this pathology, suggesting brain copper supplementation may constitute an effective means of preventing its formation. We evaluated whether the blood-brain-barrier-permeable copper delivery drug, CuATSM, attenuated the misfolding and deposition of wild-type disSOD1 and associated neuron death in a novel mouse model that expresses this pathology. These factors were profiled using proteomic and elemental mass spectrometry, together with biochemical and histological workflows. We demonstrated copper supplementation corrects altered post-translational modifications on soluble SOD1 and improves the enzymatic activity of the protein in the brains of these animals. These changes were associated with a significant reduction in disSOD1 pathology and preservation of dopamine neurons in the SN, which were highly correlated with tissue copper levels. Our data position wild-type disSOD1 pathology as a novel drug target for Parkinson disease and suggest that brain copper supplementation may constitute an effective means of slowing SN dopamine neuron death in this disorder.

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