AI Article Synopsis

  • Auranofin (AUF) is a gold-based drug that's mainly used to treat arthritis but is being studied for treating cancer too.
  • It works by stopping a protein called thioredoxin reductase, but it also affects cancer cells in other ways depending on the type of cancer and how much is used.
  • In tests on breast cancer cells, AUF caused stress inside the cells that made them stop growing and weakened their structure, showing that AUF can have special effects that might help fight cancer better.

Article Abstract

Auranofin (Ridaura, AUF) is a gold complex originally approved as an antirheumatic agent that has emerged as a potential candidate for multiple repurposed therapies. The best-studied anticancer mechanism of AUF is the inhibition of thioredoxin reductase (TrxR). However, a number of reports indicate a more complex and multifaceted mode of action for AUF that could be cancer cell type- and dose-dependent. In this study, we observed that AUF displayed variable cytotoxicity in five triple-negative breast cancer cell lines. Using representative MDA-MB-231 cells treated with moderate and cytotoxic doses of AUF, we evidenced that an AUF-mediated TrxR inhibition alone may not be sufficient to induce cell death. Cytotoxic doses of AUF elicited rapid and drastic intracellular oxidative stress affecting the mitochondria, cytoplasm and nucleus. A "redoxome" proteomics investigation revealed that a short treatment with a cytotoxic dose AUF altered the redox state of a number of cysteines-containing proteins, pointing out that the cell proliferation/cell division/cell cycle and cell-cell adhesion/cytoskeleton structure were the mostly affected pathways. Experimentally, AUF treatment triggered a dose-dependent S-phase arrest and a rapid disintegration of the actin cytoskeleton structure. Our study shows a new spectrum of AUF-induced early effects and should provide novel insights into the complex redox-based mechanisms of this promising anticancer molecule.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9562029PMC
http://dx.doi.org/10.3390/cancers14194864DOI Listing

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