| Literature DB >> 34958363 |
Ottis Scrivner1, Long Dao2, M Karen Newell-Rogers2, Babbak Shahandeh3, Frank L Meyskens3, Susan Kurumi Kozawa4, Feng Liu-Smith4, Germán Plascencia-Villa5, Miguel José-Yacamán6, Shang Jia7, Christopher J Chang7,8, Patrick J Farmer1.
Abstract
In this report, we investigate the toxicity of the ionophore thiomaltol (Htma) and Cu salts to melanoma. Divalent metal complexes of thiomaltol display toxicity against A375 melanoma cell culture resulting in a distinct apoptotic response at submicromolar concentrations, with toxicity of Cu(tma)2 > Zn(tma)2 >> Ni(tma)2. In metal-chelated media, Htma treatment shows little toxicity, but the combination with supplemental CuCl2, termed Cu/Htma treatment, results in toxicity that increases with suprastoichiometric concentrations of CuCl2 and correlates with the accumulation of intracellular copper. Electron microscopy and confocal laser scanning microscopy of Cu/Htma treated cells shows a rapid accumulation of copper within lysosomes over the course of hours, concurrent with the onset of apoptosis. A buildup of ubiquitinated proteins due to proteasome inhibition is seen on the same timescale and correlates with increases of copper without additional Htma.Entities:
Keywords: apoptosis; copper ionophore; melanoma; proteasome inhibition; thiomaltol
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Year: 2022 PMID: 34958363 PMCID: PMC8763036 DOI: 10.1093/mtomcs/mfab074
Source DB: PubMed Journal: Metallomics ISSN: 1756-5901 Impact factor: 4.526