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Thiosemicarbazone Mixed-Valence Cu(I/II) Complex Against Lung Adenocarcinoma Cells Through Multiple Pathways Involving Cuproptosis

Overview
Journal J Med Chem
Specialty Chemistry
Date 2024 May 23
PMID 38778566
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Abstract

Induction of cuproptosis and targeting of multiple signaling pathways show promising applications in tumor therapy. In this study, we synthesized two thiosemicarbazone-copper complexes ([Cu(L)Cl] 1 and [CuCu(L)Cl] 2, where HL is the ()--methyl-2-(phenyl(pyridin-2-yl)methylene ligand), to assess their antilung cancer activities. Both copper complexes showed better anticancer activity than cisplatin and exhibited hemolysis comparable to that of cisplatin. experiments showed that complex 2 retarded the A549 cell growth in a mouse xenograft model with low systemic toxicity. Primarily, complex 2 kills lung cancer cells and by triggering multiple pathways, including cuproptosis. Complex 2 is the first mixed-valent Cu(I/II) complex to induce cellular events consistent with cuproptosis in cancer cells, which may stimulate the development of mixed-valent copper complexes and provide effective cancer therapy.

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