Hydrolytically stable PdII and PtII complexes supported by acyclic diaminocarbene ligands represent a novel class of structural organometallic anticancer agents exhibiting nanomolar antiproliferative activity in a panel of cancer cell lines (IC50 0.07–0.81 μM) and up to 300-fold selectivity for cancer cells over normal primary fibroblasts. The lead drug candidate was 300 times more potent than cisplatin in vitro and showed higher efficacy in reducing the growth of aggressive MDA-MB-231 xenograft tumors in mice. © 2024 Wiley-VCH GmbH.
Original languageEnglish
Article numbere202400101
JournalChemistry - A European Journal
DOIs
StateE-pub ahead of print - 16 Feb 2024

    Research areas

  • antitumor agents, diaminocarbenes, drug discovery, palladium, platinum, Cancer cells, Cells, Diseases, Drug products, Mammals, Organometallics, Palladium compounds, Platinum compounds, Acyclic diaminocarbenes, Anti-cancer agents, Antiproliferative activities, Antitumour agents, Cancer cell lines, Diaminocarbenes, Drug discovery, Nanomolar, Triple-negative breast cancers, Cell culture

ID: 117120693