Exploring the potential of gold(III) cyclometallated compounds as cytotoxic agents: variations on the C^N theme
Articolo
Data di Pubblicazione:
2015
Citazione:
Exploring the potential of gold(III) cyclometallated compounds as cytotoxic agents: variations on the C^N theme / Bertrand, B; Spreckelmeyer, S; Bodio, E; Cocco, Fabio; Picquet, M; Richard, P; Le Gendre, P; Orvig, C; Cinellu, Maria Agostina; Casini, A.. - In: DALTON TRANSACTIONS. - ISSN 1477-9226. - 44:(2015), pp. 11911-11918.
Abstract:
A series of novel (C^N) cyclometallated Au(III) complexes of general formula [Au(pyb-H)L1L2]n+ (pyb-H =
C^N cyclometallated 2-benzylpyridine, L1 and L2 being chlorido, phosphane or glucosethiolato ligands,
n = 0 or 1) have been synthesized and fully characterized using different techniques, including NMR,
IR and far-IR, mass spectrometry, as well as elemental analysis. The crystal structure of one compound
has been solved using X-ray diffraction methods. All compounds were tested in vitro in five human cancer
cell lines including the lung, breast, colon and ovarian cancer cells. For comparison purposes, all compounds
were also tested in a model of healthy human cells from the embryonic kidney. Notably, all new
compounds were more toxic than their cyclometallated precursor bearing two chlorido ligands, and the
derivative bearing one phosphane ligand presented the most promising toxicity profile in our in vitro
screening, displaying a p53 dependent activity in colorectal cancer HCT116 cells. Finally, for the first time
C^N cyclometallated gold(III) complexes were shown to be potent inhibitors of the zinc finger protein
PARP-1, involved in the mechanism of cisplatin resistance.
C^N cyclometallated 2-benzylpyridine, L1 and L2 being chlorido, phosphane or glucosethiolato ligands,
n = 0 or 1) have been synthesized and fully characterized using different techniques, including NMR,
IR and far-IR, mass spectrometry, as well as elemental analysis. The crystal structure of one compound
has been solved using X-ray diffraction methods. All compounds were tested in vitro in five human cancer
cell lines including the lung, breast, colon and ovarian cancer cells. For comparison purposes, all compounds
were also tested in a model of healthy human cells from the embryonic kidney. Notably, all new
compounds were more toxic than their cyclometallated precursor bearing two chlorido ligands, and the
derivative bearing one phosphane ligand presented the most promising toxicity profile in our in vitro
screening, displaying a p53 dependent activity in colorectal cancer HCT116 cells. Finally, for the first time
C^N cyclometallated gold(III) complexes were shown to be potent inhibitors of the zinc finger protein
PARP-1, involved in the mechanism of cisplatin resistance.
Tipologia CRIS:
1.1 Articolo in rivista
Keywords:
Cyclometalated gold complexes; cytotoxicity; PARP inhibition
Elenco autori:
Bertrand, B; Spreckelmeyer, S; Bodio, E; Cocco, Fabio; Picquet, M; Richard, P; Le Gendre, P; Orvig, C; Cinellu, Maria Agostina; Casini, A.
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