Rationale [Cu(P)4][BF4]-type complexes (P = tertiary phosphine) have shown significant antitumor activity. This biological property appears to be activated via formation of coordinative unsaturated [Cu(P)n]+ species (n < 4), that may interact with various molecules starting from the solvent(s) in which they are dissolved. Aim of our study was to investigate the interaction of these species with different solvent mixtures. Methods The interaction has been investigated in electrospray ionization mass spectrometry, and the interaction products have been characterized by multiple collisional experiments, using an ion trap mass instrument. Density Functional Theory (DFT) calculations studies, using a meta-hybrid exchange correlation (xc) functional and an implicit solvent model, were employed to investigate the equilibrium distribution of species in solution. Results Depending on the nature of the solvent mixture and coordinated phosphine, three [Cu(P)4][BF4]-type complexes undergo dissociation with formation of [Cu(P)2]+, [Cu(P)(solv)]+ and [Cu(solv)2]+ species (solv = solvent). Preferred collisionally induced fragmentations pathways provide qualitative information on the selectivity of [Cu(P)n]+ for specific solvents and donor atoms. Formation free energies and equilibrium constants pertaining [CuI(PTA)n]+, [CuI/II(solv)n]m+ (n <= 4; m = 1, 2) and [CuI(PTA)2-k(sol)k]+ (k = 1,2) provide a comprehensive picture of equilibria in solution. Conclusions DMSO and acetonitrile strongly affect [Cu(P)n]+ assemblies producing mixed-ligand [Cu(P)(DMSO)]+ and [Cu(P)(MeCN)]+ species. Excess of both DMSO and MeCN solvents are able to fully displace coordinated phosphines giving [Cu(solv)2]+-type adducts. The presence of phosphines in the native complex is mandatory to retain the reduced oxidation state of copper. Instead, the more labile [CuI(MeCN)4]+ complex dissolved in DMSO and MeCN display a combination of Cu(I) and Cu(II) adducts.
Interaction products of cytotoxic Cu(I) complexes with different solvent mixtures: an electrospray ionization mass spectrometry and density functional theory study
Tisato F;Forrer D;Tamburini S;Vittadini A;Traldi P;Porchia M
2017
Abstract
Rationale [Cu(P)4][BF4]-type complexes (P = tertiary phosphine) have shown significant antitumor activity. This biological property appears to be activated via formation of coordinative unsaturated [Cu(P)n]+ species (n < 4), that may interact with various molecules starting from the solvent(s) in which they are dissolved. Aim of our study was to investigate the interaction of these species with different solvent mixtures. Methods The interaction has been investigated in electrospray ionization mass spectrometry, and the interaction products have been characterized by multiple collisional experiments, using an ion trap mass instrument. Density Functional Theory (DFT) calculations studies, using a meta-hybrid exchange correlation (xc) functional and an implicit solvent model, were employed to investigate the equilibrium distribution of species in solution. Results Depending on the nature of the solvent mixture and coordinated phosphine, three [Cu(P)4][BF4]-type complexes undergo dissociation with formation of [Cu(P)2]+, [Cu(P)(solv)]+ and [Cu(solv)2]+ species (solv = solvent). Preferred collisionally induced fragmentations pathways provide qualitative information on the selectivity of [Cu(P)n]+ for specific solvents and donor atoms. Formation free energies and equilibrium constants pertaining [CuI(PTA)n]+, [CuI/II(solv)n]m+ (n <= 4; m = 1, 2) and [CuI(PTA)2-k(sol)k]+ (k = 1,2) provide a comprehensive picture of equilibria in solution. Conclusions DMSO and acetonitrile strongly affect [Cu(P)n]+ assemblies producing mixed-ligand [Cu(P)(DMSO)]+ and [Cu(P)(MeCN)]+ species. Excess of both DMSO and MeCN solvents are able to fully displace coordinated phosphines giving [Cu(solv)2]+-type adducts. The presence of phosphines in the native complex is mandatory to retain the reduced oxidation state of copper. Instead, the more labile [CuI(MeCN)4]+ complex dissolved in DMSO and MeCN display a combination of Cu(I) and Cu(II) adducts.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
