RESUMO
Vanadium interactions with low molecular mass binders in biological fluids entail the existence of vanadium species with variable chemical and biological properties. In the course of efforts to elucidate the chemistry related to such interactions, we have explored the oxidative chemistry of vanadium(III) with the physiologically relevant tricarboxylic citric acid. Aqueous reactions involving VCl(3) and anhydrous citric acid, at pH approximately 7, resulted in blue solutions. Investigation into the nature of the species arising in those solutions revealed, through UV/visible and EPR spectroscopies, oxidation of vanadium(III) to vanadium(IV). Further addition of H(2)O(2) resulted in the oxidation of vanadium(IV) to vanadium(V), and the isolation of a new vanadium(V)-citrate complex in the form of its potassium salt. Analogous reactions with K(4)[V(2)O(2)(C(6)H(4)O(7))(2)].6H(2)O and H(2)O(2) or V(2)O(5) and citrate at pH approximately 5.5 afforded the same material. Elemental analysis pointed to the molecular formulation K(4)[V(2)O(4)(C(6)H(5)O(7))(2)].5.6H(2)O (1). Complex 1 was further characterized by FT-IR and X-ray crystallography. 1 crystallizes in the triclinic space group P(-)1, with a = 11.093(4) A, b = 9.186(3) A, c = 15.503(5) A, alpha = 78.60(1) degrees, beta = 86.16(1) degrees, gamma = 69.87(1) degrees, V = 1454.0(8) A(3), and Z = 2. The X-ray structure of 1 reveals the presence of a dinuclear vanadium(V)-citrate complex containing a V(V)(2)O(2) core. The citrate ligands are triply deprotonated, and as such they bind to vanadium(V) ions, thus generating a distorted trigonal bipyramidal geometry. Binding occurs through the central alkoxide and carboxylate groups, with the remaining two terminal carboxylates being uncoordinated. One of those carboxylates is protonated and contributes to hydrogen bond formation with the deprotonated terminal carboxylate of an adjacent molecule. Therefore, an extended network of hydrogen-bonded V(V)(2)O(2)-core-containing dimers is created in the lattice of 1. pH-dependent transformations of 1 in aqueous media suggest its involvement in a web of vanadium(V)-citrate dinuclear species, consistent with past solution speciation studies investigating biologically relevant forms of vanadium.
RESUMO
The established biochemical potential of vanadium has spurred considerable research interest in our lab, with specific focus on pertinent synthetic studies of vanadium(III) with a biologically relevant, organic, dicarboxylic acid, malic acid, in aqueous solutions. Simple reactions between VCl3 and malic acid in water, at different pH values, in the presence of H2O2, led to the crystalline dimeric complexes (Cat)4[VO(O2)(C4H3O5)]2*nH2O (Cat = K+, n = 4, 1; Cat = NH4+, n = 3, 2) and K2[VO(O2)(C4H4O5)]2*2H2O (3). All three complexes were characterized by elemental analysis, FT-IR, and UV/visible spectroscopies. Compound 1 crystallizes in the monoclinic space group P2(1)/c, with a = 8.380(5) A, b = 9.252(5) A, c = 13.714(8) A, beta = 93.60(2) degrees, V = 1061(1) A3, and Z = 4. Compound 2 crystallizes in the triclinic space group P1, with a = 9.158(4) A, b = 9.669(4) A, c = 14.185(6) A, alpha = 104.81(1) degrees, beta = 90.31(1) degrees, gamma = 115.643(13) degrees, V = 1085.0(7) A(3), and Z = 2. Compound 3 crystallizes in the monoclinic space group P2(1)/c, with a = 9.123(8) A, b = 9.439(8) A, c = 10.640(9) A, beta = 104.58(3) degrees, V = 887(1) A3, and Z = 2. The X-ray structures showed that, in 1 and 2, the dimers consist of two (V(V)=O)2O2 rhombic units to which two malate ligands are attached. The ligands are triply deprotonated and, as such, they coordinate to vanadium(V), promoting a pentagonal bipyramidal geometry. In 3, the dimeric (V(V)=O)2O2 rhombic unit persists, with the two doubly deprotonated malate ligands coordinated to the vanadium(V) ions. UV/vis and EPR spectroscopic studies on the intermediate blue solutions of the synthesis reactions of 1-3 support the existence of vanadyl-containing dimeric species. These species further react with H2O2 to yield oxidation of V(IV)2O2 to V(V)2O2 and coordination of the peroxide to vanadium(V). From the collective data on 1-3, it appears that pH acts as a decisive factor in dictating the structural features of the isolated complexes. The details of the introduced structural differentiation in the reported complexes, and their potential relevance to vanadium(V) dicarboxylate systems in biological media are dwelled on.
