Redox reactions of a pyrazine-bridged RuIII(edta) binuclear complex: spectrochemical, spectroelectrochemical and theoretical studies

Abstract

The redox reactions of a pyrazine-bridged binuclear [(edta)Ru^IIIpzRu^III(edta)]²⁻ (edta⁴⁻ = ethylenediaminetetraacetate; pz = pyrazine) have been investigated spectrochemically and spectroelectrochemically for the first time. The kinetics of the reduction of [(edta)Ru^IIIpzRu^III(edta)]²⁻ (Ru^III–Ru^III) with the ascorbic acid anion (HA⁻) was studied as a function of ascorbic concentration and temperature at a fixed pH 6.0. The overall reaction of Ru^III–Ru^III was found to consist of two-steps involving the initial formation of the mixed-valence [(edta)Ru^IIpzRu^III(edta)]³⁻ (Ru^II–Ru^III) intermediate complex (λ_max = 462 nm, ε_max = 10 000 M⁻¹ cm⁻¹), which undergoes further reduction by ascorbic acid to produce the [(edta)Ru^IIpzRu^II(edta)]⁴⁻(Ru^II–Ru^II) ultimate product complex (λ_max = 540 nm, ε_max = 20 700 M⁻¹ cm⁻¹). Our studies further revealed that the Ru^II–Ru^III and Ru^II–Ru^II species are formed in the electrochemical reduction of the Ru^III–Ru^III complex at 0.0 and −0.4 V (vs. SHE), respectively. Formation of Ru^II–Ru^III and Ru^II–Ru^II was further corroborated by magnetic moment measurements and DFT calculations. Kinetic data and activation parameters are interpreted in terms of a mechanism involving rate-determining outer-sphere electron transfer between Ru(III) and the ascorbate monoanion (HA⁻) at pH 6.0. A detailed reaction mechanism in agreement with the spectral, spectro-electrochemical and kinetic data is presented. The results of the spectral and kinetic studies of the reaction of the Ru^II–Ru^II complex with molecular oxygen (O₂) reveal the ability of the Ru^II–Ru^II species to effect the oxygen reduction reaction (ORR) leading to the formation of H₂O₂, a partial reduction product of dioxygen (O₂).