RESUMO

With a view to developing multimetallic molecular catalysts that mimic the oxygen-evolving catalyst (OEC) in Nature's photosystem II, the synthesis of various dicubanoid manganese clusters is described and their catalytic activity investigated for water oxidation in basic, aqueous solution. Pyridinemethanol-based ligands are known to support polynuclear and cubanoid structures in manganese coordination chemistry. The chelators 2,6-pyridinedimethanol (H2 L1 ) and 6-methyl-2-pyridinemethanol (HL2 ) were chosen to yield polynuclear manganese complexes; namely, the tetranuclear defective dicubanes [MnII 2 MnIII 2 (HL1 )4 (OAc)4 (OMe)2 ] and [MnII 2 MnIII 2 (HL1 )6 (OAc)2 ] (OAc)2 ⋅2 H2 O, as well as the octanuclear-dicubanoid [MnII 6 MnIII 2 (L2 )4 (O)2 (OAc)10 (HOMe/OH2 )2 ]⋅3MeOH⋅MeCN. In freshly prepared solutions, polynuclear species were detected by electrospray ionization mass spectrometry, whereas X-band electron paramagnetic resonance studies in dilute, liquid solution suggested the presence of divalent mononuclear Mn species with g values of 2. However, the magnetochemical investigation of the complexes' solutions by the Evans technique confirmed a haphazard combination of manganese coordination complexes, from mononuclear to polynuclear species. Subsequently, the newly synthesized and characterized manganese molecular complexes were employed as precursors to prepare electrode-deposited films in a buffer-free solution to evaluate and compare their stability and catalytic activity for water oxidation electrocatalysis.

RESUMO

The role of NO in biology is well established. However, an increasing body of evidence suggests that azanone (HNO), could also be involved in biological processes, some of which are attributed to NO. In this context, one of the most important and yet unanswered questions is whether and how HNO is produced in vivo. A possible route concerns the chemical or enzymatic reduction of NO. In the present work, we have taken advantage of a selective HNO sensing method, to show that NO is reduced to HNO by biologically relevant alcohols with moderate reducing capacity, such as ascorbate or tyrosine. The proposed mechanism involves a nucleophilic attack to NO by the alcohol, coupled to a proton transfer (PCNA: proton-coupled nucleophilic attack) and a subsequent decomposition of the so-produced radical to yield HNO and an alkoxyl radical.

Assuntos

Álcoois/química , Ácido Ascórbico/química , Óxido Nítrico/química , Óxidos de Nitrogênio/química , Tirosina/química , Álcoois/metabolismo , Animais , Ácido Ascórbico/metabolismo , Bovinos , Células Endoteliais/metabolismo , Óxido Nítrico/metabolismo , Óxidos de Nitrogênio/metabolismo , Oxirredução , Tirosina/metabolismo