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  • Title: Spectroscopic and electronic structure studies of symmetrized models for reduced members of the dimethylsulfoxide reductase enzyme family.
    Author: McNaughton RL, Lim BS, Knottenbelt SZ, Holm RH, Kirk ML.
    Journal: J Am Chem Soc; 2008 Apr 09; 130(14):4628-36. PubMed ID: 18341333.
    Abstract:
    Enzymes belonging to the dimethylsulfoxide reductase (DMSOR) family of pyranopterin Mo enzymes have a unique active-site geometry in the reduced form that lacks a terminal oxo ligand, unlike the reduced active sites of other pyranopterin Mo enzymes. Furthermore, the DMSOR family is characterized by the coordination of two pyranopterin-ene-1,2-dithiolate ligands in their active sites, which is distinctive among the other pyranopterin Mo enzymes but analogous to all of the currently known tungsten-containing enzymes. Electronic absorption, resonance Raman, and ground- and excited-state density functional calculations of symmetrized analogues of the reduced DMSOR active site ([NEt4][Mo(IV)(QAd)(S2C2Me2)2] where Ad = 2-adamantyl; Q = O, S, Se) have allowed for a detailed description of Mo-bisdithiolene electronic structure in the absence of a strong-field oxo ligand. The electronic absorption spectra are dominated by dithiolene S --> Mo charge-transfer transitions, and the totally symmetric Mo-S Raman stretch is observed at approximately 400 cm(-1) for all three complexes. These data indicate that the Mo-bisdithiolene bonding scheme in high-symmetry [Mo(QAd)(S2C2Me2)2]- complexes is not strongly perturbed by the apical QAd- ligands, but instead, the dithiolene ligands define the t(2g) ligand field splitting. The effects of conserved geometric distortions observed in DMSOR, relative to these high-symmetry models, were explored by spectroscopically calibrated bonding calculations, and the results are discussed within the context of electronic structure contributions to ground-state destabilization and transition-state stabilization. The specific electronic structure tuning of the endogenous amino acid ligation on the mechanism of DMSOR is also discussed.
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