Methionine Ligand Interaction in a Blue Copper Protein Characterized by Site-Selective Infrared Spectroscopy

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The reactivity of metal sites in proteins is tuned by protein-based ligands. For example, in blue copper proteins such as plastocyanin (Pc), the structure imparts a highly elongated bond between the Cu and a methionine (Met) axial ligand to modulate its redox properties. Despite extensive study, a complete understanding of the contribution of the protein to redox activity is challenged by experimentally accessing both redox states of metalloproteins. Using infrared (IR) spectroscopy in combination with site-selective labeling with carbon deuterium (C-D) vibrational probes, we characterized the localized changes at the Cu ligand Met97 in the oxidized and reduced states, as well as the Zn(II) or Co(II)-substituted, the pH-induced low-coordinate, the apoprotein, and the unfolded states. The IR absorptions of (d(3)-methyl)Met97 are highly sensitive to interaction of the sulfur-based orbitals with the metal center and are demonstrated to be useful reporters of its modulation in the different states. Unrestricted Kohn-Sham density functional theory calculations performed on a model of the Cu site of Pc confirm the observed dependence. IR spectroscopy was then applied to characterize the impact of binding to the physiological redox partner cytochrome (cyt) f. The spectral changes suggest a slightly stronger Cu-S(Met97) interaction in the complex with cyt f that has potential to modulate the electron transfer properties. Besides providing direct, molecular-level comparison of the oxidized and reduced states of Pc from the perspective of the axial Met ligand and evidence for perturbation of the Cu site properties by redox partner binding, this study demonstrates the localized spatial information afforded by IR spectroscopy of selectively incorporated C-D probes
Publisher
AMER CHEMICAL SOC
Issue Date
2016-06
Language
English
Article Type
Article
Keywords

PLASTOCYANIN SINGLE-CRYSTALS; CARBON-DEUTERIUM BONDS; NOSTOC SP PCC-7119; ELECTRONIC-STRUCTURE; CYTOCHROME-F; SUBSTITUTED PSEUDOAZURIN; POPLAR PLASTOCYANIN; ACTIVE-SITE; DYNAMICS; COORDINATION

Citation

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, v.138, no.22, pp.7187 - 7193

ISSN
0002-7863
DOI
10.1021/jacs.6b03916
URI
http://hdl.handle.net/10203/212130
Appears in Collection
CH-Journal Papers(저널논문)
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