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Published May 16, 2012 | Accepted Version + Supplemental Material
Journal Article Open

Outer-Sphere Contributions to the Electronic Structure of Type Zero Copper Proteins

Abstract

Bioinorganic canon states that active-site thiolate coordination promotes rapid electron transfer (ET) to and from type 1 copper proteins. In recent work, we have found that copper ET sites in proteins also can be constructed without thiolate ligation (called "type zero" sites). Here we report multifrequency electron paramagnetic resonance (EPR), magnetic circular dichroism (MCD), and nuclear magnetic resonance (NMR) spectroscopic data together with density functional theory (DFT) and spectroscopy-oriented configuration interaction (SORCI) calculations for type zero Pseudomonas aeruginosa azurin variants. Wild-type (type 1) and type zero copper centers experience virtually identical ligand fields. Moreover, O-donor covalency is enhanced in type zero centers relative that in the C112D (type 2) protein. At the same time, N-donor covalency is reduced in a similar fashion to type 1 centers. QM/MM and SORCI calculations show that the electronic structures of type zero and type 2 are intimately linked to the orientation and coordination mode of the carboxylate ligand, which in turn is influenced by outer-sphere hydrogen bonding.

Additional Information

© 2012 American Chemical Society. Received: March 13, 2012; Published: May 7, 2012. We thank Eckhard Bill and Andreas Göbels for assistance with MCD data collection. The NMR spectrometer in Rosario was purchased with funds from ANPCyT and CONICET. A.J.V. thanks ANPCyT for funding (PICT 2007-0314). A.J.V. is staff member of CONICET and an HHMI International Scholar, and M.E.Z. is recipient of a doctoral fellowship from CONICET. M.S. was supported by Alexander von Humboldt and K.S. Krishnan Research Associateship fellowships for funding. Financial support of this work by the SFB 624 ('Template Effects') and the Max-Planck-Society is also gratefully acknowledged. K.M.L., J.H.R., and H.B.G. were supported by NIH DK019038 and Stanford GCEP.

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Accepted Version - nihms-375939.pdf

Supplemental Material - ja302190r_si_001.pdf

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