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1. Tuning reduction potentials of type 1 copper center in azurin by replacing a histidine ligand with its isostructural analogues

2. The Important Role of Covalent Anchor Positions in Tuning Catalytic Properties of a Rationally Designed MnSalen-Containing Metalloenzyme

3. Noncovalent Modulation of pH-Dependent Reactivity of a Mn-Salen Cofactor in Myoglobin with Hydrogen Peroxide

4. Experimental evidence for a link among cupredoxins: Red, blue, and purple copper transformations in nitrous oxide reductase

5. Perturbations to the Geometric and Electronic Structure of the CuA Site: Factors that Influence Delocalization and Their Contributions to Electron Transfer

6. Reduction Potential Tuning of the Blue Copper Center in Pseudomonas aeruginosa Azurin by the Axial Methionine as Probed by Unnatural Amino Acids

7. Rationally tuning the reduction potential of a single cupredoxin beyond the natural range

8. Artificial Metalloproteins: Design and Engineering

9. Protein scaffold of a designed metalloenzyme enhances the chemoselectivity in sulfoxidation of thioanisole

10. A site-selective dual anchoring strategy for artificial metalloprotein design

11. Mononuclear nitrogen/sulfur-ligated zinc methoxide and hydroxide complexes: investigating ligand effects on the hydrolytic stability of zinc alkoxide species

12. Synthesis and characterization of mononuclear zinc aryloxide complexes supported by nitrogen/sulfur ligands possessing an internal hydrogen bond donor

13. Catalytic Reduction of NO to N2O by a Designed Heme Copper Center in Myoglobin: Implications for the Role of Metal Ions

14. Protein scaffold of a designed metalloenzyme enhances the chemoselectivity in sulfoxidation of thioanisole.

15. A temperature independent pH (TIP) buffer for biomedical biophysical applications at low temperatures.

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