Abstract

The project focuses on the mechanisms of action of enzymes called hydrogenases, of which there are two, [NiFe]- and the [FeFe]-hydrogenases, reflecting the metals at the active sites. These enzymes, which underpin H2-dependent metabolism of many pathogens in the human gut, act on two substrates protons (H+) and H2. Several related families of enzymes are known. The results are further relevant to fundamental catalyst technology. The work aims to clarify the structure and reactivity of the Ni-C, Ni-SI, Ni-R and Ni-L states of the [NiFe]-hydrogenases and the Hred state of the [FeFe]-hydrogenases. Special attention is directed at the location and behavior H2-derived substrates that are usually invisible to protein spectroscopy and are undetectable by protein crystallography. The active sites of these enzymes are highly unusual, featuring several distinctive cofactors, such as CO, cyanide, and, in the [FeFe] case, an aminodithiolate. The work employs the tools of organometallic chemistry to produce models (replicas) of the active sites. Molecular-level insights into behavior of the hydrogenic ligands will be examined by NMR spectroscopy and X-ray crystallography with attention to stereochemistry, redox potentials, acid-base behavior, and kinetic properties. The first theme examines methods for stabilizing nickelIII, characteristic of N-C state, using organometallic ligands that emulate the donor properties of thiolate ligands. The second theme examines the role of the cyanide cofactors bound to Fe, with attention to developing tools to modify the behavior of these groups.
This aim builds on preliminary evidence that boron reagents enable biomimetic activation of hydrogen in iron cyanides. The third theme, with a primary focus on the [FeFe] enzymes, elucidates the factors that lead to bidirectionality, the ability of models to both produce and oxidized H2. The last theme, which also emphasizes [FeFe]-hydrogenase, examines hypotheses that seek to explain the unusual structure-function of the reduced state of the enzyme. This theme will lead to new ligand scaffolds that stabilize terminal hydride ligands.

Public Health Relevance

Hydrogen is a metabolic substrate and product for both pathogenic and beneficial members of human gut flora. This metabolism is mediated by hydrogenase enzymes. Through the work proposed herein we will elucidate the function of these enzymes on a molecular level, with emphasis on interactions involving iron and hydrogen.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM061153-14
Application #
8894517
Study Section
Macromolecular Structure and Function A Study Section (MSFA)
Program Officer
Anderson, Vernon
Project Start
2000-07-01
Project End
2018-04-30
Budget Start
2015-05-01
Budget End
2016-04-30
Support Year
14
Fiscal Year
2015
Total Cost
Indirect Cost

  Institution

Name
University of Illinois Urbana-Champaign
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820

  Publications

Li, Qianli; Lalaoui, Noémie; Woods, Toby J et al. (2018) Electron-Rich, Diiron Bis(monothiolato) Carbonyls: C-S Bond Homolysis in a Mixed Valence Diiron Dithiolate. Inorg Chem 57:4409-4418
Sommer, Constanze; Richers, Casseday P; Lubitz, Wolfgang et al. (2018) A [RuRu] Analogue of an [FeFe]-Hydrogenase Traps the Key Hydride Intermediate of the Catalytic Cycle. Angew Chem Int Ed Engl 57:5429-5432
Carlson, Michaela R; Gray, Danielle L; Richers, Casseday P et al. (2018) Sterically Stabilized Terminal Hydride of a Diiron Dithiolate. Inorg Chem 57:1988-2001
Pelmenschikov, Vladimir; Birrell, James A; Pham, Cindy C et al. (2017) Reaction Coordinate Leading to H2 Production in [FeFe]-Hydrogenase Identified by Nuclear Resonance Vibrational Spectroscopy and Density Functional Theory. J Am Chem Soc 139:16894-16902
Lalaoui, Noémie; Woods, Toby; Rauchfuss, Thomas B et al. (2017) Characterization of a Borane ? Complex of a Diiron Dithiolate: Model for an Elusive Dihydrogen Adduct. Organometallics 36:2054-2057
Yu, Xin; Tung, Chen-Ho; Wang, Wenguang et al. (2017) Interplay between Terminal and Bridging Diiron Hydrides in Neutral and Oxidized States. Organometallics 36:2245-2253
Schilter, David; Gray, Danielle L; Fuller, Amy L et al. (2017) Synthetic Models for Nickel-Iron Hydrogenase Featuring Redox-Active Ligands. Aust J Chem 70:505-515
Reijerse, Edward J; Pham, Cindy C; Pelmenschikov, Vladimir et al. (2017) Direct Observation of an Iron-Bound Terminal Hydride in [FeFe]-Hydrogenase by Nuclear Resonance Vibrational Spectroscopy. J Am Chem Soc 139:4306-4309
Carlson, Michaela R; Gilbert-Wilson, Ryan; Gray, Danielle R et al. (2017) Diiron Dithiolate Hydrides Complemented with Proton-Responsive Phosphine-Amine Ligands. Eur J Inorg Chem 2017:3169-3173
Zhao, Peihua; Gray, Danielle L; Rauchfuss, Thomas B (2016) Rational Synthesis of the Carbonyl(perthiolato)diiron [Fe2(S3CPh2)(CO)6] and Related Complexes. Eur J Inorg Chem 2016:2681-2683

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