Abstract

The experimental approaches to, and application of, NMR spectroscopy of particularly paramagnetic derivatives of O2 binding myoglobin and hemoglobin will be explored and expanded to elucidate electronic and molecular structural control mechanisms of their ligation and autoxidizability. The ultimate aim is to understand the molecular mechanism of oxygen binding so as to aid in the design of genetically engineered hemoglobin as a blood substitute and to understand the pathological properties of natural mutant hemoglobins. The program continues to develop effective methods for definitive assignments and molecular structural determination of the heme cavity, and will emphasize the development of robust bases for interpreting hyperfine shifts for each of the globin oxidation/spin states in terms of functionally relevant structural determinants. This latter goal will rely on detailed studies on a series of diverse, structurally characterized reference globins, a series of point mutants of these reference globin designed to perturb selected structurally/dynamic properties of the active site, as well as both reference and point mutated globins reconstituted with modified hemes designed to separate the rhombic influences of the vinyls from that characteristic of the globin cavity. The hyperfine shifts in cyanomet globins will be interpreted in terms of the axial His orientation, the His-Fe bond strength as well as distal residue hydrogen bonding to, and steric interaction with, the bound ligand. The correlation between globin induced changes in hyperfine shift and axial His orientation in metglobins will be established, probes to quantitate partial water ligation perfected, and the thermodynamics and dynamics of such water ligation characterized. The nature of the distal interactions that determine the unusual orientation of the major magnetic axis in deoxy globins, as well as the correlation between heme contact shift pattern and both His orientation and the presence of non-ligated distal water will be established. The developed approaches will be used to resolve differences in the solution versus crystal orientation of the distal His in Chironomus Hb, structurally characterize equilibrium intermediates in the thermal denaturation of Aplysia Mb, characterize the sequence alignment, folding topology and identify distal residues in a series of """"""""mini"""""""" or """"""""compact"""""""" (109-118 residue) globins, characterize the distal H- bonding network in the extremely O2-avid, and on occasion, extremely autoxidative-resistant, trematode globins, and characterize the changes in distal interactions and proximal His-Fe bond strain that accompanies the allosteric transition in ligated HbA.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL016087-28
Application #
6329999
Study Section
Metallobiochemistry Study Section (BMT)
Program Officer
Thomas, John
Project Start
1976-12-01
Project End
2005-02-28
Budget Start
2001-03-01
Budget End
2002-02-28
Support Year
28
Fiscal Year
2001
Total Cost
$301,970
Indirect Cost

  Institution

Name
University of California Davis
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
094878337
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Ma, Li-Hua; Liu, Yangzhong; Zhang, Xuhong et al. (2009) 1H NMR study of the effect of variable ligand on heme oxygenase electronic and molecular structure. J Inorg Biochem 103:10-9
La Mar, Gerd N (2007) Application of the paramagnetic dipole field for solution NMR active site structure determination in low-spin, cyanide-inhibited ferric hemoproteins. IUBMB Life 59:513-27
Bondarenko, Vasyl; Dewilde, Sylvia; Moens, Luc et al. (2006) Solution 1H NMR characterization of the axial bonding of the two His in oxidized human cytoglobin. J Am Chem Soc 128:12988-99
Xia, Zhicheng; Nguyen, Bao D; Brunori, Maurizio et al. (2005) 1H-NMR study of the effect of temperature through reversible unfolding on the heme pocket molecular structure and magnetic properties of aplysia limacina cyano-metmyoglobin. Biophys J 89:4149-58
Bondarenko, Vasyl; Wang, Jingtao; Kalish, Heather et al. (2005) Solution 1H NMR study of the accommodation of the side chain of n-butyl-etiohemin-I incorporated into the active site of cyano-metmyoglobin. J Biol Inorg Chem 10:283-93
Tran, Anh-Tuyet T; Kolczak, Urszula; La Mar, Gerd N (2004) Solution 1H NMR study of the active site molecular structure and magnetic properties of the cyanomet complex of the isolated, tetrameric beta-chain from human adult hemoglobin. Biochim Biophys Acta 1701:75-87
Du, Weihong; Xia, Zhicheng; Dewilde, Sylvia et al. (2003) 1H NMR study of the molecular structure and magnetic properties of the active site for the cyanomet complex of O2-avid hemoglobin from the trematode Paramphistomum epiclitum. Eur J Biochem 270:2707-20
Ma, Dejian; Musto, Raffaella; Smith, Kevin M et al. (2003) Solution NMR characterization of the electronic structure and magnetic properties of high-spin ferrous heme in deoxy myoglobin from Aplysia limacina. J Am Chem Soc 125:8494-504
Tran, Anh-Tuyet T; Kolczak, Urszula; La Mar, Gerd N (2003) Solution 1H NMR study of the active site molecular structure and magnetic properties of the cyanomet complex of the isolated alpha-chain from human hemoglobin A. Biochim Biophys Acta 1650:59-72
Du, Weihong; Syvitski, Ray; Dewilde, Sylvia et al. (2003) Solution 1h NMR characterization of equilibrium heme orientational disorder with functional consequences in mouse neuroglobin. J Am Chem Soc 125:8080-1

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