Abstract

Acidic proteins found in mineralized tissue act as biology's crystal engineers. Their activities are responsible for the material properties of hard tissues, and their activities directly control the hierarchical architecture of these tissues. However, despite their importance in such fundamental physiological processes as bone and tooth formation, there is remarkably little known of the protein structure-function relationships which govern crystal recognition. The primary goal of this program is to obtain a molecular description of the structure-function relationships used by small acidic proteins in the crystal engineering of hydroxyapatite and calcium oxalate (the principle mineral phases of bone/teeth and kidney stones, respectively). Preliminary genetic engineering results with a small model protein, consisting structurally of a long alpha-helix and two antiparallel beta-sheets, have demonstrated that the protein surface electrostatic charge distribution can directly dictate whether secondary nucleation and crystal growth is promoted or inhibited. The molecular recognition mechanisms underlying this observation will be studied with a combination of kinetic and thermodynamic techniques, along with direct solid-state NMR determination of the protein-crystal interfacial structure. Further studies will characterize how secondary structure scaffolds are used to present carboxylate side-chains with stereospecificities that direct interactions with hydroxyapatite and calcium oxalate. Genetic engineering techniques will be used to systematically place carboxylate side-chains on the alpha-helix and anti- parallel beta-sheets, and the subsequent molecular interactions with the crystals will again be studied with solid-state NMR techniques. In addition, the functional properties of these proteins will be assessed using a variety of techniques including constant composition kinetics, direct binding adsorption analysis, particle size determination, electron microscopy, and zeta-potential measurements. The disruption of normal biomineralization processes can lead to pathological mineralization or demineralization, such as in atherosclerotic plaque formation, artificial heart valve calcification, kidney stone build-up, dental calculus formation, or bone and tooth demineralization. A better understanding of the biomolecular mechanisms used to promote or retard crystal growth could provide important design principles for the development of calcification inhibitors and promoters in orthopaedics, cardiology and dentistry.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE012554-04
Application #
6176646
Study Section
Biophysical Chemistry Study Section (BBCB)
Program Officer
Drummond, James
Project Start
1997-09-30
Project End
2002-07-31
Budget Start
2000-08-01
Budget End
2001-07-31
Support Year
4
Fiscal Year
2000
Total Cost
$429,031
Indirect Cost

  Institution

Name
University of Washington
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Scudeller, Luisa A; Srinivasan, Selvi; Rossi, Alexandre M et al. (2017) Orientation and conformation of osteocalcin adsorbed onto calcium phosphate and silica surfaces. Biointerphases 12:02D411
Roehrich, Adrienne; Drobny, Gary (2013) Solid-state NMR studies of biomineralization peptides and proteins. Acc Chem Res 46:2136-44
Weidner, Tobias; Castner, David G (2013) SFG analysis of surface bound proteins: a route towards structure determination. Phys Chem Chem Phys 15:12516-24
Weidner, Tobias; Dubey, Manish; Breen, Nicholas F et al. (2012) Direct observation of phenylalanine orientations in statherin bound to hydroxyapatite surfaces. J Am Chem Soc 134:8750-3
Breen, Nicholas F; Li, Kun; Olsen, Gregory L et al. (2011) Deuterium magic angle spinning NMR used to study the dynamics of peptides adsorbed onto polystyrene and functionalized polystyrene surfaces. J Phys Chem B 115:9452-60
Ndao, Moise; Ash, Jason T; Stayton, Patrick S et al. (2010) The Role of Basic Amino Acids in the Molecular Recognition of Hydroxyapatite by Statherin using Solid State NMR. Surf Sci 604:L39-L42
Weidner, Tobias; Breen, Nicholas F; Li, Kun et al. (2010) Sum frequency generation and solid-state NMR study of the structure, orientation, and dynamics of polystyrene-adsorbed peptides. Proc Natl Acad Sci U S A 107:13288-93
Masica, David L; Ash, Jason T; Ndao, Moise et al. (2010) Toward a structure determination method for biomineral-associated protein using combined solid- state NMR and computational structure prediction. Structure 18:1678-87
Breen, Nicholas F; Weidner, Tobias; Li, Kun et al. (2009) A solid-state deuterium NMR and sum-frequency generation study of the side-chain dynamics of peptides adsorbed onto surfaces. J Am Chem Soc 131:14148-9
Ndao, Moise; Ash, Jason T; Breen, Nicholas F et al. (2009) A (13)C{(31)P} REDOR NMR investigation of the role of glutamic acid residues in statherin- hydroxyapatite recognition. Langmuir 25:12136-43

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