Abstract

The purpose of this project is to determine the structure-function relationship of enamel matrix proteins as potential regulators of enamel mineral formation. Our working hypothesis is that soluble hydrophilic enamel proteins (e.g. enamelin) in association with insoluble matrix components (e.g. amelogenin aggregates) provide the appropriate surface characteristics to induce the nucleation of calcium phosphates. In the presence of appropriate concentrations of mineral ions, this results in the formation of very thin ribbons of enamel mineral. The growth of these enamel ribbons in thickness and width is immediately inhibited by hydrophobic proteins (e.g. amelogenins in solution) which absorb onto specific faces of the forming crystals. It is further hypothesized that the onset of growth of these mineral ribbons during tissue maturation is controlled by the degradation of these absorbed protein inhibitors by enamel proteinases. To gain a better understanding how matrix proteins can control mineralization in a tissue like enamel, we gain a better understanding how matrix proteins can control mineralization in a tissue like enamel, we proposed to determine the adsorption isotherms for the major enamel matrix proteins onto hydroxyapatite (HA) and octacalcium phosphate (OCP) crystals, using recombinant amelogenin and enamelin. HA and OCP were chosen for study as prototypes for forming enamel mineral. We further propose to determine the inhibitory effect of adsorbed recombinant amelogenin and enamelin on HA seeded crystal growth and relate these findings to the extent of protein adsorption. We will further assess the ability of recombinant enamel proteinases (e.g. enameylsin and EMPSl) to degrade enamel proteins which are absorbed onto HA and OCP surfaces, since this may be an important mechanism by which enamel proteinases can control mineralization. We further propose to assess the ability of recombinant amelogenin and enamelin to promote calcium phosphate nucleation in vitro, using agarose gels and proteins covalently linked to sepharose beads, and to influence crystal morphology. Long term, these studies may be important to the development of new biomimetic approaches which could be used to treat damaged or diseased teeth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Program Projects (P01)
Project #
5P01DE013237-04
Application #
6656477
Study Section
Project Start
2002-08-01
Project End
2003-07-31
Budget Start
Budget End
Support Year
4
Fiscal Year
2002
Total Cost
$132,152
Indirect Cost

  Institution

Name
Forsyth Institute
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02142

  Publications

Hermo, Louis; Chung, Shari; Gregory, Mary et al. (2008) Alterations in the testis of hormone sensitive lipase-deficient mice is associated with decreased sperm counts, sperm motility, and fertility. Mol Reprod Dev 75:565-77
Primiani, Nadia; Gregory, Mary; Dufresne, Julie et al. (2007) Microvillar size and espin expression in principal cells of the adult rat epididymis are regulated by androgens. J Androl 28:659-69
Hermo, Louis; Korah, Nadine; Gregory, Mary et al. (2007) Structural alterations of epididymal epithelial cells in cathepsin A-deficient mice affect the blood-epididymal barrier and lead to altered sperm motility. J Androl 28:784-97
Khatchadourian, Karine; Smith, Charles E; Metzler, Martina et al. (2007) Structural abnormalities in spermatids together with reduced sperm counts and motility underlie the reproductive defect in HIP1-/- mice. Mol Reprod Dev 74:341-59
Margolis, H C; Beniash, E; Fowler, C E (2006) Role of macromolecular assembly of enamel matrix proteins in enamel formation. J Dent Res 85:775-93
Turk, Benjamin E; Lee, Daniel H; Yamakoshi, Yasuo et al. (2006) MMP-20 is predominately a tooth-specific enzyme with a deep catalytic pocket that hydrolyzes type V collagen. Biochemistry 45:3863-74
Smith, Charles E; Nanci, Antonio; Moffatt, Pierre (2006) Evidence by signal peptide trap technology for the expression of carbonic anhydrase 6 in rat incisor enamel organs. Eur J Oral Sci 114 Suppl 1:147-53; discussion 164-5, 380-1
Fowler, Christabel E; Beniash, Elia; Yamakoshi, Yasuo et al. (2006) Co-operative mineralization and protein self-assembly in amelogenesis: silica mineralization and assembly of recombinant amelogenins in vitro. Eur J Oral Sci 114 Suppl 1:297-303; discussion 327-9, 382
Ruz, Ricardo; Gregory, Mary; Smith, Charles E et al. (2006) Expression of aquaporins in the efferent ductules, sperm counts, and sperm motility in estrogen receptor-alpha deficient mice fed lab chow versus casein. Mol Reprod Dev 73:226-37
Bartlett, J D; Dwyer, S E; Beniash, E et al. (2005) Fluorosis: a new model and new insights. J Dent Res 84:832-6

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