4.4 Article

Spatially and temporally controlled biomineralization is facilitated by interaction between self-assembled dentin matrix protein 1 and calcium phosphate nuclei in solution

Journal

BIOCHEMISTRY
Volume 44, Issue 49, Pages 16140-16148

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/bi051045l

Keywords

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Funding

  1. NIDCR NIH HHS [DE 11657, DE 13836, R01 DE013836, R01 DE011657-11, R56 DE011657, R01 DE011657] Funding Source: Medline

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Bone and dentin biomineralization are well-regulated processes mediated by extracellular matrix proteins. it is widely believed that specific matrix proteins in these tissues modulate nucleation of apatite nanoparticles and their growth into micrometer-sized crystals via molecular recognition at the proteinmineral interface. However, this assumption has been supported only circumstantially, and the exact mechanism remains unknown. Dentin matrix protein I (DMPl) is an acidic matrix protein, present in the mineralized matrix of bone and dentin. In this study, we have demonstrated using synchrotron smallangle X-ray scattering that DMPI in solution can undergo oligornerization and temporarily stabilize the newly formed calcium phosphate nanoparticle precursors by sequestering them and preventing their further aggregation and precipitation. The solution structure represents the first low-resolution structural information for DMPl. Atomic force microscopy and transmission electron microscopy studies further confirmed that the nascent calcium phosphate nuclei formed in solution were assembled into ordered protein-mineral complexes with the aid of oligomerized DMP1, recombinant and native. This study reveals a novel mechanism by which DMP1 might facilitate initiation of mineral nucleation at specific sites during bone and dentin mineralization and prevent spontaneous calcium phosphate precipitation in areas in which mineralization is not desirable.

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