Barrier Formation

Author:

Lyaruu D.M.1,Medina J.F.2,Sarvide S.2,Bervoets T.J.M.1,Everts V.1,DenBesten P.3,Smith C.E.4,Bronckers A.L.J.J.1

Affiliation:

1. Department of Oral Cell Biology, Academic Centre for Dentistry Amsterdam, University of Amsterdam, and MOVE Research Institute, VU University Amsterdam, Amsterdam, Netherlands

2. Division of Gene Therapy and Hepatology, School of Medicine/CIMA, University of Navarra, and Ciberehd, Pamplona, Spain

3. Department of Oral Sciences, University of California, San Francisco, CA, USA

4. Facility for Electron Microscopy Research, Department of Anatomy and Cell Biology and Faculty of Dentistry, McGill University, Montreal, Canada

Abstract

Enamel fluorosis is an irreversible structural enamel defect following exposure to supraoptimal levels of fluoride during amelogenesis. We hypothesized that fluorosis is associated with excess release of protons during formation of hypermineralized lines in the mineralizing enamel matrix. We tested this concept by analyzing fluorotic enamel defects in wild-type mice and mice deficient in anion exchanger-2a,b ( Ae2a,b), a transmembrane protein in maturation ameloblasts that exchanges extracellular Cl for bicarbonate. Defects were more pronounced in fluorotic Ae2a,b−/− mice than in fluorotic heterozygous or wild-type mice. Phenotypes included a hypermineralized surface, extensive subsurface hypomineralization, and multiple hypermineralized lines in deeper enamel. Mineral content decreased in all fluoride-exposed and Ae2a,b−/− mice and was strongly correlated with Cl. Exposure of enamel surfaces underlying maturation-stage ameloblasts to pH indicator dyes suggested the presence of diffusion barriers in fluorotic enamel. These results support the concept that fluoride stimulates hypermineralization at the mineralization front. This causes increased release of protons, which ameloblasts respond to by secreting more bicarbonates at the expense of Cl levels in enamel. The fluoride-induced hypermineralized lines may form barriers that impede diffusion of proteins and mineral ions into the subsurface layers, thereby delaying biomineralization and causing retention of enamel matrix proteins.

Publisher

SAGE Publications

Subject

General Dentistry

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