Literature DB >> 20018657

A role for suppressed incisor cuspal morphogenesis in the evolution of mammalian heterodont dentition.

Atsushi Ohazama1, James Blackburn, Thantrira Porntaveetus, Masato S Ota, Hong Y Choi, Eric B Johnson, Philip Myers, Shelly Oommen, Kazuhiro Eto, John A Kessler, Takashi Kondo, Gareth J Fraser, J Todd Streelman, Ulyses F J Pardiñas, Abigail S Tucker, Pablo E Ortiz, Cyril Charles, Laurent Viriot, Joachim Herz, Paul T Sharpe.   

Abstract

Changes in tooth shape have played a major role in vertebrate evolution with modification of dentition allowing an organism to adapt to new feeding strategies. The current view is that molar teeth evolved from simple conical teeth, similar to canines, by progressive addition of extra "cones" to form progressively complex multicuspid crowns. Mammalian incisors, however, are neither conical nor multicuspid, and their evolution is unclear. We show that hypomorphic mutation of a cell surface receptor, Lrp4, which modulates multiple signaling pathways, produces incisors with grooved enamel surfaces that exhibit the same molecular characteristics as the tips of molar cusps. Mice with a null mutation of Lrp4 develop extra cusps on molars and have incisors that exhibit clear molar-like cusp and root morphologies. Molecular analysis identifies misregulation of Shh and Bmp signaling in the mutant incisors and suggests an uncoupling of the processes of tooth shape determination and morphogenesis. Incisors thus possess a developmentally suppressed, cuspid crown-like morphogenesis program similar to that in molars that is revealed by loss of Lrp4 activity. Several mammalian species naturally possess multicuspid incisors, suggesting that mammals have the capacity to form multicuspid teeth regardless of location in the oral jaw. Localized loss of enamel may thus have been an intermediary step in the evolution of cusps, both of which use Lrp4-mediated signaling.

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Year:  2009        PMID: 20018657      PMCID: PMC2806730          DOI: 10.1073/pnas.0907236107

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  28 in total

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