Literature DB >> 32224162

Genetic and pharmacologic modulation of cementogenesis via pyrophosphate regulators.

E Y Chu1, T D Vo2, M B Chavez3, A Nagasaki2, E L Mertz4, F H Nociti5, S F Aitken2, D Kavanagh6, K Zimmerman6, X Li6, P R Stabach6, D T Braddock6, J L Millán7, B L Foster3, M J Somerman2.   

Abstract

Pyrophosphate (PPi) serves as a potent and physiologically important regulator of mineralization, with systemic and local concentrations determined by several key regulators, including: tissue-nonspecific alkaline phosphatase (ALPL gene; TNAP protein), the progressive ankylosis protein (ANKH; ANK), and ectonucleotide pyrophosphatase/phosphodiesterase 1 (ENPP1; ENPP1). Results to date have indicated important roles for PPi in cementum formation, and we addressed several gaps in knowledge by employing genetically edited mouse models where PPi metabolism was disrupted and pharmacologically modulating PPi in a PPi-deficient mouse model. We demonstrate that acellular cementum growth is inversely proportional to PPi levels, with reduced cementum in Alpl KO (increased PPi levels) mice and excess cementum in Ank KO mice (decreased PPi levels). Moreover, simultaneous ablation of Alpl and Ank results in reestablishment of functional cementum in dKO mice. Additional reduction of PPi by dual deletion of Ank and Enpp1 does not further increase cementogenesis, and PDL space is maintained in part through bone modeling/remodeling by osteoclasts. Our results provide insights into cementum formation and expand our knowledge of how PPi regulates cementum. We also demonstrate for the first time that pharmacologic manipulation of PPi through an ENPP1-Fc fusion protein can regulate cementum growth, supporting therapeutic interventions targeting PPi metabolism. Published by Elsevier Inc.

Entities:  

Keywords:  Bone; Cementum; Mineralized tissue/development; Tooth development

Mesh:

Substances:

Year:  2020        PMID: 32224162      PMCID: PMC7482720          DOI: 10.1016/j.bone.2020.115329

Source DB:  PubMed          Journal:  Bone        ISSN: 1873-2763            Impact factor:   4.398


  43 in total

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4.  Mineralization defects in cementum and craniofacial bone from loss of bone sialoprotein.

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Journal:  Bone       Date:  2015-05-09       Impact factor: 4.398

5.  Hypophosphatasia: Natural history study of 101 affected children investigated at one research center.

Authors:  Michael P Whyte; Deborah Wenkert; Fan Zhang
Journal:  Bone       Date:  2016-08-27       Impact factor: 4.398

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Authors:  Ronald A Albright; Paul Stabach; Wenxiang Cao; Dillon Kavanagh; Isabelle Mullen; Alexander A Braddock; Mariel S Covo; Martin Tehan; Guangxiao Yang; Zhiliang Cheng; Keith Bouchard; Zhao-Xue Yu; Stephanie Thorn; Xiangning Wang; Ewa J Folta-Stogniew; Alejandro Negrete; Albert J Sinusas; Joseph Shiloach; George Zubal; Joseph A Madri; Enrique M De La Cruz; Demetrios T Braddock
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10.  Orodental phenotype and genotype findings in all subtypes of hypophosphatasia.

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2.  Insights into dental mineralization from three heritable mineralization disorders.

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Review 3.  Guidelines for Micro-Computed Tomography Analysis of Rodent Dentoalveolar Tissues.

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4.  Delivery of Alkaline Phosphatase Promotes Periodontal Regeneration in Mice.

Authors:  A Nagasaki; K Nagasaki; B D Kear; W D Tadesse; V Thumbigere-Math; J L Millán; B L Foster; M J Somerman
Journal:  J Dent Res       Date:  2021-04-10       Impact factor: 8.924

5.  Ablation of Pyrophosphate Regulators Promotes Periodontal Regeneration.

Authors:  A Nagasaki; K Nagasaki; E Y Chu; B D Kear; W D Tadesse; S E Ferebee; L Li; B L Foster; M J Somerman
Journal:  J Dent Res       Date:  2020-12-24       Impact factor: 8.924

Review 6.  Tissue-Nonspecific Alkaline Phosphatase-A Gatekeeper of Physiological Conditions in Health and a Modulator of Biological Environments in Disease.

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  7 in total

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