Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche

Two decades after signals controlling bone length were discovered, the endogenous ligands determining bone width remain unknown. We show that postnatal establishment of normal bone width in mice, as mediated by bone-forming activity of the periosteum, requires BMP signaling at the innermost layer of...

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Autores principales: Salazar, Valerie S, Capelo, Luciane P, Cantù, Claudio, Zimmerli, Dario, Gosalia, Nehal, Pregizer, Steven, Cox, Karen, Ohte, Satoshi, Feigenson, Marina, Gamer, Laura, Nyman, Jeffry S, Carey, David J, Economides, Aris, Basler, Konrad, Rosen, Vicki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2019
Materias:
Cell Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6386520/
https://www.ncbi.nlm.nih.gov/pubmed/30735122
http://dx.doi.org/10.7554/eLife.42386
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author Salazar, Valerie S
Capelo, Luciane P
Cantù, Claudio
Zimmerli, Dario
Gosalia, Nehal
Pregizer, Steven
Cox, Karen
Ohte, Satoshi
Feigenson, Marina
Gamer, Laura
Nyman, Jeffry S
Carey, David J
Economides, Aris
Basler, Konrad
Rosen, Vicki
author_facet Salazar, Valerie S
Capelo, Luciane P
Cantù, Claudio
Zimmerli, Dario
Gosalia, Nehal
Pregizer, Steven
Cox, Karen
Ohte, Satoshi
Feigenson, Marina
Gamer, Laura
Nyman, Jeffry S
Carey, David J
Economides, Aris
Basler, Konrad
Rosen, Vicki
author_sort Salazar, Valerie S
collection PubMed
description Two decades after signals controlling bone length were discovered, the endogenous ligands determining bone width remain unknown. We show that postnatal establishment of normal bone width in mice, as mediated by bone-forming activity of the periosteum, requires BMP signaling at the innermost layer of the periosteal niche. This developmental signaling center becomes quiescent during adult life. Its reactivation however, is necessary for periosteal growth, enhanced bone strength, and accelerated fracture repair in response to bone-anabolic therapies used in clinical orthopedic settings. Although many BMPs are expressed in bone, periosteal BMP signaling and bone formation require only Bmp2 in the Prx1-Cre lineage. Mechanistically, BMP2 functions downstream of Lrp5/6 pathway to activate a conserved regulatory element upstream of Sp7 via recruitment of Smad1 and Grhl3. Consistent with our findings, human variants of BMP2 and GRHL3 are associated with increased risk of fractures.
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spelling pubmed-63865202019-02-25 Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche Salazar, Valerie S Capelo, Luciane P Cantù, Claudio Zimmerli, Dario Gosalia, Nehal Pregizer, Steven Cox, Karen Ohte, Satoshi Feigenson, Marina Gamer, Laura Nyman, Jeffry S Carey, David J Economides, Aris Basler, Konrad Rosen, Vicki eLife Cell Biology Two decades after signals controlling bone length were discovered, the endogenous ligands determining bone width remain unknown. We show that postnatal establishment of normal bone width in mice, as mediated by bone-forming activity of the periosteum, requires BMP signaling at the innermost layer of the periosteal niche. This developmental signaling center becomes quiescent during adult life. Its reactivation however, is necessary for periosteal growth, enhanced bone strength, and accelerated fracture repair in response to bone-anabolic therapies used in clinical orthopedic settings. Although many BMPs are expressed in bone, periosteal BMP signaling and bone formation require only Bmp2 in the Prx1-Cre lineage. Mechanistically, BMP2 functions downstream of Lrp5/6 pathway to activate a conserved regulatory element upstream of Sp7 via recruitment of Smad1 and Grhl3. Consistent with our findings, human variants of BMP2 and GRHL3 are associated with increased risk of fractures. eLife Sciences Publications, Ltd 2019-02-08 /pmc/articles/PMC6386520/ /pubmed/30735122 http://dx.doi.org/10.7554/eLife.42386 Text en © 2019, Salazar et al http://creativecommons.org/licenses/by/4.0/ http://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Cell Biology
Salazar, Valerie S
Capelo, Luciane P
Cantù, Claudio
Zimmerli, Dario
Gosalia, Nehal
Pregizer, Steven
Cox, Karen
Ohte, Satoshi
Feigenson, Marina
Gamer, Laura
Nyman, Jeffry S
Carey, David J
Economides, Aris
Basler, Konrad
Rosen, Vicki
Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title_full Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title_fullStr Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title_full_unstemmed Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title_short Reactivation of a developmental Bmp2 signaling center is required for therapeutic control of the murine periosteal niche
title_sort reactivation of a developmental bmp2 signaling center is required for therapeutic control of the murine periosteal niche
topic Cell Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6386520/
https://www.ncbi.nlm.nih.gov/pubmed/30735122
http://dx.doi.org/10.7554/eLife.42386
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