Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth

Regulated growth plate activity is essential for postnatal bone development and body stature, yet the systems regulating epiphyseal fusion are poorly understood. Here, we show that the tissue inhibitors of metalloprotease (TIMP) gene family is essential for normal bone growth after birth. Whole-body...

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Autores principales: Saw, Sanjay, Aiken, Alison, Fang, Hui, McKee, Trevor D., Bregant, Sarah, Sanchez, Otto, Chen, Yan, Weiss, Ashley, Dickson, Brendan C., Czarny, Bertrand, Sinha, Ankit, Fosang, Amanda, Dive, Vincent, Waterhouse, Paul D., Kislinger, Thomas, Khokha, Rama
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Rockefeller University Press 2019
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6719459/
https://www.ncbi.nlm.nih.gov/pubmed/31371388
http://dx.doi.org/10.1083/jcb.201906059
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author Saw, Sanjay
Aiken, Alison
Fang, Hui
McKee, Trevor D.
Bregant, Sarah
Sanchez, Otto
Chen, Yan
Weiss, Ashley
Dickson, Brendan C.
Czarny, Bertrand
Sinha, Ankit
Fosang, Amanda
Dive, Vincent
Waterhouse, Paul D.
Kislinger, Thomas
Khokha, Rama
author_facet Saw, Sanjay
Aiken, Alison
Fang, Hui
McKee, Trevor D.
Bregant, Sarah
Sanchez, Otto
Chen, Yan
Weiss, Ashley
Dickson, Brendan C.
Czarny, Bertrand
Sinha, Ankit
Fosang, Amanda
Dive, Vincent
Waterhouse, Paul D.
Kislinger, Thomas
Khokha, Rama
author_sort Saw, Sanjay
collection PubMed
description Regulated growth plate activity is essential for postnatal bone development and body stature, yet the systems regulating epiphyseal fusion are poorly understood. Here, we show that the tissue inhibitors of metalloprotease (TIMP) gene family is essential for normal bone growth after birth. Whole-body quadruple-knockout mice lacking all four TIMPs have growth plate closure in long bones, precipitating limb shortening, epiphyseal distortion, and widespread chondrodysplasia. We identify TIMP/FGF-2/IHH as a novel nexus underlying bone lengthening where TIMPs negatively regulate the release of FGF-2 from chondrocytes to allow IHH expression. Using a knock-in approach that combines MMP-resistant or ADAMTS-resistant aggrecans with TIMP deficiency, we uncouple growth plate activity in axial and appendicular bones. Thus, natural metalloprotease inhibitors are crucial regulators of chondrocyte maturation program, growth plate integrity, and skeletal proportionality. Furthermore, individual and combinatorial TIMP-deficient mice demonstrate the redundancy of metalloprotease inhibitor function in embryonic and postnatal development.
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spelling pubmed-67194592019-09-17 Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth Saw, Sanjay Aiken, Alison Fang, Hui McKee, Trevor D. Bregant, Sarah Sanchez, Otto Chen, Yan Weiss, Ashley Dickson, Brendan C. Czarny, Bertrand Sinha, Ankit Fosang, Amanda Dive, Vincent Waterhouse, Paul D. Kislinger, Thomas Khokha, Rama J Cell Biol Research Articles Regulated growth plate activity is essential for postnatal bone development and body stature, yet the systems regulating epiphyseal fusion are poorly understood. Here, we show that the tissue inhibitors of metalloprotease (TIMP) gene family is essential for normal bone growth after birth. Whole-body quadruple-knockout mice lacking all four TIMPs have growth plate closure in long bones, precipitating limb shortening, epiphyseal distortion, and widespread chondrodysplasia. We identify TIMP/FGF-2/IHH as a novel nexus underlying bone lengthening where TIMPs negatively regulate the release of FGF-2 from chondrocytes to allow IHH expression. Using a knock-in approach that combines MMP-resistant or ADAMTS-resistant aggrecans with TIMP deficiency, we uncouple growth plate activity in axial and appendicular bones. Thus, natural metalloprotease inhibitors are crucial regulators of chondrocyte maturation program, growth plate integrity, and skeletal proportionality. Furthermore, individual and combinatorial TIMP-deficient mice demonstrate the redundancy of metalloprotease inhibitor function in embryonic and postnatal development. Rockefeller University Press 2019-09-02 2019-08-01 /pmc/articles/PMC6719459/ /pubmed/31371388 http://dx.doi.org/10.1083/jcb.201906059 Text en © 2019 Saw et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Saw, Sanjay
Aiken, Alison
Fang, Hui
McKee, Trevor D.
Bregant, Sarah
Sanchez, Otto
Chen, Yan
Weiss, Ashley
Dickson, Brendan C.
Czarny, Bertrand
Sinha, Ankit
Fosang, Amanda
Dive, Vincent
Waterhouse, Paul D.
Kislinger, Thomas
Khokha, Rama
Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title_full Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title_fullStr Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title_full_unstemmed Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title_short Metalloprotease inhibitor TIMP proteins control FGF-2 bioavailability and regulate skeletal growth
title_sort metalloprotease inhibitor timp proteins control fgf-2 bioavailability and regulate skeletal growth
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6719459/
https://www.ncbi.nlm.nih.gov/pubmed/31371388
http://dx.doi.org/10.1083/jcb.201906059
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