Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures

Most components of the cholinergic system are detected in skeletogenic cell types in vitro, yet the function of this system in skeletogenesis remains unclear. Here, we analyzed endochondral ossification in mutant murine fetuses, in which genes of the rate-limiting cholinergic enzymes acetyl- (AChE),...

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Autores principales: Spieker, Janine, Mudersbach, Thomas, Vogel-Höpker, Astrid, Layer, Paul G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5261733/
https://www.ncbi.nlm.nih.gov/pubmed/28118357
http://dx.doi.org/10.1371/journal.pone.0170252
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author Spieker, Janine
Mudersbach, Thomas
Vogel-Höpker, Astrid
Layer, Paul G.
author_facet Spieker, Janine
Mudersbach, Thomas
Vogel-Höpker, Astrid
Layer, Paul G.
author_sort Spieker, Janine
collection PubMed
description Most components of the cholinergic system are detected in skeletogenic cell types in vitro, yet the function of this system in skeletogenesis remains unclear. Here, we analyzed endochondral ossification in mutant murine fetuses, in which genes of the rate-limiting cholinergic enzymes acetyl- (AChE), or butyrylcholinesterase (BChE), or both were deleted (called here A(-)B(+), A(+)B(-), A(-)B(-), respectively). In all mutant embryos bone growth and cartilage remodeling into mineralizing bone were accelerated, as revealed by Alcian blue (A-blu) and Alizarin red (A-red) staining. In A(+)B(-) and A(-)B(-) onset of mineralization was observed before E13.5, about 2 days earlier than in wild type and A(-)B(+) mice. In all mutants between E18.5 to birth A-blu staining disappeared from epiphyses prematurely. Instead, A-blu(+) cells were dislocated into diaphyses, most pronounced so in A(-)B(-) mutants, indicating additive effects of both missing ChEs in A(-)B(-) mutant mice. The remodeling effects were supported by in situ hybridization (ISH) experiments performed on cryosections from A(-)B(-) mice, in which Ihh, Runx2, MMP-13, ALP, Col-II and Col-X were considerably decreased, or had disappeared between E18.5 and P0. With a second approach, we applied an improved in vitro micromass model from chicken limb buds that allowed histological distinction between areas of cartilage, apoptosis and mineralization. When treated with the AChE inhibitor BW284c51, or with nicotine, there was decrease in cartilage and accelerated mineralization, suggesting that these effects were mediated through nicotinic receptors (α7-nAChR). We conclude that due to absence of either one or both cholinesterases in KO mice, or inhibition of AChE in chicken micromass cultures, there is increase in cholinergic signalling, which leads to increased chondroblast production and premature mineralization, at the expense of incomplete chondrogenic differentiation. This emphasizes the importance of cholinergic signalling in cartilage and bone formation.
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spelling pubmed-52617332017-02-17 Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures Spieker, Janine Mudersbach, Thomas Vogel-Höpker, Astrid Layer, Paul G. PLoS One Research Article Most components of the cholinergic system are detected in skeletogenic cell types in vitro, yet the function of this system in skeletogenesis remains unclear. Here, we analyzed endochondral ossification in mutant murine fetuses, in which genes of the rate-limiting cholinergic enzymes acetyl- (AChE), or butyrylcholinesterase (BChE), or both were deleted (called here A(-)B(+), A(+)B(-), A(-)B(-), respectively). In all mutant embryos bone growth and cartilage remodeling into mineralizing bone were accelerated, as revealed by Alcian blue (A-blu) and Alizarin red (A-red) staining. In A(+)B(-) and A(-)B(-) onset of mineralization was observed before E13.5, about 2 days earlier than in wild type and A(-)B(+) mice. In all mutants between E18.5 to birth A-blu staining disappeared from epiphyses prematurely. Instead, A-blu(+) cells were dislocated into diaphyses, most pronounced so in A(-)B(-) mutants, indicating additive effects of both missing ChEs in A(-)B(-) mutant mice. The remodeling effects were supported by in situ hybridization (ISH) experiments performed on cryosections from A(-)B(-) mice, in which Ihh, Runx2, MMP-13, ALP, Col-II and Col-X were considerably decreased, or had disappeared between E18.5 and P0. With a second approach, we applied an improved in vitro micromass model from chicken limb buds that allowed histological distinction between areas of cartilage, apoptosis and mineralization. When treated with the AChE inhibitor BW284c51, or with nicotine, there was decrease in cartilage and accelerated mineralization, suggesting that these effects were mediated through nicotinic receptors (α7-nAChR). We conclude that due to absence of either one or both cholinesterases in KO mice, or inhibition of AChE in chicken micromass cultures, there is increase in cholinergic signalling, which leads to increased chondroblast production and premature mineralization, at the expense of incomplete chondrogenic differentiation. This emphasizes the importance of cholinergic signalling in cartilage and bone formation. Public Library of Science 2017-01-24 /pmc/articles/PMC5261733/ /pubmed/28118357 http://dx.doi.org/10.1371/journal.pone.0170252 Text en © 2017 Spieker et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Spieker, Janine
Mudersbach, Thomas
Vogel-Höpker, Astrid
Layer, Paul G.
Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title_full Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title_fullStr Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title_full_unstemmed Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title_short Endochondral Ossification Is Accelerated in Cholinesterase-Deficient Mice and in Avian Mesenchymal Micromass Cultures
title_sort endochondral ossification is accelerated in cholinesterase-deficient mice and in avian mesenchymal micromass cultures
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5261733/
https://www.ncbi.nlm.nih.gov/pubmed/28118357
http://dx.doi.org/10.1371/journal.pone.0170252
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AT vogelhopkerastrid endochondralossificationisacceleratedincholinesterasedeficientmiceandinavianmesenchymalmicromasscultures
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