Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice

Degenerative joint diseases such as osteoarthritis are characterised by aberrant region-specific bone formation and abnormal bone mineral content. A recent study suggested a role for the complement membrane attack complex in experimental models of osteoarthritis. Since CD59a is the principal regulat...

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Autores principales: Bloom, Anja C., Collins, Fraser L., van't Hof, Rob J., Ryan, Elizabeth S., Jones, Emma, Hughes, Timothy R., Morgan, B. Paul, Erlandsson, Malin, Bokarewa, Maria, Aeschlimann, Daniel, Evans, Bronwen A.J., Williams, Anwen S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2016
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Original Full Length Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4764651/
https://www.ncbi.nlm.nih.gov/pubmed/26721735
http://dx.doi.org/10.1016/j.bone.2015.12.014
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author Bloom, Anja C.
Collins, Fraser L.
van't Hof, Rob J.
Ryan, Elizabeth S.
Jones, Emma
Hughes, Timothy R.
Morgan, B. Paul
Erlandsson, Malin
Bokarewa, Maria
Aeschlimann, Daniel
Evans, Bronwen A.J.
Williams, Anwen S.
author_facet Bloom, Anja C.
Collins, Fraser L.
van't Hof, Rob J.
Ryan, Elizabeth S.
Jones, Emma
Hughes, Timothy R.
Morgan, B. Paul
Erlandsson, Malin
Bokarewa, Maria
Aeschlimann, Daniel
Evans, Bronwen A.J.
Williams, Anwen S.
author_sort Bloom, Anja C.
collection PubMed
description Degenerative joint diseases such as osteoarthritis are characterised by aberrant region-specific bone formation and abnormal bone mineral content. A recent study suggested a role for the complement membrane attack complex in experimental models of osteoarthritis. Since CD59a is the principal regulator of the membrane attack complex in mice, we evaluated the impact of CD59a gene deletion upon maintenance of bone architecture. In vivo bone morphology analysis revealed that male CD59a-deficient mice have increased femur length and cortical bone volume, albeit with reduced bone mineral density. However, this phenomenon was not observed in female mice. Histomorphometric analysis of the trabecular bone showed increased rates of bone homeostasis, with both increased bone resorption and mineral apposition rate in CD59a-deficient male mice. When bone cells were studied in isolation, in vitro osteoclastogenesis was significantly increased in male CD59a-deficient mice, although osteoblast formation was not altered. Our data reveal, for the first time, that CD59a is a regulator of bone growth and homeostasis. CD59a ablation in male mice results in longer and wider bones, but with less density, which is likely a major contributing factor for their susceptibility to osteoarthritis. These findings increase our understanding of the role of complement regulation in degenerative arthritis.
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spelling pubmed-47646512016-03-08 Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice Bloom, Anja C. Collins, Fraser L. van't Hof, Rob J. Ryan, Elizabeth S. Jones, Emma Hughes, Timothy R. Morgan, B. Paul Erlandsson, Malin Bokarewa, Maria Aeschlimann, Daniel Evans, Bronwen A.J. Williams, Anwen S. Bone Original Full Length Article Degenerative joint diseases such as osteoarthritis are characterised by aberrant region-specific bone formation and abnormal bone mineral content. A recent study suggested a role for the complement membrane attack complex in experimental models of osteoarthritis. Since CD59a is the principal regulator of the membrane attack complex in mice, we evaluated the impact of CD59a gene deletion upon maintenance of bone architecture. In vivo bone morphology analysis revealed that male CD59a-deficient mice have increased femur length and cortical bone volume, albeit with reduced bone mineral density. However, this phenomenon was not observed in female mice. Histomorphometric analysis of the trabecular bone showed increased rates of bone homeostasis, with both increased bone resorption and mineral apposition rate in CD59a-deficient male mice. When bone cells were studied in isolation, in vitro osteoclastogenesis was significantly increased in male CD59a-deficient mice, although osteoblast formation was not altered. Our data reveal, for the first time, that CD59a is a regulator of bone growth and homeostasis. CD59a ablation in male mice results in longer and wider bones, but with less density, which is likely a major contributing factor for their susceptibility to osteoarthritis. These findings increase our understanding of the role of complement regulation in degenerative arthritis. Elsevier Science 2016-03 /pmc/articles/PMC4764651/ /pubmed/26721735 http://dx.doi.org/10.1016/j.bone.2015.12.014 Text en © 2016 Amgen Inc. http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Original Full Length Article
Bloom, Anja C.
Collins, Fraser L.
van't Hof, Rob J.
Ryan, Elizabeth S.
Jones, Emma
Hughes, Timothy R.
Morgan, B. Paul
Erlandsson, Malin
Bokarewa, Maria
Aeschlimann, Daniel
Evans, Bronwen A.J.
Williams, Anwen S.
Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title_full Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title_fullStr Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title_full_unstemmed Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title_short Deletion of the membrane complement inhibitor CD59a drives age and gender-dependent alterations to bone phenotype in mice
title_sort deletion of the membrane complement inhibitor cd59a drives age and gender-dependent alterations to bone phenotype in mice
topic Original Full Length Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4764651/
https://www.ncbi.nlm.nih.gov/pubmed/26721735
http://dx.doi.org/10.1016/j.bone.2015.12.014
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