Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing

PHOSPHO1 is one of principal proteins involved in initiating bone matrix mineralisation. Recent studies have found that Phospho1 KO mice (Phospho1-R74X) display multiple skeletal abnormalities with spontaneous fractures, bowed long bones, osteomalacia and scoliosis. These analyses have however been...

Descripción completa

Detalles Bibliográficos
Autores principales: Javaheri, B., Carriero, A., Staines, K.A., Chang, Y.-M., Houston, D.A., Oldknow, K.J., Millan, J.L., Kazeruni, Bassir N., Salmon, P., Shefelbine, S., Farquharson, C., Pitsillides, A.A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2015
Materias:
Original Full Length Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4652607/
https://www.ncbi.nlm.nih.gov/pubmed/26232374
http://dx.doi.org/10.1016/j.bone.2015.07.035
_version_ 1782401786219331584
author Javaheri, B.
Carriero, A.
Staines, K.A.
Chang, Y.-M.
Houston, D.A.
Oldknow, K.J.
Millan, J.L.
Kazeruni, Bassir N.
Salmon, P.
Shefelbine, S.
Farquharson, C.
Pitsillides, A.A.
author_facet Javaheri, B.
Carriero, A.
Staines, K.A.
Chang, Y.-M.
Houston, D.A.
Oldknow, K.J.
Millan, J.L.
Kazeruni, Bassir N.
Salmon, P.
Shefelbine, S.
Farquharson, C.
Pitsillides, A.A.
author_sort Javaheri, B.
collection PubMed
description PHOSPHO1 is one of principal proteins involved in initiating bone matrix mineralisation. Recent studies have found that Phospho1 KO mice (Phospho1-R74X) display multiple skeletal abnormalities with spontaneous fractures, bowed long bones, osteomalacia and scoliosis. These analyses have however been limited to young mice and it remains unclear whether the role of PHOSPHO1 is conserved in the mature murine skeleton where bone turnover is limited. In this study, we have used ex-vivo computerised tomography to examine the effect of Phospho1 deletion on tibial bone architecture in mice at a range of ages (5, 7, 16 and 34 weeks of age) to establish whether its role is conserved during skeletal growth and maturation. Matrix mineralisation has also been reported to influence terminal osteoblast differentiation into osteocytes and we have also explored whether hypomineralised bones in Phospho1 KO mice exhibit modified osteocyte lacunar and vascular porosity. Our data reveal that Phospho1 deficiency generates age-related defects in trabecular architecture and compromised cortical microarchitecture with greater porosity accompanied by marked alterations in osteocyte shape, significant increases in osteocytic lacuna and vessel number. Our in vitro studies examining the behaviour of osteoblast derived from Phospho1 KO and wild-type mice reveal reduced levels of matrix mineralisation and modified osteocytogenic programming in cells deficient in PHOSPHO1. Together our data suggest that deficiency in PHOSPHO1 exerts modifications in bone architecture that are transient and depend upon age, yet produces consistent modification in lacunar and vascular porosity. It is possible that the inhibitory role of PHOSPHO1 on osteocyte differentiation leads to these age-related changes in bone architecture. It is also intriguing to note that this apparent acceleration in osteocyte differentiation evident in the hypomineralised bones of Phospho1 KO mice suggests an uncoupling of the interplay between osteocytogenesis and biomineralisation. Further studies are required to dissect the molecular processes underlying the regulatory influences exerted by PHOSPHO1 on the skeleton with ageing.
format Online
Article
Text
id pubmed-4652607
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Elsevier Science
record_format MEDLINE/PubMed
spelling pubmed-46526072015-12-17 Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing Javaheri, B. Carriero, A. Staines, K.A. Chang, Y.-M. Houston, D.A. Oldknow, K.J. Millan, J.L. Kazeruni, Bassir N. Salmon, P. Shefelbine, S. Farquharson, C. Pitsillides, A.A. Bone Original Full Length Article PHOSPHO1 is one of principal proteins involved in initiating bone matrix mineralisation. Recent studies have found that Phospho1 KO mice (Phospho1-R74X) display multiple skeletal abnormalities with spontaneous fractures, bowed long bones, osteomalacia and scoliosis. These analyses have however been limited to young mice and it remains unclear whether the role of PHOSPHO1 is conserved in the mature murine skeleton where bone turnover is limited. In this study, we have used ex-vivo computerised tomography to examine the effect of Phospho1 deletion on tibial bone architecture in mice at a range of ages (5, 7, 16 and 34 weeks of age) to establish whether its role is conserved during skeletal growth and maturation. Matrix mineralisation has also been reported to influence terminal osteoblast differentiation into osteocytes and we have also explored whether hypomineralised bones in Phospho1 KO mice exhibit modified osteocyte lacunar and vascular porosity. Our data reveal that Phospho1 deficiency generates age-related defects in trabecular architecture and compromised cortical microarchitecture with greater porosity accompanied by marked alterations in osteocyte shape, significant increases in osteocytic lacuna and vessel number. Our in vitro studies examining the behaviour of osteoblast derived from Phospho1 KO and wild-type mice reveal reduced levels of matrix mineralisation and modified osteocytogenic programming in cells deficient in PHOSPHO1. Together our data suggest that deficiency in PHOSPHO1 exerts modifications in bone architecture that are transient and depend upon age, yet produces consistent modification in lacunar and vascular porosity. It is possible that the inhibitory role of PHOSPHO1 on osteocyte differentiation leads to these age-related changes in bone architecture. It is also intriguing to note that this apparent acceleration in osteocyte differentiation evident in the hypomineralised bones of Phospho1 KO mice suggests an uncoupling of the interplay between osteocytogenesis and biomineralisation. Further studies are required to dissect the molecular processes underlying the regulatory influences exerted by PHOSPHO1 on the skeleton with ageing. Elsevier Science 2015-12 /pmc/articles/PMC4652607/ /pubmed/26232374 http://dx.doi.org/10.1016/j.bone.2015.07.035 Text en © 2015 The Authors. Published by Elsevier 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
Javaheri, B.
Carriero, A.
Staines, K.A.
Chang, Y.-M.
Houston, D.A.
Oldknow, K.J.
Millan, J.L.
Kazeruni, Bassir N.
Salmon, P.
Shefelbine, S.
Farquharson, C.
Pitsillides, A.A.
Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title_full Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title_fullStr Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title_full_unstemmed Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title_short Phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
title_sort phospho1 deficiency transiently modifies bone architecture yet produces consistent modification in osteocyte differentiation and vascular porosity with ageing
topic Original Full Length Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4652607/
https://www.ncbi.nlm.nih.gov/pubmed/26232374
http://dx.doi.org/10.1016/j.bone.2015.07.035
work_keys_str_mv AT javaherib phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT carrieroa phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT staineska phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT changym phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT houstonda phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT oldknowkj phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT millanjl phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT kazerunibassirn phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT salmonp phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT shefelbines phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT farquharsonc phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing
AT pitsillidesaa phospho1deficiencytransientlymodifiesbonearchitectureyetproducesconsistentmodificationinosteocytedifferentiationandvascularporositywithageing

Ejemplares similares