Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility

A Carriero; M Doube; M Vogt; B Busse; J Zustin; A Levchuk; P Schneider; R Müller; S J Shefelbine

doi:10.1016/j.bone.2013.12.020

Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility

Standard

Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility. / Carriero, A; Doube, M; Vogt, M; Busse, B; Zustin, J; Levchuk, A; Schneider, P; Müller, R; Shefelbine, S J.

In: BONE, Vol. 61, 01.04.2014, p. 116-24.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Carriero, A, Doube, M, Vogt, M, Busse, B, Zustin, J, Levchuk, A, Schneider, P, Müller, R & Shefelbine, SJ 2014, 'Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility', BONE, vol. 61, pp. 116-24. https://doi.org/10.1016/j.bone.2013.12.020

APA

Carriero, A., Doube, M., Vogt, M., Busse, B., Zustin, J., Levchuk, A., Schneider, P., Müller, R., & Shefelbine, S. J. (2014). Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility. BONE, 61, 116-24. https://doi.org/10.1016/j.bone.2013.12.020

Vancouver

Carriero A, Doube M, Vogt M, Busse B, Zustin J, Levchuk A et al. Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility. BONE. 2014 Apr 1;61:116-24. https://doi.org/10.1016/j.bone.2013.12.020

Bibtex

@article{9314f5e422a642cdaa3aef9456972fa1,

title = "Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility",

abstract = "Osteogenesis imperfecta (brittle bone disease) is caused by mutations in the collagen genes and results in skeletal fragility. Changes in bone porosity at the tissue level indicate changes in bone metabolism and alter bone mechanical integrity. We investigated the cortical bone tissue porosity of a mouse model of the disease, oim, in comparison to a wild type (WT-C57BL/6), and examined the influence of canal architecture on bone mechanical performance. High-resolution 3D representations of the posterior tibial and the lateral humeral mid-diaphysis of the bones were acquired for both mouse groups using synchrotron radiation-based computed tomography at a nominal resolution of 700nm. Volumetric morphometric indices were determined for cortical bone, canal network and osteocyte lacunae. The influence of canal porosity architecture on bone mechanics was investigated using microarchitectural finite element (μFE) models of the cortical bone. Bright-field microscopy of stained sections was used to determine if canals were vascular. Although total cortical porosity was comparable between oim and WT bone, oim bone had more numerous and more branched canals (p<0.001), and more osteocyte lacunae per unit volume compared to WT (p<0.001). Lacunae in oim were more spherical in shape compared to the ellipsoidal WT lacunae (p<0.001). Histology revealed blood vessels in all WT and oim canals. μFE models of cortical bone revealed that small and branched canals, typical of oim bone, increase the risk of bone failure. These results portray a state of compromised bone quality in oim bone at the tissue level, which contributes to its deficient mechanical properties.",

author = "A Carriero and M Doube and M Vogt and B Busse and J Zustin and A Levchuk and P Schneider and R M{\"u}ller and Shefelbine, {S J}",

year = "2014",

month = apr,

day = "1",

doi = "10.1016/j.bone.2013.12.020",

language = "English",

volume = "61",

pages = "116--24",

journal = "BONE",

issn = "8756-3282",

publisher = "Elsevier Inc.",

}

RIS

TY - JOUR

T1 - Altered lacunar and vascular porosity in osteogenesis imperfecta mouse bone as revealed by synchrotron tomography contributes to bone fragility

AU - Carriero, A

AU - Doube, M

AU - Vogt, M

AU - Busse, B

AU - Zustin, J

AU - Levchuk, A

AU - Schneider, P

AU - Müller, R

AU - Shefelbine, S J

PY - 2014/4/1

Y1 - 2014/4/1

N2 - Osteogenesis imperfecta (brittle bone disease) is caused by mutations in the collagen genes and results in skeletal fragility. Changes in bone porosity at the tissue level indicate changes in bone metabolism and alter bone mechanical integrity. We investigated the cortical bone tissue porosity of a mouse model of the disease, oim, in comparison to a wild type (WT-C57BL/6), and examined the influence of canal architecture on bone mechanical performance. High-resolution 3D representations of the posterior tibial and the lateral humeral mid-diaphysis of the bones were acquired for both mouse groups using synchrotron radiation-based computed tomography at a nominal resolution of 700nm. Volumetric morphometric indices were determined for cortical bone, canal network and osteocyte lacunae. The influence of canal porosity architecture on bone mechanics was investigated using microarchitectural finite element (μFE) models of the cortical bone. Bright-field microscopy of stained sections was used to determine if canals were vascular. Although total cortical porosity was comparable between oim and WT bone, oim bone had more numerous and more branched canals (p<0.001), and more osteocyte lacunae per unit volume compared to WT (p<0.001). Lacunae in oim were more spherical in shape compared to the ellipsoidal WT lacunae (p<0.001). Histology revealed blood vessels in all WT and oim canals. μFE models of cortical bone revealed that small and branched canals, typical of oim bone, increase the risk of bone failure. These results portray a state of compromised bone quality in oim bone at the tissue level, which contributes to its deficient mechanical properties.

AB - Osteogenesis imperfecta (brittle bone disease) is caused by mutations in the collagen genes and results in skeletal fragility. Changes in bone porosity at the tissue level indicate changes in bone metabolism and alter bone mechanical integrity. We investigated the cortical bone tissue porosity of a mouse model of the disease, oim, in comparison to a wild type (WT-C57BL/6), and examined the influence of canal architecture on bone mechanical performance. High-resolution 3D representations of the posterior tibial and the lateral humeral mid-diaphysis of the bones were acquired for both mouse groups using synchrotron radiation-based computed tomography at a nominal resolution of 700nm. Volumetric morphometric indices were determined for cortical bone, canal network and osteocyte lacunae. The influence of canal porosity architecture on bone mechanics was investigated using microarchitectural finite element (μFE) models of the cortical bone. Bright-field microscopy of stained sections was used to determine if canals were vascular. Although total cortical porosity was comparable between oim and WT bone, oim bone had more numerous and more branched canals (p<0.001), and more osteocyte lacunae per unit volume compared to WT (p<0.001). Lacunae in oim were more spherical in shape compared to the ellipsoidal WT lacunae (p<0.001). Histology revealed blood vessels in all WT and oim canals. μFE models of cortical bone revealed that small and branched canals, typical of oim bone, increase the risk of bone failure. These results portray a state of compromised bone quality in oim bone at the tissue level, which contributes to its deficient mechanical properties.

U2 - 10.1016/j.bone.2013.12.020

DO - 10.1016/j.bone.2013.12.020

M3 - SCORING: Journal article

C2 - 24373921

VL - 61

SP - 116

EP - 124

JO - BONE

JF - BONE

SN - 8756-3282

ER -