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Publication : Femoral peak bone mass and osteoclast number in an animal model of age-related spontaneous osteopenia.

First Author  Okamoto Y Year  1995
Journal  Anat Rec Volume  242
Issue  1 Pages  21-8
PubMed ID  7604978 Mgi Jnum  J:25058
Mgi Id  MGI:72772 Doi  10.1002/ar.1092420104
Citation  Okamoto Y, et al. (1995) Femoral peak bone mass and osteoclast number in an animal model of age-related spontaneous osteopenia. Anat Rec 242(1):21-8
abstractText  BACKGROUND: SAMP6 was developed as a murine model of age-related spontaneous osteopenia characterized by low peak bone mass. A morphometric study of the growing femur in SAMP6 and sex-matched SAMP2 at 10 days to 4 months of age was done to examine the pathogenic process related to osteopenia. METHODS: Age-related changes in cortical bone thickness, femur score, trabecular bone volume, thickness of epiphyseal growth plate, number of osteoclasts, and osteoclast surface were measured with a computerized image analyzer. Osteoclasts were examined cytomorphometrically after TRAP (tartrate resistant acid phosphatase) staining of the femoral sections. RESULTS: Cortical bone thickness and femur score increased significantly with age, while trabecular bone volume decreased significantly. Comparing mean values of cortical bone thickness, femur score and trabecular bone volume, we noted significantly lower mean values in SAMP6 than in SAMP2 mice. These significant inter-stain differences first became evident in 20-40-day-old mice, but there was no significant difference in thickness of the epiphyseal growth plate between the two strains. The mean values of the number of osteoclasts per unit bone surface length and of the osteoclast surface in SAMP6 were significantly greater than in age- and sex-matched SAMP2. Histograms of distribution of size of osteoclasts of 40-day-old male mice revealed that larger ones were more frequently seen in SAMP6. Furthermore, the ratio of osteoclasts/TRAP positive cells free in the bone marrow cavity was significantly higher in SAMP6 than in SAMP2. CONCLUSION: Activated bone resorption may play a role in the osteopenia seen in SAMP6.
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