| Literature DB >> 26717576 |
Jeffrey B Mason1, Boston C Terry2, Samer S Merchant2, Holly M Mason1, Mahdi Nazokkarmaher1.
Abstract
Previously, transplantation of ovaries from young, cycling mice into old, postreproductive-age mice increased life span and decreased cardiomyopathy at death. We anticipated that the same factors that increased life span and decreased cardiomyopathy could also influence the progression of orthopedic disease. At 11 months of age, prepubertally ovariectomized and ovary-intact mice (including reproductively cycling and acyclic mice) received new 60-day-old ovaries. At death, epiphyseal bone in the proximal tibia and the distal femur and mid-shaft tibial and femoral diaphyseal bone was analyzed with micro-computed tomography. For qualitative analysis of osteophytosis, we also included mineralized connective tissue within the stifle joint. Prepubertal ovariectomy had the greatest influence on bone volume, ovarian transplantation had the greatest influence on bone architecture and both treatments influenced bone density. Ovarian transplantation increased cortical, but not trabecular bone density and tended to increase osteophytosis and heterotopic mineralization, except in acyclic recipients. These effects may have been dictated by the timing of the treatments, with ovariectomy appearing to influence early development and ovarian transplantation limited to influencing only the postreproductive period. However, major differences observed between cycling, acyclic and ovariectomized recipients of new ovaries may have been, in part due to differences in the levels of hormone receptors present and the responsiveness of specific bone processes to hormone signaling. Changes that resulted from these treatments may represent a compensatory response to normal age-associated, negative, orthopedic changes. Alternatively, differences between treatments may simply be the 'preservation' of unblemished orthopedic conditions, prior to the influence of negative, age-associated effects. These findings may suggest that in women, tailoring hormone replacement therapy to the patient's current reproductive status may improve therapy effectiveness and that beginning therapy earlier may help preserve trabecular bone mineral density that would otherwise be lost during perimenopause.Entities:
Mesh:
Year: 2015 PMID: 26717576 PMCID: PMC4696788 DOI: 10.1371/journal.pone.0145821
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1Experimental Design.
IT (intact), OX (prepubertally OVX), S (sham surgery) and TX (ovarian transplantation). n = 10 for each μCT scanned group.
Fig 2Joint grading.
a) cranial view of a 3D reconstruction of uCT data from a joint with minimal perturbations. b) cranial view of a 3D reconstruction of uCT data from a joint with maximal perturbations. Measured parameters include A-distal femur width, B-medial collateral ligament thickness, C-joint width at the articulating surface, D-proximal tibia/fibula width, E-medial collateral ligament length.
Effect on epiphyseal medial and lateral tibial plateaus and femoral condyles combined (mean values +/- SD).
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a,b,c,d,eDifferent alphabetic superscripts signify values significantly different from one another.
Effect on diaphyseal mid-shaft tibia and femur bone parameters between treatments (mean values +/- SD).
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a,b,c,d,eDifferent alphabetic superscripts signify values significantly different from one another.
Joint grading from micro-computed tomography 3D reconstructed images (mean values +/- SD).
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MC = medial collateral ligament; LC = lateral collateral ligament.
For MC ossification complete, LC ossification complete and Complete med-lat ossification measurements; 0 = no/none and 1 = yes/complete.
Osteophytosis score; 1 = no pathology, 2 = mild pathology, 3 = extensive conjoined, >3 surfaces, 4 = complete loss of joint architecture.
a,b,c,d,eDifferent alphabetic superscripts signify values significantly different from one another.