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Parathyroid hormone and bisphosphonate have opposite effects on stress fracture repair.

机译:甲状旁腺激素和双膦酸酯对应力性骨折的修复作用相反。

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This study was aimed to investigate the effects of Parathyroid hormone (PTH) and alendronate (ALN) on stress fracture repair. Stress fractures were induced in the ulnae of female adult rats. Animals were treated daily with vehicle, PTH (40 microg/kg) or alendronate (2 microg/kg), respectively. Bone mineral content (BMC) and bone mineral density (BMD) of bilateral ulnae were measured at two, four and eight weeks following induction of stress fracture. Histology at the ulna midshaft was undertaken at 2 and 4 weeks and mechanical testing was done at 8 weeks after stress fracture. PTH increased BMC significantly by 7% at 4 weeks and BMD and BMC significantly by 10% and 7% at 8 weeks compared to the control. Alendronate did not change BMD or BMC in comparison with the control. PTH significantly stimulated bone formation by 114% at 2 weeks, increased intracortical resorption area by 23% at 4 weeks, and enhanced the ultimate force of the affected ulnae by 15% at 8 weeks compared to the control. Alendronate significantly suppressed bone formation rate by 44% compared to the control at 4 weeks. These data indicate that PTH may accelerate intracortical bone remodeling induced by microdamage and alendronate may delay intracortical bone remodeling during stress fracture repair in rats. This study suggests that PTH may be used to facilitate stress fracture repair whereas bisphosphonates may delay tissue level repair of stress fractures.
机译:本研究旨在探讨甲状旁腺激素(PTH)和阿仑膦酸盐(ALN)对应力性骨折修复的影响。在成年雌性大鼠的尺骨上诱发了应力性骨折。每天分别用赋形剂,PTH(40微克/千克)或阿仑膦酸盐(2微克/千克)治疗动物。在诱发应力性骨折后两周,四周和八周测量双侧尺骨的骨矿物质含量(BMC)和骨矿物质密度(BMD)。尺骨中轴的组织学检查在应力断裂后的第2和4周进行,力学测试在第8周进行。与对照组相比,PTH在4周时BMC显着增加了7%,而BMD和BMC在8周时显着增加了10%和7%。与对照相比,阿仑膦酸酯未改变BMD或BMC。与对照组相比,PTH在2周时显着刺激了114%的骨形成,在4周时皮质内吸收面积增加了23%,并在8周时将受影响的尺骨的极限力量提高了15%。与对照组相比,阿仑膦酸盐在4周时显着抑制了44%的骨形成率。这些数据表明,PTH可能会加速由微损伤引起的皮质内骨重塑,而阿仑膦酸盐可能会延迟大鼠应力性骨折修复过程中的皮质内骨重塑。这项研究表明,PTH可用于促进应力性骨折的修复,而双膦酸盐可能会延迟应力性骨折的组织水平的修复。

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