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阿仑膦酸钠给药对去势大鼠骨密度和骨强度的影响。

Effect of alendronate administration on bone mineral density and bone strength in castrated rats.

作者信息

Broulik P D, Rosenkrancová J, Růzicka P, Sedlácek R

机构信息

Third Medical Clinic, First Medical Faculty, Charles University, Prague 2-12808, Czech Republic.

出版信息

Horm Metab Res. 2005 Jul;37(7):414-8. doi: 10.1055/s-2005-870234.

Abstract

Castration of male rats leads to increased bone turnover and osteopenia. This study was conducted to examine the effects of the aminobisphosphonate alendronate on castration-induced bone changes. Bisphosphonates are drugs that inhibit bone turnover by decreasing the resorption. Since they suppress bone remodeling, they may also prevent the repair of microdamage and decrease bone strength. Although the mechanical properties of bones are directly related to the determination of fracture risk, bisphosphonate effects on the related variables have scarcely been investigated. Twenty-four male Wistar rats at two months of age were castrated or sham-operated to evaluate the effects of long-term administration (six months) of sodium alendronate at a dose of 1 mg/kg/day. The bones were tested mechanically by a three-point bending test in a Mini Bionix (MTS) testing system. High bone remodeling seen in castrated rats expressed by increased TrACP and B-ALP was suppressed by alendronate administration. Bone from castrated rats was characterized by a reduction in bone density as well as ash, calcium and phosphate content. Castration significantly altered mechanical properties of bone and femoral cortical thickness. When castrated rats were treated with high dose of alendronate, the changes in bone density resulting from castration were entirely prevented, and mechanical analysis revealed preserved mechanical strength of femur and cortical thickness. We conclude that castration induces cortical bone loss associated with high bone turnover in the male rat, and this bone loss can be prevented by alendronate through the inhibition of osteoclastic activity, while preserving the mechanical properties of bone. These results document the efficacy of alendronate, even at high doses, in preventing bone loss, loss of bone mechanical strength, and the rise in biochemical bone turnover indicators due to castration in rats, and raises the possibility that a alendronate could be equally effective in humans.

摘要

雄性大鼠去势会导致骨转换增加和骨质减少。本研究旨在探讨氨基双膦酸盐阿仑膦酸钠对去势诱导的骨骼变化的影响。双膦酸盐是一类通过减少骨吸收来抑制骨转换的药物。由于它们抑制骨重塑,也可能会阻止微损伤的修复并降低骨强度。尽管骨骼的力学性能与骨折风险的确定直接相关,但双膦酸盐对相关变量的影响几乎未被研究过。将24只两个月大的雄性Wistar大鼠进行去势或假手术,以评估每日剂量为1 mg/kg的阿仑膦酸钠长期给药(六个月)的效果。在Mini Bionix(MTS)测试系统中通过三点弯曲试验对骨骼进行力学测试。阿仑膦酸钠给药可抑制去势大鼠中因TrACP和B-ALP升高所表现出的高骨转换。去势大鼠的骨骼表现为骨密度以及灰分、钙和磷含量降低。去势显著改变了骨骼的力学性能和股骨皮质厚度。当用高剂量阿仑膦酸钠治疗去势大鼠时,完全防止了去势导致的骨密度变化,力学分析显示股骨的力学强度和皮质厚度得以保留。我们得出结论,去势诱导雄性大鼠皮质骨丢失并伴有高骨转换,而阿仑膦酸钠可通过抑制破骨细胞活性来预防这种骨丢失,同时保留骨骼的力学性能。这些结果证明了阿仑膦酸钠即使在高剂量下,在预防大鼠因去势导致的骨丢失、骨力学强度丧失以及生化骨转换指标升高方面的有效性,并增加了阿仑膦酸钠在人类中可能同样有效的可能性。

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