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Comparable Effects of Strontium Ranelate and Alendronate Treatment on Fracture Reduction in a Mouse Model of Osteogenesis Imperfecta

机译:锶ronnelate和alynethate治疗对成骨骨膜小鼠模型骨折减少的可比效果

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摘要

Alendronate (Aln) has been the first-line drug for osteogenesis imperfecta (OI), while the comparable efficacy of Aln and strontium ranelate (SrR) remains unclear. This study is aimed at comparing the effects of SrR and Aln treatment in a mouse model of OI. Three-week-old oim/oim and wt/wt female mice were treated with SrR (1800 mg/kg/day), Aln (0.21 mg/kg/week), or vehicle (Veh) for 11 weeks. After the treatment, the average number of fractures sustained per mouse was significantly reduced in both SrR- and Aln-treated oim/oim mice. The effect was comparable between these two agents. Both SrR and Aln significantly increased trabecular bone mineral density, bone histomorphometric parameters (bone volume, trabecular number, and cortical thickness and area), and biomechanical parameters (maximum load and stiffness) as compared with the Veh group. Both treatments reduced bone resorption parameters, with Aln demonstrating a stronger inhibitory effect than SrR. In contrast to its inhibitory effect on bone resorption, SrR maintained bone formation. Aln, however, also suppressed bone formation coupled with an inhibitory effect on bone resorption. The results of this study indicate that SrR has comparable effects with Aln on reducing fractures and improving bone mass and strength. In clinical practice, SrR may be considered an option for patients with OI when other medications are not suitable or have evident contraindications.
机译:Alendronate(ALN)一直是骨质发生的第一线药物(OI),而ALN和锶ranelate(srr)的相当疗效仍不清楚。本研究旨在比较SRR和ALN治疗在OI小鼠模型中的影响。用SRR(1800mg / kg /天),ALN(0.21mg / kg /周)或载体(载体)处理三周历史的OIM / OIM和WT / WT雌性小鼠11周。治疗后,在SRR-和ALN处理的OIM / OIM小鼠中,每只小鼠持续的平均骨折数显着降低。这两个药剂之间的效果是可比的。与车辆相比,SRR和ALN均显着提高了小梁骨矿物密度,骨组织骨密度参数(骨骼体积,骨骼量,骨骼,小颌骨数和皮质厚度和面积),以及生物力学参数(最大载荷和刚度)。两种治疗减少了骨吸收参数,ALN展示比SRR更强的抑制作用。与其对骨吸收的抑制作用相反,SRR保持骨形成。然而,ALN也抑制了骨形成,与骨吸收上的抑制作用相结合。该研究的结果表明,SRR与ALN具有可比的效果,减少骨折并改善骨质量和强度。在临床实践中,当其他药物不适合或具有明显的禁忌症时,SRR可以被认为是OI患者的一种选择。

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