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Duration-dependent effects of clinically relevant oral alendronate doses on cortical bone toughness in beagle dogs

机译:临床相关的口服阿仑膦酸盐剂量对比格犬皮质骨韧性的持续时间依赖性影响

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摘要

Bisphosphonates (BPs) have been shown to significantly reduce bone toughness in vertebrae within one year when given at clinical doses to dogs. Although BPs also reduce toughness in cortical bone when given at high doses, their effect on cortical bone material properties when given at clinical doses is less clear. In part, this may be due to the use of small sample sizes that were powered to demonstrate differences in bone mineral density rather than bone’s material properties. Our lab has conducted several studies in which dogs were treated with alendronate at a clinically relevant dose. The goal of this study was to examine these published and unpublished data collectively to determine whether there is a significant time-dependent effect of alendronate on toughness of cortical bone. This analysis seemed particularly relevant given the recent occurrence of atypical femoral fractures in humans. Differences in the toughness of ribs taken from dogs derived from five separate experiments were measured. The dogs were orally administered saline (CON, 1 ml/kg/day) or alendronate (ALN) at a clinical dose (0.2 mg/kg/day). Treatment duration ranged from 3 months to 3 years. Groups were compared using ANOVA, and time trends analyzed with linear regression analysis. Linear regressions of the percent difference in toughness between CON and ALN at each time point revealed a significant reduction in toughness with longer exposure to ALN. The downward trend was primarily driven by a downward trend in post-yield toughness, whereas toughness in the pre-yield region was not changed relative to CON. These data suggest that a longer duration of treatment with clinical doses of ALN results in deterioration of cortical bone toughness in a time-dependent manner. As the duration of treatment is lengthened, the cortical bone exhibits increasingly brittle behavior. This may be important in assessing the role that long-term BP treatments play in the risk of atypical fractures of femoral cortical bone in humans.
机译:以狗为临床剂量,双膦酸盐(BPs)已显示在一年内显着降低椎骨的骨骼韧性。尽管高剂量使用BP也会降低皮质骨的韧性,但当临床使用BP时它们对皮质骨材料特性的影响尚不清楚。在某种程度上,这可能是由于使用了较小的样本量,这些样本有力地证明了骨矿物质密度的差异,而不是骨骼的材料特性。我们的实验室进行了几项研究,其中对狗用了临床相关剂量的阿仑膦酸盐治疗。这项研究的目的是集体检查这些已发表和未发表的数据,以确定阿仑膦酸盐对皮质骨的韧性是否具有明显的时间依赖性。考虑到人类最近发生的非典型股骨骨折,这一分析似乎特别相关。测量了来自五个独立实验的狗肋骨韧性的差异。给犬口服临床剂量(0.2 mg / kg /天)的生理盐水(CON,1 ml / kg /天)或阿仑膦酸盐(ALN)。治疗时间从3个月到3年不等。使用方差分析比较各组,并使用线性回归分析分析时间趋势。在每个时间点,CON和ALN之间的韧性百分比差异的线性回归显示,随着长时间暴露在ALN中,韧性显着降低。下降趋势主要是由屈服后韧性下降趋势驱动的,而相对于CON,屈服前区域的韧性没有变化。这些数据表明,使用临床剂量的ALN进行更长时间的治疗会导致皮质骨韧性以时间依赖性方式降低。随着治疗时间的延长,皮质骨表现出越来越脆的行为。这对于评估长期BP治疗在人类股骨皮质非典型骨折风险中的作用可能很重要。

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