首页> 美国卫生研究院文献>The Journal of Nutrition >Cortical and Trabecular Bone Bone Mineral Density and Resistance to ex Vivo Fracture Are Not Altered in Response to Life-Long Vitamin A Supplementation in Aging Rats
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Cortical and Trabecular Bone Bone Mineral Density and Resistance to ex Vivo Fracture Are Not Altered in Response to Life-Long Vitamin A Supplementation in Aging Rats

机译:补充维生素A对衰老大鼠的反应皮质和小梁骨骨矿物质密度以及对离体骨折的抵抗力没有改变

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摘要

High vitamin A (VA) intakes have been correlated with increased risk of bone fracture. Over 50% of the U.S. adult population reports use of dietary supplements, which can result in VA intakes > 200% of the RDA. In this study, 2 experiments were designed to determine the effect of dietary VA on cortical and trabecular bone properties and resistance to ex vivo fracture. In Expt. 1, we investigated whether orally administered VA accumulates in bone. Seven-week-old rats were treated daily with VA (6 mg/d for 14 d). Total retinol increased in both the tibia and femur (P < 0.01). In Expt. 2, we conducted a longitudinal study in which rats were fed 1 of 3 levels of dietary VA (marginal, adequate, and supplemented, equal to 0.35, 4, and 50 μg retinol/g diet, respectively) from weaning until the ages of 2–3 mo (young), 8–10 mo (middle-age), and 18–20 mo (old). Tibial trabecular and cortical bone structure, bone mineral density, and resistance to fracture were measured using micro-computed tomography and material testing system analysis, respectively. The VA-marginal diet affected measures of cortical bone dimension, suggesting bone remodeling was altered. VA supplementation increased medullary area and decreased cortical thickness in young rats (P < 0.05), but these changes were not present during aging. VA supplementation did not affect resistance to fracture or bone mineral content in old rats. From these results, we conclude that VA-marginal status affects trabecular bone more than cortical bone, and VA supplementation at a moderate level over the lifetime is unlikely to increase the risk of age-related bone fracture in rats.
机译:高维生素A(VA)摄入与骨折风险增加相关。美国有超过50%的成年人口使用膳食补充剂,这可能导致VA摄入量> RDA的200%。在这项研究中,设计了2个实验来确定日粮VA对皮质和小梁骨特性以及对离体骨折的抵抗力的影响。在Expt。如图1所示,我们研究了口服VA在骨中是否蓄积。每天用VA(6 mg / d,持续14 d)治疗7周龄大鼠。胫骨和股骨中总视黄醇增加(P <0.01)。在Expt。参照图2,我们进行了一项纵向研究,从断奶到2岁,分别向大鼠喂食了3种水平的日粮VA(分别为0.35、4和50μg视黄醇/ g饮食)中的1种。 –3 mo(年轻),8–10 mo(中年)和18–20 mo(旧)。分别使用微型计算机断层扫描和材料测试系统分析来测量胫骨小梁和皮质的骨结构,骨矿物质密度和抗断裂性。 VA边缘饮食会影响皮质骨尺寸的测量,表明骨骼重塑已改变。 VA补充增加了幼鼠的髓质面积并降低了皮层厚度(P <0.05),但这些变化在衰老过程中并不存在。 VA补充剂不会影响老年大鼠对骨折或骨矿物质含量的抵抗力。根据这些结果,我们得出结论:VA边缘状态对小梁骨的影响大于皮质骨,并且在终生中适度补充VA不太可能增加大鼠与年龄相关的骨折的风险。

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