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Characteristics of bone strength and metabolism in type 2 diabetic model Tsumura, Suzuki, Obese Diabetes mice

机译:2型糖尿病模型Tsumura,Suzuki,肥胖糖尿病小鼠的骨强度和代谢特征

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ObjectiveType 2 diabetes mellitus (T2DM) is a metabolic disease characterized by hyperglycemia, hyperinsulinemia, and complications such as obesity and osteoporosis. The Tsumura, Suzuki, Obese Diabetes (TSOD) mouse is an animal model of spontaneous obese T2DM. However, bone metabolism in TSOD mice is yet to be investigated. The objective of the present study was to investigate the effects of T2DM on bone mass, metabolism, microstructure, and strength in TSOD mice.MethodsWe determined the following parameters in TSOD mice and Tsumura, Suzuki, Non-obesity (TSNO) mice (as controls): serum glucose levels; serum insulin levels; bone mass; bone microstructure; bone metabolic markers; and bone strength. We also performed the oral glucose tolerance test and examined histological sections of the femur. We compared these data between both groups at pre-diabetic (10?weeks) and established (20?weeks) diabetic conditions.ResultsBone strength, such as extrinsic mechanical properties, increased with age in the TSOD mice and intrinsic material properties decreased at both 10?weeks and 20?weeks. Bone resorption marker levels in TSOD mice were significantly higher than those in the control mice at both ages, but there was no significant difference in bone formation markers between the groups. Bone mass in TSOD mice was lower than that in controls at both ages. The trabecular bone volume at the femoral greater trochanter increased with age in the TSOD mice. The femoral mid-diaphysis in TSOD mice was more slender and thicker than that in TSNO mice at both ages.ConclusionsBone mass of the femur was lower in TSOD mice than in TSNO mice because hyperinsulinemia during pre-diabetic and established diabetic conditions enhanced bone resorption due to high bone turnover. In addition, our data suggest that the bone mass of the femur was significantly reduced as a result of chronic hyperglycemia during established diabetic conditions in TSOD mice. We suggest that bone strength in the femur deteriorated due to the reduction of bone mass and because the femoral mid-diaphysis was more slender in TSOD mice.
机译:Objective 2型糖尿病(T2DM)是一种以高血糖,高胰岛素血症和肥胖症和骨质疏松症等并发症为特征的代谢性疾病。 Tsumura铃木肥胖型糖尿病(TSOD)小鼠是自发性肥胖T2DM的动物模型。然而,尚待研究TSOD小鼠的骨代谢。本研究的目的是研究T2DM对TSOD小鼠骨量,代谢,微结构和强度的影响。方法我们确定了TSOD小鼠和Tsumura,Suzuki,非肥胖(TSNO)小鼠(作为对照)的以下参数):血清葡萄糖水平;血清胰岛素水平;骨量;骨微结构骨代谢指标;和骨骼强度。我们还进行了口服葡萄糖耐量试验并检查了股骨的组织学切片。我们比较了两组在糖尿病前(10周)和确定的(20周)糖尿病条件下的数据。结果TSOD小鼠的骨强度(例如外在力学性能)随年龄增长而增加,而固有物质特性在10天都降低周和20周。在两个年龄段,TSOD小鼠的骨吸收标记物水平均显着高于对照小鼠,但两组之间的骨形成标记物没有显着差异。在两个年龄段,TSOD小鼠的骨量均低于对照组。在TSOD小鼠中,股骨大转子处的小梁骨体积随年龄增加而增加。在两个年龄段,TSOD小鼠的股骨中骨干比TSNO小鼠更细长,更厚。结论TSOD小鼠的股骨质量比TSNO小鼠低,这是因为糖尿病前期和确定的糖尿病状态下的高胰岛素血症会增加由于骨转换率高。另外,我们的数据表明,在TSOD小鼠确定的糖尿病状态下,慢性高血糖导致股骨的骨量显着减少。我们建议,由于骨量的减少以及股骨中骨干在TSOD小鼠中更细长,导致股骨的骨强度下降。

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