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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Relationship of Volumetric BMD and Structural Parameters at Different Skeletal Sites to Sex Steroid Levels in Men.
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Relationship of Volumetric BMD and Structural Parameters at Different Skeletal Sites to Sex Steroid Levels in Men.

机译:男性不同骨骼部位的骨密度和结构参数与男性类固醇水平的关系。

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摘要

In a population-based, cross-sectional study, we related age-associated changes in vBMD and in bone structural parameters to circulating bioavailable estradiol and testosterone levels in men. Associations between these bone mass/structural parameters and sex steroid levels were progressively stronger with age. Our previously postulated "threshold" for skeletal estrogen deficiency was most evident at cortical sites. INTRODUCTION: Serum sex steroids, particularly estrogen levels, are associated with bone mass in men, and previous work has suggested that there may be a "threshold" bioavailable estradiol (bio E(2)) level below which the male skeleton becomes estrogen deficient. However, previous studies addressing this issue have exclusively used DXA, which cannot separate trabecular from cortical bone or provide information on bone geometry or structure. MATERIALS AND METHODS: In an age-stratified population sample of 314 men (age, 22-91 years), we assessed volumetric BMD (vBMD) and bone geometry by QCT at the lumbar spine, femoral neck, distal radius, and distal tibia and related these to circulating bio E(2) and bio testosterone (T) levels. RESULTS: Compared with young men (age, 20-39 years), middle-aged men (age, 40-59 years) had significantly lower bio T (-26%, p < 0.001) and bio E(2) (-9%, p = 0.038) levels, and these decreases were even greater in the elderly men (age >/= 60 years, -60% and -38% for bio T and bio E(2), respectively, p < 0.001 for both). Reflecting their intact gonadal status, vBMD/structural parameters were not related to sex steroid levels in young men, whereas bio E(2) levels were associated consistently with vBMD and variably with bone geometric parameters in the elderly men; middle-aged men showed associations with bio E(2) and bio T at some sites. At all cortical sites, vBMD was associated with bio E(2) at low (<30 pM, R = 0.27-0.41, p < 0.05-0.001) but not high (>/=30 pM, R = -0.003 to 0.12, p = not significant) levels; no such differences were evident at trabecular sites. CONCLUSIONS: In men, bio E(2) is the most consistent predictor of vBMD and some bone geometric variables as assessed by QCT. We also extend our previous findings on a possible "threshold" for skeletal estrogen deficiency by showing that this is most evident for cortical sites.
机译:在一项基于人群的横断面研究中,我们将vBMD和骨骼结构参数中与年龄相关的变化与男性循环中可利用的雌二醇和睾丸激素水平相关联。这些骨质量/结构参数与性类固醇水平之间的关联随着年龄的增长而逐渐增强。我们先前假设的骨骼雌激素缺乏症的“阈值”在皮层部位最为明显。简介:血清性类固醇,特别是雌激素水平与男性骨量有关,以前的研究表明,可能存在“阈值”生物利用雌二醇(bio E(2))水平,低于此水平,男性骨骼就会变得雌激素缺乏。但是,针对该问题的先前研究仅使用DXA,它无法将小梁与皮质骨分开,也无法提供有关骨几何形状或结构的信息。材料与方法:在314名男性(年龄为22-91岁)的年龄分层的人群样本中,我们通过QCT对腰椎,股骨颈,distal骨远端和胫骨远端的BMD(vBMD)和骨骼几何进行了评估。这些与循环生物E(2)和生物睾丸激素(T)水平相关。结果:与年轻男性(20-39岁)相比,中年男性(40-59岁)的生物T值(-26%,p <0.001)和生物E(2)显着较低(-9 %,p = 0.038)水平,而这些下降幅度在老年男性中更为明显(年龄> / = 60岁,bio T和bio E(2)分别为-60%和-38​​%,两者均p <0.001 )。反映其完整的性腺状态,vBMD /结构参数与年轻男性中的性类固醇水平无关,而生物E(2)水平与vBMD一致且与老年男性的骨几何参数相关;中年男子在某些部位表现出与生物E(2)和生物T的关联。在所有皮质位点,vBMD与低(<30 pM,R = 0.27-0.41,p <0.05-0.001)但不高(> / = 30 pM,R = -0.003至0.12, p =不显着)水平;在小梁部位没有明显的差异。结论:在男性中,bio E(2)是vBMD和一些由QCT评估的骨几何变量最一致的预测因子。我们还通过显示对皮质部位最明显的证据,扩展了先前关于可能存在的骨骼雌激素缺乏症“阈值”的发现。

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