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脂联素及其与儿童期骨量积累的关系。

Adiponectin and its association with bone mass accrual in childhood.

机构信息

Academic Rheumatology, School of Clinical Sciences, Bristol, University of Bristol, Bristol, United Kingdom.

出版信息

J Bone Miner Res. 2010 Oct;25(10):2212-20. doi: 10.1002/jbmr.116.

Abstract

Circulating adiponectin levels are inversely related to bone mineral density (BMD) in humans and animal models. Previous studies in humans have been confined largely to adult populations, and whether adiponectin influences bone mass accrual in childhood is unclear. We examined this question using the Avon Longitudinal Study of Parents and Children (ALSPAC) birth cohort by investigating relationships between circulating adiponectin levels at a mean age of 9.9 years, indices of bone mass as measured by total-body dual-energy X-ray absorptiometry (DXA) at ages 9.9 and 15.5 years, and cortical bone parameters as measured by peripheral quantitative computed tomography (pQCT) of the midtibia at age 15.5 years. A total of 4927 children were included at age 9.9 years, of whom 97% and 90% of boys and girls, respectively, were in prepuberty or early puberty, as defined by Tanner stage 1-2. A total of 2754 children were included at age 15.5 years, of whom 95% and 97% of boys and girls, respectively, were in late puberty, as defined by Tanner stage 4-5. Circulating adiponectin was found to be related to fat mass, lean mass, and, to a lesser extent, height, so analyses were adjusted for these three variables to identify possible independent effects of adiponectin on bone development. Adiponectin was inversely related to total-body-less-head bone mineral content (BMC; -3.0%), bone area (BA; -1.8%), BMC divided by BA (BMD; -4.8%), and BMC adjusted for BA by linear regression (aBMC; -5.6%), as measured at age 9.9 years (coefficients show change per doubling in adiponectin concentration, p < .001). Consistent with these results, inverse associations also were seen between adiponectin and cortical BMC (-4.8%) and cortical bone area (-4.7%), as measured by tibial pQCT at age 15.5 years (p < .001). Further pQCT results suggested that this inverse association of adiponectin with skeletal development predominantly involved a negative association with endosteal relative to periosteal expansion, as reflected by cortical thickness (-6.0%, p < .001). We conclude that, independent of fat mass, lean mass, and height, adiponectin is associated with lower bone mass in childhood predominantly owing to an influence on relative endosteal expansion. Since these associations were observed before and after puberty, this suggests that setting of adiponectin levels in midchildhood has the potential to exert long-term effects on bone strength and fracture risk.

摘要

循环脂联素水平与人类和动物模型的骨密度(BMD)呈负相关。先前在人类中的研究主要局限于成年人群,而脂联素是否影响儿童时期的骨量积累尚不清楚。我们通过调查阿冯纵向研究父母和孩子(ALSPAC)出生队列中的问题,使用全身双能 X 射线吸收法(DXA)在 9.9 岁和 15.5 岁时测量的总骨量指数,以及通过胫骨中端外周定量计算机断层扫描(pQCT)测量的皮质骨参数来检验这一问题。共有 4927 名儿童在 9.9 岁时被纳入研究,其中男孩和女孩分别有 97%和 90%处于青春期前或早期青春期,根据 Tanner 分期 1-2 定义。共有 2754 名儿童在 15.5 岁时被纳入研究,其中男孩和女孩分别有 95%和 97%处于青春期晚期,根据 Tanner 分期 4-5 定义。发现循环脂联素与脂肪量、瘦体量有关,与身高的关系较小,因此,分析中调整了这三个变量,以确定脂联素对骨骼发育的可能独立影响。脂联素与全身(不包括头部)骨矿物质含量(BMC;-3.0%)、骨面积(BA;-1.8%)、BMC 除以 BA(BMD;-4.8%)和通过线性回归校正 BA 的 BMC(aBMC;-5.6%)呈负相关,这是在 9.9 岁时测量的(系数显示每倍增脂联素浓度的变化,p<0.001)。与这些结果一致,在 15.5 岁时通过胫骨 pQCT 测量,脂联素与皮质 BMC(-4.8%)和皮质骨面积(-4.7%)也呈负相关(p<0.001)。进一步的 pQCT 结果表明,脂联素与骨骼发育的这种负相关主要涉及与骨内膜相比骨外膜的负相关,这反映在皮质厚度上(-6.0%,p<0.001)。我们的结论是,独立于脂肪量、瘦体量和身高,脂联素与儿童时期较低的骨量有关,主要是由于对相对骨内膜扩张的影响。由于这些关联在青春期前后都有观察到,这表明儿童中期脂联素水平的设定有可能对骨强度和骨折风险产生长期影响。

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