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维生素D受体基因的两种多态性——与绝经后妇女骨量及有无激素替代治疗情况下骨量的5年变化的关联:丹麦骨质疏松症预防研究

Two polymorphisms in the vitamin D receptor gene--association with bone mass and 5-year change in bone mass with or without hormone-replacement therapy in postmenopausal women: the Danish Osteoporosis Prevention Study.

作者信息

Tofteng C L, Jensen J E B, Abrahamsen B, Odum L, Brot C

机构信息

Department 545, The Osteoporosis Research Clinic, Hvidovre Hospital, Denmark.

出版信息

J Bone Miner Res. 2002 Aug;17(8):1535-44. doi: 10.1359/jbmr.2002.17.8.1535.

Abstract

The significance of an interrelation between nongenetic factors and genotype effects in the regulation of bone mass is not clear. In this prospective study of 429 healthy early postmenopausal Danish women, we investigated the association between bone mineral density (BMD) and the FokI and BsmI polymorphisms in the vitamin D receptor (VDR) gene. Participants were allocated to either hormone-replacement therapy (HRT) or no treatment by randomization or personal choice. After 5 years, 332 women with unchanged treatment status were available for analyses, 98 of these women were still on HRT. No association with initial BMD or 5-year change in BMD was found for either polymorphism. In women with body mass index (BMI) < 25 (n = 282), the f allele was associated with lower BMD of the hip (p < 0.001) and forearm (p = 0.001), and the b allele was associated with lower spine BMD (p = 0.02). Comparing thin/normal weight women with overweight/ obese women of the same genotype, FF women had similar BMD at all measured sites in contrast to Ff and ff women in whom BMD, as expected, was higher in the overweight/obese women. Similar results were found for the BsmI polymorphism with no difference in BMD between BMI groups in BB women. Segregation into groups according to dietary calcium intake did not reveal any genotype association with BMD. These results provide some evidence of a modifying effect of nongenetic factors, specifically BMI, on the association between VDR genotype and BMD. High BMI may protect against lower BMD seen in association with thef or b alleles. In some genotypes (FF and BB), BMI had relatively little effect on BMD.

摘要

非遗传因素与基因型效应在骨量调节中的相互关系的重要性尚不清楚。在这项针对429名健康的丹麦绝经后早期女性的前瞻性研究中,我们调查了骨矿物质密度(BMD)与维生素D受体(VDR)基因中的FokI和BsmI多态性之间的关联。参与者通过随机分组或个人选择被分配接受激素替代疗法(HRT)或不接受治疗。5年后,332名治疗状态未改变的女性可供分析,其中98名女性仍在接受HRT。未发现任何一种多态性与初始BMD或BMD的5年变化有关联。在体重指数(BMI)<25的女性(n = 282)中,f等位基因与较低的髋部BMD(p < 0.001)和前臂BMD(p = 0.001)相关,b等位基因与较低的脊柱BMD(p = 0.02)相关。将相同基因型的瘦/正常体重女性与超重/肥胖女性进行比较,FF女性在所有测量部位的BMD相似,而Ff和ff女性的BMD正如预期的那样,超重/肥胖女性更高。对于BsmI多态性也发现了类似结果,BB女性的BMI组之间BMD没有差异。根据膳食钙摄入量分组并未揭示任何基因型与BMD的关联。这些结果提供了一些证据,表明非遗传因素,特别是BMI,对VDR基因型与BMD之间的关联具有调节作用。高BMI可能预防与f或b等位基因相关的较低BMD。在某些基因型(FF和BB)中,BMI对BMD的影响相对较小。

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