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老年绝经后女性中维生素D受体、雌激素受体和I型胶原蛋白α1基因多态性与骨质疏松性髋部骨折

Polymorphisms of the VDR, ER and COLIA1 genes and osteoporotic hip fracture in elderly postmenopausal women.

作者信息

Aerssens J, Dequeker J, Peeters J, Breemans S, Broos P, Boonen S

机构信息

Arthritis and Metabolic Bone Disease Research Unit, Division of Traumatology and Emergency Surgery, K.U. Leuven, Belgium.

出版信息

Osteoporos Int. 2000;11(7):583-91. doi: 10.1007/s001980070079.

Abstract

In view of the reported associations between osteoporosis and polymorphisms of the vitamin D receptor (VDR), collagen Ialpha1 (COLIA1) and estrogen receptor (ER) genes, an association study was performed between VDR, COLLIA1, and ER genotypes and bone mineral density, biochemical markers of bone turnover and hip fracture occurrence in Belgian older postmenopausal women. The gene polymorphisms were evaluated by restriction fragment length polymorphism analyses, using the restriction enzymes BsmI (VDR), AccB7I (COLIA1), and PvuII and XbaI (ER), respectively. As expected, bone mineral density and biochemical analyses demonstrated significant differences between hip fracture patients and elderly controls. However, no significant differences in genotype distributions or allele frequencies were observed between the cases (n = 135, age 78 +/- 9 years) and controls (n = 239, age 76 +/- 4 years) for any of the gene polymorphisms. Stratification of both study populations according to VDR, COLIA1 or ER genotype did not reveal any statistically significant difference in bone density or bone turnover between subgroups with different genotypes. In conclusion, despite its limited statistical power the outcome of this study does not support the hypothesis of a major contribution of the VDR, COLIA1 or ER polymorphisms to explain variations in bone mineral density or bone turnover, or to identify elderly women at risk of osteoporotic hip fracture.

摘要

鉴于有报道称骨质疏松症与维生素 D 受体(VDR)、I 型胶原蛋白α1(COLIA1)和雌激素受体(ER)基因的多态性之间存在关联,我们对比利时绝经后老年女性的 VDR、COLIA1 和 ER 基因分型与骨密度、骨转换生化标志物及髋部骨折发生率进行了关联研究。分别使用限制性内切酶 BsmI(VDR)、AccB7I(COLIA1)以及 PvuII 和 XbaI(ER),通过限制性片段长度多态性分析来评估基因多态性。正如预期的那样,骨密度和生化分析显示髋部骨折患者与老年对照组之间存在显著差异。然而,对于任何一种基因多态性,病例组(n = 135,年龄 78±9 岁)和对照组(n = 239,年龄 76±4 岁)之间在基因型分布或等位基因频率上均未观察到显著差异。根据 VDR、COLIA1 或 ER 基因型对两个研究人群进行分层后,不同基因型亚组之间在骨密度或骨转换方面未发现任何统计学上的显著差异。总之,尽管本研究的统计效力有限,但其结果并不支持 VDR、COLIA1 或 ER 的多态性对解释骨密度或骨转换的变化,或对识别有骨质疏松性髋部骨折风险的老年女性起主要作用这一假设。

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