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23 个候选基因与骨密度关联的高密度多态性分析。

High-density polymorphisms analysis of 23 candidate genes for association with bone mineral density.

机构信息

Centre de Recherche de l'Hôpital St-François d'Assise du Centre hospitalier universitaire de Québec, Québec, Canada G1L 3L5.

出版信息

Bone. 2010 Nov;47(5):975-81. doi: 10.1016/j.bone.2010.06.030. Epub 2010 Jul 30.

DOI:10.1016/j.bone.2010.06.030
PMID:20654748
Abstract

Osteoporosis is a bone disease characterized by low bone mineral density (BMD), a highly heritable and polygenic trait. Women are more prone than men to develop osteoporosis due to a lower peak bone mass and accelerated bone loss at menopause. Peak bone mass has been convincingly shown to be due to genetic factors with heritability up to 80%. Menopausal bone loss has been shown to have around 38% to 49% heritability depending on the site studied. To have more statistical power to detect small genetic effects we focused on premenopausal women. We studied 23 candidate genes, some involved in calcium and vitamin-D regulation and others because estrogens strongly induced their gene expression in mice where it was correlated with humerus trabecular bone density. High-density polymorphisms were selected to cover the entire gene variability and 231 polymorphisms were genotyped in a first sample of 709 premenopausal women. Positive associations were retested in a second, independent, sample of 673 premenopausal women. Ten polymorphisms remained associated with BMD in the combined samples and one was further associated in a large sample of postmenopausal women (1401 women). This associated polymorphism was located in the gene CSF3R (granulocyte colony stimulating factor receptor) that had never been associated with BMD before. The results reported in this study suggest a role for CSF3R in the determination of bone density in women.

摘要

骨质疏松症是一种以骨密度低(BMD)为特征的骨骼疾病,具有高度遗传性和多基因特性。由于女性的峰值骨量较低,绝经后骨量流失加速,因此比男性更容易患上骨质疏松症。峰值骨量已被确凿证明是由遗传因素决定的,遗传率高达 80%。绝经后骨丢失的遗传率约为 38%至 49%,具体取决于研究的部位。为了有更多的统计能力来检测小的遗传效应,我们专注于绝经前妇女。我们研究了 23 个候选基因,其中一些与钙和维生素 D 的调节有关,另一些则与雌激素在小鼠中强烈诱导其基因表达有关,而这种表达与肱骨小梁骨密度相关。选择高密度多态性来覆盖整个基因变异性,并在 709 名绝经前妇女的第一个样本中对 231 个多态性进行了基因分型。在第二个独立的 673 名绝经前妇女样本中对阳性关联进行了重新测试。在合并样本中,有 10 个多态性与 BMD 相关,其中一个在一个大型绝经后妇女样本(1401 名妇女)中进一步相关。相关的多态性位于 CSF3R 基因(粒细胞集落刺激因子受体)中,该基因以前从未与 BMD 相关。本研究报告的结果表明 CSF3R 在女性骨密度的决定中起作用。

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