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雌激素受体α CA二核苷酸重复多态性与围绝经期女性的骨质流失率以及绝经后女性的骨矿物质密度和骨质疏松性骨折风险相关。

Estrogen receptor alpha CA dinucleotide repeat polymorphism is associated with rate of bone loss in perimenopausal women and bone mineral density and risk of osteoporotic fractures in postmenopausal women.

作者信息

Lai B M H, Cheung C L, Luk K D K, Kung A W C

机构信息

Department of Medicine, The University of Hong Kong, Queen Mary Hospital, Pokfulam, Hong Kong, China.

出版信息

Osteoporos Int. 2008 Apr;19(4):571-9. doi: 10.1007/s00198-007-0482-1. Epub 2007 Sep 26.

DOI:10.1007/s00198-007-0482-1
PMID:17896124
Abstract

UNLABELLED

The association between a newly identified CA repeat polymorphism of the estrogen receptor alpha gene (ESR1) with osteoporosis was investigated. Postmenopausal women with <18 CA repeats had low BMD, increased rate of bone loss and increased fracture risk.

INTRODUCTION

Studies have shown that intronic dinucleotide repeat polymorphisms in some genes are associated with disease risk by modulating mRNA splicing efficiency. D6S440 is a newly identified intronic CA repeat polymorphism located downstream of the 5'-splicing site of exon 5 of ESR1.

METHODS

The associations of D6S440 with bone mineral density (BMD), rate of bone loss and fracture risk were evaluated in 452 pre-, 110 peri- and 622 postmenopausal southern Chinese women using regression models.

RESULTS

Post- but not premenopausal women with less CA repeats had lower spine and hip BMD. The number of CA repeats was linearly related to hip BMD in postmenopausal women (beta=0.008; p=0.004). Postmenopausal women with CA repeats <18 had higher risks of having osteoporosis (BMD T-score< -2.5 at the spine: OR 2.46, 95% CI 1.30-4.65; at the hip: OR 3.79(1.64-8.74)) and low trauma fractures (OR 2.31(1.29-4.14)) than those with >or= 18 repeats. Perimenopausal women with <18 CA repeats had significantly greater bone loss in 18 months at the hip than those with >or= 18 repeats (-1.96% vs. -1.61%, p = 0.029).

CONCLUSIONS

ESR1 CA repeat polymorphism is associated with BMD variation, rate of bone loss and fracture risk, and this may be a useful genetic marker for fracture risk assessment.

摘要

未标注

研究了新发现的雌激素受体α基因(ESR1)CA重复多态性与骨质疏松症之间的关联。绝经后妇女中CA重复次数<18次者骨密度低、骨质流失率增加且骨折风险增加。

引言

研究表明,某些基因中的内含子二核苷酸重复多态性通过调节mRNA剪接效率与疾病风险相关。D6S440是新发现的位于ESR1外显子5的5'-剪接位点下游的内含子CA重复多态性。

方法

采用回归模型对452名绝经前、110名围绝经期和622名绝经后中国南方女性评估D6S440与骨密度(BMD)、骨质流失率和骨折风险的关联。

结果

绝经后而非绝经前妇女中,CA重复次数较少者脊柱和髋部骨密度较低。绝经后妇女中CA重复次数与髋部骨密度呈线性相关(β=0.008;p=0.004)。CA重复次数<18次的绝经后妇女患骨质疏松症(脊柱BMD T值<-2.5:比值比2.46,95%可信区间1.30-4.65;髋部:比值比3.79(1.64-8.74))和低创伤性骨折(比值比2.31(1.29-4.14))的风险高于CA重复次数≥18次者。围绝经期妇女中CA重复次数<18次者髋部在18个月内的骨质流失明显多于CA重复次数≥18次者(-1.96%对-1.61%,p=0.029)。

结论

ESR1 CA重复多态性与骨密度变化、骨质流失率和骨折风险相关,这可能是骨折风险评估的一个有用的遗传标志物。

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