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BMP2基因变异:年轻成年女性和老年女性的骨密度与超声检查

Variation in the BMP2 gene: bone mineral density and ultrasound in young adult and elderly women.

作者信息

McGuigan Fiona E, Larzenius Emma, Callreus Mattias, Gerdhem Paul, Luthman Holger, Akesson Kristina

机构信息

Clinical and Molecular Osteoporosis Research Unit, Department of Clinical Sciences Malmö, Lund University, Malmö, Sweden.

出版信息

Calcif Tissue Int. 2007 Oct;81(4):254-62. doi: 10.1007/s00223-007-9054-9. Epub 2007 Aug 29.

Abstract

Bone morphogenetic protein-2 (BMP2) plays a key role in bone formation and maintenance. Studies of polymorphisms within the gene in relation to bone mineral density (BMD) and fracture have been inconsistent. Our aim was to investigate associations between polymorphisms in the BMP2 gene and bone mass, fracture, and quantitative ultrasound (QUS) measures at different stages of skeletal development. Study subjects were participants of two population-based cohorts of Swedish women: the PEAK-25 cohort of young adult women aged 25 years (n = 993) and the OPRA cohort of elderly women aged 75 years (n = 1,001). We analyzed four single-nucleotide polymorphisms (SNPs) across the BMP2 gene including the Ser37Ala SNP previously identified in relation to BMD, QUS of the calcaneus, and, in the elderly women, fracture. BMP2 gene variations were associated with QUS of bone, independent of BMD, but only in the young women. Even after adjusting for confounding factors, SNP rs235754 in the 3' region of the gene was significantly associated with the ultrasound parameters speed of sound (P = 0.003) and stiffness (P = 0.002). The 5' SNP rs235710 showed trends for QUS parameters (P = 0.02-0.07). No association with BMP2 SNPs was observed in either cohort for either BMD or fracture. While further, more extensive genotyping across the gene is recommended, as we may not have captured all information, our preliminary data suggest that variation in BMP2 may play a previously unidentified role in aspects of bone quality, which may be age- and site-dependent.

摘要

骨形态发生蛋白2(BMP2)在骨骼形成和维持中起关键作用。关于该基因内多态性与骨密度(BMD)和骨折关系的研究结果并不一致。我们的目的是研究BMP2基因多态性与骨骼发育不同阶段的骨量、骨折及定量超声(QUS)测量值之间的关联。研究对象为瑞典女性的两个基于人群的队列参与者:25岁年轻成年女性的PEAK - 25队列(n = 993)和75岁老年女性的OPRA队列(n = 1,001)。我们分析了BMP2基因上的四个单核苷酸多态性(SNP),包括先前已确定与BMD、跟骨QUS以及老年女性骨折相关的Ser37Ala SNP。BMP2基因变异与骨QUS相关,独立于BMD,但仅在年轻女性中如此。即使在调整混杂因素后,该基因3'区域的SNP rs235754仍与超声参数声速(P = 0.003)和硬度(P = 0.002)显著相关。5' SNP rs235710在QUS参数方面显示出趋势(P = 0.02 - 0.07)。在两个队列中,未观察到BMP2 SNP与BMD或骨折之间存在关联。虽然建议对该基因进行进一步更广泛的基因分型,因为我们可能未获取所有信息,但我们的初步数据表明,BMP2的变异可能在骨质量方面发挥了先前未被识别的作用,这可能与年龄和部位有关。

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