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弗雷明汉心脏研究中掌骨大小和形态的全基因组连锁扫描。

A genome wide linkage scan of metacarpal size and geometry in the Framingham Study.

作者信息

Karasik David, Shimabuku Nicole A, Zhou Yanhua, Zhang Yuqing, Cupples L Adrienne, Kiel Douglas P, Demissie Serkalem

机构信息

Hebrew SeniorLife Institute for Aging Research and Harvard Medical School, Boston, Massachusetts 02131, USA.

出版信息

Am J Hum Biol. 2008 Nov-Dec;20(6):663-70. doi: 10.1002/ajhb.20791.

Abstract

Bone geometry is a significant component of bone strength, and has a clinical utility in predicting fractures and quantifying bone loss. Bone geometry is known to have a substantial genetic component. We performed linkage analysis to identify chromosomal regions governing metacarpal bone geometry. A genome-wide scan (with a set of 615 markers with spacing of approximately 5.7 cM) was performed on 1,702 individuals from 330 extended families of the Framingham Study. Midshaft width was measured and several indices calculated, namely Metacarpal Cortical Thickness (MCT), Cortical Index (MCI), and Section Modulus (MZ), using digitized X-rays of 1,380 participants (men, n = 666, mean age 55.2 yr, women, n = 714, 55.5 yr). Metacarpals 2, 3, and 4 were averaged. Heritability was significant for all indices, ranging from 0.51 to 0.72. Linkage analysis of indices adjusted for age, age(2), and estrogen status in women, identified chromosomal regions 6p21, 9p21, 11q21-q22, and Xq26-Xq27, with LOD scores >2.0. Additional adjustment for smoking, height, and BMI, generally reduced the LOD scores. Finally, bivariate linkage analysis confirmed that a QTL on chr. 6 (51 cM) was shared by midshaft width and MZ (LOD = 2.40, adjusted for all covariates). Neither MCT nor MCI shared linkage loci with width or MZ. In conclusion, we have identified chromosomal regions potentially linked to bone geometry. Genes in these regions may regulate bone geometry via effects on body size. Identification and subsequent characterization of loci for bone geometry can further elucidate the genetic contributions to bone's resistance to stress.

摘要

骨几何形态是骨强度的重要组成部分,在预测骨折和量化骨质流失方面具有临床应用价值。已知骨几何形态具有很大的遗传成分。我们进行连锁分析以确定控制掌骨几何形态的染色体区域。对弗雷明汉心脏研究中330个大家庭的1702名个体进行了全基因组扫描(使用一组间距约为5.7厘摩的615个标记)。测量了1380名参与者(男性,n = 666,平均年龄55.2岁;女性,n = 714,55.5岁)掌骨干中部宽度并计算了几个指标,即掌骨皮质厚度(MCT)、皮质指数(MCI)和截面模量(MZ),对第2、3和4掌骨进行了平均。所有指标的遗传力均显著,范围为0.51至0.72。对年龄、年龄平方和女性雌激素状态进行校正后的指标连锁分析,确定了染色体区域6p21、9p21、11q21 - q22和Xq26 - Xq27,其对数优势分数(LOD)>2.0。对吸烟、身高和体重指数进行进一步校正后,通常会降低LOD分数。最后,双变量连锁分析证实,6号染色体上51厘摩处的一个数量性状基因座(QTL)为掌骨干中部宽度和MZ所共有(LOD = 2.40,对所有协变量进行了校正)。MCT和MCI均未与宽度或MZ共享连锁位点。总之,我们确定了可能与骨几何形态相关的染色体区域。这些区域中的基因可能通过对体型的影响来调节骨几何形态。确定并随后表征骨几何形态的基因座可进一步阐明基因对骨抗应力能力的贡献。

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