Peacock Munro, Koller Daniel L, Fishburn Tonya, Krishnan Subha, Lai Dongbing, Hui Siu, Johnston C Conrad, Foroud Tatiana, Econs Michael J
Department of Medicine, Indiana University School of Medicine, University Hospital and Out Patient Center, 550 North University Boulevard, Room 5595, Indianapolis, Indiana 46202-5250, USA.
J Clin Endocrinol Metab. 2005 May;90(5):3060-6. doi: 10.1210/jc.2004-2143. Epub 2005 Mar 1.
A major determinant of osteoporotic fracture is peak bone mineral density (BMD). In women peak BMD is highly heritable and several quantitative trait loci (QTL) have been reported. There are few comparable data in men. This study in men aimed to establish the heritability of peak BMD, identify QTL contributing to normal variation in BMD, and determine which QTL might be sex specific.
BMD at the spine and hip were measured in 323 pairs of brothers aged 18-61 yr (264 white pairs; 59 black pairs). Heritability was calculated and linkage analysis performed with spine and hip BMD phenotypes.
Heritability estimates ranged from 0.61 to 0.87 and were not significantly different between white and black men. A 9-cM genome-wide scan followed by genotyping with more closely spaced markers identified suggestive QTL (logarithm of the odds > 2.2) for BMD on chromosomes 1q (spine), 2p (spine), 2q (hip), 14p (spine), 18 (hip), and 21 (hip). Comparison with published data in 774 pairs of premenopausal sisters suggested that the QTL on 1q (spine), 2q (hip), 14p (spine), and 21q (hip) were male specific, whereas those on 2p (spine) and 18 (hip) were not sex specific.
This study demonstrates that BMD in healthy men is highly heritable with similar estimates of the genetic contribution to BMD in both whites and blacks. Of the six QTL identified, three were specific for spine BMD and three were specific for hip BMD. When compared with published QTL for peak BMD in women from the same geographical region, four of the QTL appeared to be male specific. The occurrence of sex-specific genes in humans for BMD has potentially important implications for the pathogenesis and treatment of osteoporosis.
骨质疏松性骨折的一个主要决定因素是峰值骨密度(BMD)。在女性中,峰值骨密度具有高度遗传性,并且已经报道了几个数量性状基因座(QTL)。男性中类似的数据较少。这项针对男性的研究旨在确定峰值骨密度的遗传性,识别导致骨密度正常变异的QTL,并确定哪些QTL可能具有性别特异性。
对323对年龄在18至61岁之间的兄弟(264对白种人兄弟;59对黑种人兄弟)测量其脊柱和髋部的骨密度。计算遗传性,并对脊柱和髋部骨密度表型进行连锁分析。
遗传性估计值范围为0.61至0.87,白种人和黑种人男性之间无显著差异。进行了一次9厘摩(cM)的全基因组扫描,随后使用间距更近的标记进行基因分型,在1号染色体(脊柱)、2号染色体短臂(脊柱)、2号染色体长臂(髋部)、14号染色体短臂(脊柱)、18号染色体(髋部)和21号染色体(髋部)上鉴定出了提示性的骨密度QTL(优势对数>2.2)。与774对绝经前姐妹的已发表数据进行比较表明,1号染色体(脊柱)、2号染色体长臂(髋部)、14号染色体短臂(脊柱)和21号染色体长臂(髋部)上的QTL是男性特异性的,而2号染色体短臂(脊柱)和18号染色体(髋部)上的QTL不是性别特异性的。
这项研究表明,健康男性的骨密度具有高度遗传性,白种人和黑种人对骨密度的遗传贡献估计相似。在鉴定出的6个QTL中,3个对脊柱骨密度具有特异性,3个对髋部骨密度具有特异性。与来自同一地理区域的女性峰值骨密度的已发表QTL相比,其中4个QTL似乎是男性特异性的。人类中骨密度性别特异性基因的存在对骨质疏松症的发病机制和治疗具有潜在的重要意义。
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