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峰值骨量的决定因素:加拿大年轻女性队列的临床与遗传分析

Determinants of peak bone mass: clinical and genetic analyses in a young female Canadian cohort.

作者信息

Rubin L A, Hawker G A, Peltekova V D, Fielding L J, Ridout R, Cole D E

机构信息

Division of Rheumatology, Sunnybrook and Women's College Health Sciences Centre, Toronto, Ontario, Canada.

出版信息

J Bone Miner Res. 1999 Apr;14(4):633-43. doi: 10.1359/jbmr.1999.14.4.633.

Abstract

Peak bone mass has been shown to be a significant predictor of risk for osteoporosis. Previous studies have demonstrated that skeletal mass accumulation is under strong genetic control, and efforts have been made to identify candidate loci. Determinants of peak bone mass also include diet, physical activity, hormonal status, and other clinical factors. The overall contribution of these factors, genetic and nongenetic, and their interaction in determining peak bone density status have not been delineated. Six hundred and seventy-seven healthy unrelated Caucasian women ages 18-35 years were assessed. A detailed, standardized interview was conducted to evaluate lifestyle factors, menstrual and reproductive history, medical conditions, medication use, and family history of osteoporosis. Bone mineral density (BMD) was measured at the lumbar spine (L2-L4) and the femoral neck (hip) using dual-energy X-ray absorptiometry. Genotyping of the vitamin D receptor (VDR) locus at three polymorphic sites (BsmI, ApaI, and TaqI) was performed. In bivariate analyses, BMD at the lumbar spine and hip was positively correlated with weight, height, body mass index (BMI), and level of physical activity, both now and during adolescence, but negatively correlated with a family history of osteoporosis. Hip, but not spine BMD, correlated positively with dietary intake of calcium, and negatively with amenorrhea of more than 3 months, with caffeine intake, and with age. Spine, but not hip BMD, correlated positively with age and with number of pregnancies. VDR haplotype demonstrated significant associations with BMD at the hip, level of physical activity currently, and BMI. In multivariate analysis, independent predictors of greater BMD (at the hip or spine) were: age (younger for the hip, older for the spine), greater body weight, greater height (hip only), higher level of physical activity now and during adolescence, no family history of osteoporosis, and VDR genotype (hip only). Weight, age, level of physical activity, and family history are independent predictors of peak BMD. Of these factors, weight accounts for over half the explained variability in BMD. VDR alleles are significant independent predictors of peak femoral neck, but not lumbar spine BMD, even after adjusting for family history of osteoporosis, weight, age, and exercise. However, the overall contribution of this genetic determinant is modest. Taken together, these factors explained approximately 17% and 21% of the variability in peak spine and hip BMD, respectively, in our cohort. Future research should be aimed at further evaluation of genetic determinants of BMD. Most importantly, understanding the critical interactive nature between genes and the environment will facilitate development of targeted strategies directed at modifying lifestyle factors as well as earlier intervention in the most susceptible individuals.

摘要

峰值骨量已被证明是骨质疏松症风险的重要预测指标。先前的研究表明,骨骼质量积累受强大的基因控制,并且人们已努力确定候选基因座。峰值骨量的决定因素还包括饮食、身体活动、激素状态和其他临床因素。这些因素(遗传和非遗传)在决定峰值骨密度状态方面的总体贡献及其相互作用尚未明确。对677名年龄在18至35岁之间的健康无亲属关系的白人女性进行了评估。进行了详细的标准化访谈,以评估生活方式因素、月经和生殖史、医疗状况、药物使用情况以及骨质疏松症家族史。使用双能X线吸收法测量腰椎(L2 - L4)和股骨颈(髋部)的骨矿物质密度(BMD)。对维生素D受体(VDR)基因座的三个多态性位点(BsmI、ApaI和TaqI)进行基因分型。在双变量分析中,腰椎和髋部的BMD与体重、身高、体重指数(BMI)以及现在和青春期的身体活动水平呈正相关,但与骨质疏松症家族史呈负相关。髋部BMD(而非脊柱BMD)与钙的饮食摄入量呈正相关,与超过3个月的闭经、咖啡因摄入量和年龄呈负相关。脊柱BMD(而非髋部BMD)与年龄和怀孕次数呈正相关。VDR单倍型与髋部BMD、当前身体活动水平和BMI显著相关。在多变量分析中,较高BMD(髋部或脊柱)的独立预测因素为:年龄(髋部较年轻,脊柱较年长)、体重较大、身高较高(仅髋部)、现在和青春期身体活动水平较高、无骨质疏松症家族史以及VDR基因型(仅髋部)。体重、年龄、身体活动水平和家族史是峰值BMD的独立预测因素。在这些因素中,体重占BMD可解释变异性的一半以上。即使在调整骨质疏松症家族史、体重、年龄和运动因素后,VDR等位基因仍是峰值股骨颈而非腰椎BMD的显著独立预测因素。然而,这种遗传决定因素的总体贡献较小。综合来看,在我们的队列中,这些因素分别解释了峰值脊柱和髋部BMD变异性的约17%和21%。未来的研究应旨在进一步评估BMD 的遗传决定因素。最重要的是,了解基因与环境之间关键的相互作用性质将有助于制定针对性策略,以改变生活方式因素,并对最易感个体进行早期干预。

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