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Genetics of Osteoporosis

机译:骨质疏松症的遗传学

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Osteoporosis is a common disease with a strong genetic component characterized by reduced bone mass, defects in the microarchitecture of bone tissue, and an increased risk of fragility fractures. Twin and family studies have shown high heritability of bone mineral density (BMD) and other determinants of fracture risk such as ultrasound properties of bone, skeletal geometry, and bone turnover. Osteoporotic fractures also have a heritable component, but this reduces with age as environmental factors such as risk of falling come into play. Susceptibility to osteoporosis is governed by many different genetic variants and their interaction with environmental factors such as diet and exercise. Notable successes in identification of genes that regulate BMD have come from the study of rare Mendelian bone diseases characterized by major abnormalities of bone mass where variants of large effect size are operative. Genome-wide association studies have also identified common genetic variants of small effect size that contribute to regulation of BMD and fracture risk in the general population. In many cases, the loci and genes identified by these studies had not previously been suspected to play a role in bone metabolism. Although there has been extensive progress in identifying the genes and loci that contribute to the regulation of BMD and fracture over the past 15 yr, most of the genetic variants that regulate these phenotypes remain to be discovered.
机译:骨质疏松症是一种常见的疾病,具有很强的遗传成分,其特征是骨量减少,骨组织的微结构缺陷以及脆性骨折的风险增加。孪生和家族研究表明,骨矿物质密度(BMD)具有很高的遗传力,而骨折风险的其他决定因素,例如骨骼的超声特性,骨骼几何形状和骨骼更新。骨质疏松性骨折也具有可遗传的成分,但随着年龄的增长,诸如跌倒的风险等环境因素开始发挥作用,这种情况会减少。骨质疏松症的易感性由许多不同的遗传变异及其与环境因素(如饮食和运动)的相互作用所决定。鉴定可调节BMD的基因方面的显著成功来自对罕见孟德尔骨骼疾病的研究,该疾病的特征是骨量严重异常,其中有较大效应大小的变异体在起作用。全基因组关联研究还确定了影响范围较小的常见遗传变异,这些变异有助于调节普通人群的骨密度和骨折风险。在许多情况下,这些研究鉴定出的基因座和基因以前没有被怀疑在骨代谢中起作用。尽管在过去15年中鉴定有助于BMD和骨折调控的基因和基因座方面已取得了广泛的进展,但调控这些表型的大多数遗传变异仍待发现。

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