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希腊绝经前后女性雌激素受体β基因多态性与脊柱骨密度的相关性

Correlation of estrogen receptor beta gene polymorphisms with spinal bone mineral density in peri- and post-menopausal Greek women.

作者信息

Efstathiadou Z, Koukoulis G, Stakias N, Challa A, Zintzaras E, Tsatsoulis A

机构信息

Division of Endocrinology, Department of Internal Medicine, University of Ioannina School of Medicine, 45110 Ioannina, Greece.

出版信息

Maturitas. 2006 Mar 20;53(4):380-5. doi: 10.1016/j.maturitas.2005.07.005. Epub 2005 Aug 24.

Abstract

Estrogens play a significant role in bone physiology. Their action is mainly exerted through their receptors. Estrogen receptor alpha (ERalpha) plays a major role in bone homeostasis and there is evidence suggesting that estrogen receptor beta (ERbeta) has also an effect on BMD. We investigated the possible effect of two ERbeta gene polymorphisms on spinal bone mineral density (BMD) and metabolic bone markers in Greek women. Spine BMD as well as biochemical bone markers were measured in 147 healthy peri- and post-menopausal women [mean age (S.D.) 54 (7.9) years]. Genotyping was performed for two restriction fragment length polymorphisms (RFLPs) of ERbeta gene, RsaI in exon 5 and AluI in exon 8. For each polymorphism studied the cohort was divided into two groups: the "wild-type" group (RR and AA, respectively) and the "carrier" group including subjects with at least one allele with the restriction site (Rr&rr and Aa&aa, respectively). The distribution of RsaI genotypes was RR: 91.2% (n = 134), Rr: 8.2% (n = 12), and rr: 0.6% (n = 1) and of AluI genotypes AA: 36.7% (n = 54), Aa: 57.2% (n = 84), and aa: 6.1% (n = 9). No linkage disequilibrium was found between the two polymorphic sites studied. Spine BMD did not differ significantly in the two groups of either polymorphism, after adjusting for age, weight, height, and years since menopause [mean BMD (S.D.) for RR 0.841 (0.17) g/cm(2) versus Rr&rr 0.798 (0.13) g/cm(2), p = 0.25, and mean BMD (S.D.) for AA 0.828 (0.16)g/cm(2) versus Aa&aa 0.848 (0.17) g/cm(2), p = 0.32]. No significant differences were noted in metabolic bone markers except for a marginal difference of RR versus Rr/rr in urinary hydroxyproline/creatinine ratio [median (IQR) 3.88 (6.04) micromol/mmol in RR versus 8.2 (4.32) micromol/mmol in Rr/rr, p = 0.05]. Furthermore, no interaction between the two polymorphisms on BMD was found. In conclusion, in a Greek female post-menopausal population, the two ERbeta gene polymorphisms were not associated with BMD, or metabolic bone markers.

摘要

雌激素在骨骼生理中发挥着重要作用。其作用主要通过其受体发挥。雌激素受体α(ERα)在骨骼稳态中起主要作用,有证据表明雌激素受体β(ERβ)对骨密度(BMD)也有影响。我们研究了希腊女性中ERβ基因的两种多态性对脊柱骨矿物质密度(BMD)和代谢性骨标志物的可能影响。对147名健康的围绝经期和绝经后女性[平均年龄(标准差)54(7.9)岁]测量了脊柱BMD以及生化骨标志物。对ERβ基因的两个限制性片段长度多态性(RFLP)进行基因分型,即外显子5中的RsaI和外显子8中的AluI。对于所研究的每种多态性,将队列分为两组:“野生型”组(分别为RR和AA)和“携带者”组,包括至少有一个带有限制性位点等位基因的受试者(分别为Rr&rr和Aa&aa)。RsaI基因型的分布为RR:91.2%(n = 134),Rr:8.2%(n = 12),rr:0.6%(n = 1);AluI基因型的分布为AA:36.7%(n = 54),Aa:57.2%(n = 84),aa:6.1%(n = 9)。在所研究的两个多态性位点之间未发现连锁不平衡。在调整年龄、体重、身高和绝经后年限后,两种多态性的两组之间脊柱BMD均无显著差异[RR组的平均BMD(标准差)为0.841(0.17)g/cm²,Rr&rr组为0.798(0.13)g/cm²,p = 0.25;AA组的平均BMD(标准差)为0.828(0.16)g/cm²,Aa&aa组为0.848(0.17)g/cm²,p = 0.32]。除了尿羟脯氨酸/肌酐比值中RR与Rr/rr存在微小差异外[RR组中位数(四分位间距)为3.88(6.04)μmol/mmol,Rr/rr组为8.2(4.32)μmol/mmol,p = 0.05],代谢性骨标志物未发现显著差异。此外,未发现两种多态性对BMD有相互作用。总之,在希腊绝经后女性人群中,两种ERβ基因多态性与BMD或代谢性骨标志物无关。

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