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雌激素受体α变体与女性脂蛋白大小分布及颗粒水平相关:弗雷明汉心脏研究

Estrogen receptor-alpha variants are associated with lipoprotein size distribution and particle levels in women: the Framingham Heart Study.

作者信息

Demissie Serkalem, Cupples L Adrienne, Shearman Amanda M, Gruenthal Kristen M, Peter Inga, Schmid Christopher H, Karas Richard H, Housman David E, Mendelsohn Michael E, Ordovas Jose M

机构信息

Department of Biostatistics, Boston University School of Public Health, 715 Albany Street, TE425 Boston, MA 02118, USA.

出版信息

Atherosclerosis. 2006 Mar;185(1):210-8. doi: 10.1016/j.atherosclerosis.2005.06.008. Epub 2005 Jul 7.

Abstract

Plasma lipid profile is affected by endogenous estrogen levels and hormone replacement therapy (HRT). As plasma lipid concentrations have a significant heritable basis and the effects of both endogenous estrogen and use of HRT are mediated by estrogen receptors, we sought to investigate the relationships between polymorphisms in estrogen receptor-alpha (ESR1) and plasma lipid and lipoprotein concentrations. We analyzed data from 854 women (mean age 52+/-10 years) from the Framingham Heart Study. A TA repeat in the promoter region, c.30T>C in exon 1, c.454-397T>C, and c.454-351A>G in intron 1, all in linkage disequilibrium (LD), were significantly associated with low-density lipoprotein (LDL) particle size and concentration of small LDL particles. Women with the c.454-397C allele had larger LDL particle size (21.09+/-0.02 nm versus 21.01+/-0.03 nm, p=0.021) concurrent with lower small LDL particle concentration (0.47+/-0.02 mmol/L versus 0.58+/-0.03 mmol/L, p=0.008). Moreover, the TA[L]-c.30C-c.454-397C-c.454-351G haplotype (frequency, 32%) was associated with lower small LDL particle concentrations (-0.06+/-0.03 mmol/L change associated with each copy of this haplotype, p=0.011) when compared to the TA[S]-c.30T-c.454-397T-c.454-351A haplotype (frequency, 46%), where L and S are long and short TA repeats. Our results suggest that common ESR1 polymorphisms have a significant effect on lipoprotein metabolism in women.

摘要

血浆脂质谱受内源性雌激素水平和激素替代疗法(HRT)的影响。由于血浆脂质浓度有显著的遗传基础,且内源性雌激素和使用HRT的作用均由雌激素受体介导,我们试图研究雌激素受体α(ESR1)基因多态性与血浆脂质及脂蛋白浓度之间的关系。我们分析了来自弗雷明汉心脏研究的854名女性(平均年龄52±10岁)的数据。启动子区域的TA重复序列、外显子1中的c.30T>C、内含子1中的c.454 - 397T>C和c.454 - 351A>G,均处于连锁不平衡(LD)状态,与低密度脂蛋白(LDL)颗粒大小及小LDL颗粒浓度显著相关。携带c.454 - 397C等位基因的女性LDL颗粒较大(21.09±0.02纳米对21.01±0.03纳米,p = 0.021),同时小LDL颗粒浓度较低(0.47±0.02毫摩尔/升对0.58±0.03毫摩尔/升,p = 0.008)。此外,与TA[S]-c.30T-c.454 - 397T-c.454 - 351A单倍型(频率为46%)相比,TA[L]-c.30C-c.454 - 397C-c.454 - 351G单倍型(频率为32%)与较低的小LDL颗粒浓度相关(每拷贝该单倍型相关变化为-0.06±0.03毫摩尔/升,p = 0.011),其中L和S分别代表长和短的TA重复序列。我们的结果表明,常见的ESR1基因多态性对女性脂蛋白代谢有显著影响。

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