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冠状动脉和培养的主动脉平滑肌细胞表达经典雌激素受体和新发现的雌激素受体β的信使核糖核酸。

Coronary artery and cultured aortic smooth muscle cells express mRNA for both the classical estrogen receptor and the newly described estrogen receptor beta.

作者信息

Register T C, Adams M R

机构信息

Department of Comparative Medicine, Wake Forest University School of Medicine, Winston-Salem, NC 27157-1040, USA.

出版信息

J Steroid Biochem Mol Biol. 1998 Feb;64(3-4):187-91. doi: 10.1016/s0960-0760(97)00155-6.

DOI:10.1016/s0960-0760(97)00155-6
PMID:9605413
Abstract

Estrogens exhibit potent anti-atherogenic effects through mechanisms which may involve direct effects on the artery. The existence of the classical estrogen receptor (ERalpha) in vascular tissues has been established. Recently a new estrogen receptor (ERbeta) has been discovered which represents a distinct gene product with homology to the classical ERalpha. The purpose of the present study was to determine if ERbeta mRNA is expressed in vascular tissues of female and male primates. Oligonucleotide primers were developed for the specific RT-PCR amplification of ERalpha or ERbeta mRNA. RT-PCR products of the appropriate size for ERalpha and for ERbeta were observed after amplification of RNA isolated from coronary arteries of both male and female cynomolgus monkeys. Similar results were obtained from cultured aortic smooth muscle cells and from monkey reproductive tissues such as ovary and uterus. The relative expression of ERbeta to ERalpha mRNA was greatest in ovary, on the same order of magnitude in monkey vascular tissues and uterus, while the human breast cancer cell line MCF-7 exhibited a very low level of ERbeta relative to ERalpha. Sequence analysis of isolated RT-PCR products showed >95% similarity between the monkey and the published human sequences for both ERalpha and ERbeta. These findings suggest that estrogen may influence vascular gene expression not only through classical ERalpha but also through the newly described ERbeta. These findings also demonstrate the potential for targeting of these receptors in males for prevention or treatment of heart disease.

摘要

雌激素通过可能涉及对动脉直接作用的机制发挥强大的抗动脉粥样硬化作用。血管组织中经典雌激素受体(ERα)的存在已得到证实。最近发现了一种新的雌激素受体(ERβ),它是一种与经典ERα具有同源性的独特基因产物。本研究的目的是确定ERβ mRNA是否在雌性和雄性灵长类动物的血管组织中表达。开发了用于特异性RT-PCR扩增ERα或ERβ mRNA的寡核苷酸引物。从雄性和雌性食蟹猴的冠状动脉分离的RNA扩增后,观察到了适合ERα和ERβ大小的RT-PCR产物。从培养的主动脉平滑肌细胞以及猴生殖组织如卵巢和子宫中也获得了类似结果。ERβ与ERα mRNA的相对表达在卵巢中最高,在猴血管组织和子宫中处于相同数量级,而人乳腺癌细胞系MCF-7相对于ERα显示出非常低水平的ERβ。对分离的RT-PCR产物进行序列分析表明,猴的ERα和ERβ与已发表的人序列之间的相似性>95%。这些发现表明,雌激素可能不仅通过经典的ERα,而且还通过新描述的ERβ影响血管基因表达。这些发现还证明了在男性中靶向这些受体以预防或治疗心脏病的潜力。

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