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雌激素受体 alpha 与线粒体蛋白 HADHB 相互作用并影响β-氧化活性。

Estrogen receptor alpha interacts with mitochondrial protein HADHB and affects beta-oxidation activity.

机构信息

Department of Biological Sciences, University of Arkansas, Fayetteville, Arkansas 72701, USA.

出版信息

Mol Cell Proteomics. 2012 Jul;11(7):M111.011056. doi: 10.1074/mcp.M111.011056. Epub 2012 Feb 27.

Abstract

It is known that estrogen receptors can function as nuclear receptors and transcription factors in the nucleus and as signaling molecules in the plasma membrane. In addition, the localization of the receptors in mitochondria suggests that they may play important roles in mitochondria. In order to identify novel proteins that are involved in ERα-mediated actions of estrogens, we used a proteomic method that integrated affinity purification, two-dimensional gel electrophoresis, and mass spectrometry to isolate and identify cellular proteins that interact with ERα. One of the proteins identified was trifunctional protein β-subunit (HADHB), a mitochondrial protein that is required for β-oxidation of fatty acids in mitochondria. We have verified the interaction between ERα and HADHB by coimmunoprecipitation and established that ERα directly binds to HADHB by performing an in vitro binding assay. In addition, we have shown that ERα colocalizes with HADHB in the mitochondria by confocal microscopy, and the two proteins interact with each other within mitochondria by performing coimmunoprecipitation using purified mitochondria as starting materials. We have demonstrated that the expression of ERα affects HADHB activity, and a combination of 17β-estrodiol and tamoxifen affects the activity of HADHB prepared from human breast cancer cells that express ERα but not from the cells that are ERα deficient. Furthermore, we have demonstrated that 17β-estrodiol plus tamoxifen affects the association of ERα with HADHB in human cell extract. Our results suggest that HADHB is a functional molecular target of ERα in the mitochondria, and the interaction may play an important role in the estrogen-mediated lipid metabolism in animals and humans.

摘要

已知雌激素受体可以作为核受体和转录因子在核内发挥作用,也可以作为信号分子在质膜内发挥作用。此外,受体在线粒体中的定位表明它们可能在线粒体中发挥重要作用。为了鉴定参与 ERα 介导的雌激素作用的新蛋白,我们使用了一种蛋白质组学方法,该方法整合了亲和纯化、二维凝胶电泳和质谱,以分离和鉴定与 ERα 相互作用的细胞蛋白。鉴定出的一种蛋白质是三功能蛋白β亚基(HADHB),这是一种线粒体蛋白,是脂肪酸在线粒体中β氧化所必需的。我们通过共免疫沉淀验证了 ERα 和 HADHB 之间的相互作用,并通过体外结合测定证实 ERα 直接与 HADHB 结合。此外,我们通过共聚焦显微镜显示 ERα 与 HADHB 在线粒体中共定位,并且通过使用纯化的线粒体作为起始材料进行共免疫沉淀,证明这两种蛋白质在线粒体中相互作用。我们已经证明 ERα 的表达影响 HADHB 的活性,并且 17β-雌二醇和他莫昔芬的组合影响从表达 ERα的人乳腺癌细胞而不是从 ERα 缺乏的细胞中制备的 HADHB 的活性。此外,我们已经证明 17β-雌二醇加他莫昔芬影响人细胞提取物中 ERα 与 HADHB 的结合。我们的结果表明,HADHB 是 ERα 在线粒体中的功能性分子靶标,这种相互作用可能在动物和人类的雌激素介导的脂质代谢中发挥重要作用。

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