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雌激素受体β在小窝中有非基因组作用。

ERbeta has nongenomic action in caveolae.

作者信息

Chambliss Ken L, Yuhanna Ivan S, Anderson Richard G W, Mendelsohn Michael E, Shaul Philip W

机构信息

Department of Pediatrics, University of Texas Southwestern Medical Center, Dallas, Texas 75390, USA.

出版信息

Mol Endocrinol. 2002 May;16(5):938-46. doi: 10.1210/mend.16.5.0827.

Abstract

ERalpha and ERbeta serve classically as transcription factors, and ERalpha also mediates nongenomic responses to E2 such as the activation of endothelial nitric oxide synthase (eNOS). In contrast, the nongenomic capacities of endogenous ERbeta are poorly understood. We evaluated eNOS activation by E2 in cultured endothelial cells that express endogenous ERbeta to determine whether the ERbeta isoform has nongenomic action and to reveal the subcellular locale of that function. A subpopulation of ERbeta was localized to the endothelial cell plasma membrane, overexpression of ERbeta enhanced rapid eNOS stimulation by E2, and the response to endogenous ER activation was inhibited by the ERbeta-selective antagonist RR-tetrahydrochrysene (THC). eNOS activation through ERbeta was reconstituted and shown to occur independent of ERalpha in COS-7 cells, and ERbeta protein in COS-7 was directed to the plasma membrane. THC also blunted E2 activation of eNOS in isolated endothelial cell plasma membranes. Furthermore, ERbeta protein was detected and THC attenuated E2 stimulation of eNOS in isolated endothelial cell caveolae, and functional ERbeta-eNOS coupling was recapitulated in caveolae from transfected COS-7 cells. These findings in the ER-eNOS signaling paradigm indicate that endogenous ERbeta has nongenomic action in caveolae.

摘要

雌激素受体α(ERα)和雌激素受体β(ERβ)传统上作为转录因子发挥作用,并且ERα还介导对雌二醇(E2)的非基因组反应,如内皮型一氧化氮合酶(eNOS)的激活。相比之下,内源性ERβ的非基因组能力却知之甚少。我们评估了E2在表达内源性ERβ的培养内皮细胞中对eNOS的激活作用,以确定ERβ亚型是否具有非基因组作用,并揭示该功能的亚细胞定位。ERβ的一个亚群定位于内皮细胞质膜,ERβ的过表达增强了E2对eNOS的快速刺激作用,并且ERβ选择性拮抗剂RR-四氢菊烯(THC)抑制了对内源性ER激活的反应。在COS-7细胞中重建了通过ERβ激活eNOS的过程,并且表明其发生独立于ERα,并且COS-7中的ERβ蛋白定位于质膜。THC也减弱了分离的内皮细胞质膜中E2对eNOS的激活作用。此外,在分离的内皮细胞小窝中检测到了ERβ蛋白,并且THC减弱了E2对eNOS的刺激作用,并且在转染的COS-7细胞的小窝中重现了功能性ERβ-eNOS偶联。在ER-eNOS信号传导模式中的这些发现表明内源性ERβ在小窝中具有非基因组作用。

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