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小鼠主动脉中的血管雌激素受体与内皮源性一氧化氮生成。性别差异及雌激素受体基因敲除的影响。

Vascular estrogen receptors and endothelium-derived nitric oxide production in the mouse aorta. Gender difference and effect of estrogen receptor gene disruption.

作者信息

Rubanyi G M, Freay A D, Kauser K, Sukovich D, Burton G, Lubahn D B, Couse J F, Curtis S W, Korach K S

机构信息

Department of Cardiovascular Research, Berlex Biosciences, Richmond, California 94804-0099, USA.

出版信息

J Clin Invest. 1997 May 15;99(10):2429-37. doi: 10.1172/JCI119426.

Abstract

The present study was designed to test the hypothesis that estrogen receptors (ER) in the blood vessel wall play a role in the modulation of the release of endothelium-derived nitric oxide (EDNO). Both basal and stimulated release of EDNO were determined in aortic rings isolated from female and male wild-type and male homozygous estrogen receptor knock-out (ERKO) mice. 125I-17beta-estradiol binding in aortic tissue showed significantly more high affinity cytosolic- nuclear-binding sites in male compared with female wildtype mice. Estrogen receptor transcripts were present in the aorta of male wild-type mice, but they were absent in male ERKO animals. Basal release of EDNO (determined by endothelium-dependent contraction caused by NG-nitro-arginine) was significantly higher in aorta of wild-type male mice compared with wild-type female mice, and significantly lower in the aorta of male ERKO compared with male wild-type mice. Acetylcholine-induced endothelium-dependent relaxation was similar in all groups studied. No difference was observed in the activity of calcium-dependent nitric oxide synthase in homogenates of lungs and brain taken from male wild-type and ERKO mice. These studies show a significant association between the number of estrogen receptors and basal release of EDNO in the aorta of mice, and suggest that decreased vascular estrogen receptor number may represent a novel risk factor for cardiovascular diseases.

摘要

本研究旨在验证血管壁中的雌激素受体(ER)在调节内皮源性一氧化氮(EDNO)释放中起作用这一假说。分别测定了从雌性和雄性野生型以及雄性纯合雌激素受体敲除(ERKO)小鼠分离的主动脉环中EDNO的基础释放和刺激释放。与雌性野生型小鼠相比,雄性主动脉组织中的125I-17β-雌二醇结合显示出更多的高亲和力胞质-核结合位点。雌激素受体转录本存在于雄性野生型小鼠的主动脉中,但在雄性ERKO动物中不存在。与野生型雌性小鼠相比,野生型雄性小鼠主动脉中EDNO的基础释放(由NG-硝基精氨酸引起的内皮依赖性收缩测定)显著更高,与雄性野生型小鼠相比,雄性ERKO小鼠主动脉中的基础释放显著更低。在所有研究组中,乙酰胆碱诱导的内皮依赖性舒张相似。在取自雄性野生型和ERKO小鼠的肺和脑匀浆中,钙依赖性一氧化氮合酶的活性未观察到差异。这些研究表明,小鼠主动脉中雌激素受体数量与EDNO基础释放之间存在显著关联,并提示血管雌激素受体数量减少可能是心血管疾病的一个新的危险因素。

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