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首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Estrogen Receptor-β in the Paraventricular Nucleus and Rostroventrolateral Medulla Plays an Essential Protective Role in Aldosterone/Salt-Induced Hypertension in Female RatsNovelty and Significance
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Estrogen Receptor-β in the Paraventricular Nucleus and Rostroventrolateral Medulla Plays an Essential Protective Role in Aldosterone/Salt-Induced Hypertension in Female RatsNovelty and Significance

机译:室旁核和后腹外侧延髓中的雌激素受体-β在雌性大鼠醛固酮/盐诱导的高血压中起重要的保护作用

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The identification of the specific estrogen receptor (ER) subtypes that are involved in estrogen protection from hypertension and their specific locations in the central nervous system is critical to our understanding and design of effective estrogen replacement therapies in women. Using selective ER agonists and recombinant adeno-associated virus (AAV) carrying small interference (si) RNA to silence either ERα (AAV-siRNA-ERα) or ERβ (AAV-siRNA-ERβ), the present study investigated regional specificity of different ER subtypes in the protective actions of estrogen in aldosterone (Aldo)-induced hypertension. Intracerebroventricular infusions of either diarylpropionitrile, a selective ERβ agonist, or propyl-pyrazole-triol, a selective ERα agonist, attenuated Aldo/NaCl-induced hypertension in ovariectomized rats. In contrast, intracerebroventricular injections of siRNA-ERα or siRNA-ERβ augmented Aldo-induced hypertension in intact females. Site-specific paraventricular nucleus (PVN) or rostroventrolateral medulla (RVLM) injections of siRNA-ERβ augmented Aldo-induced hypertension. However, rats with PVN or RVLM injections of siRNA-ERα did not significantly increase blood pressure induced by Aldo. Real-time polymerase chain reaction analyses of the PVN and RVLM of siRNA-injected rat confirmed a marked reduction in the expression of ERα and ERβ. In cultured PVN neurons, silencing either ERα or ERβ by culturing PVN neurons with siRNA-ERα or siRNA-ERβ enhanced Aldo-induced reactive oxygen species production. Ganglionic blockade after Aldo infusion showed an increase in sympathetic activity in ERβ knockdown rats. These results indicate that both PVN and RVLM ERβ, but not ERα in these nuclei, contribute to the protective effects of estrogen against Aldo-induced hypertension. The brain regions responsible for the protective effects of estrogen interaction with ERα in Aldo-induced hypertension still need to be determined.
机译:识别参与抗高血压的雌激素保护作用的特定雌激素受体(ER)亚型及其在中枢神经系统中的特定位置对于我们理解和设计女性有效的雌激素替代疗法至关重要。本研究使用选择性ER激动剂和携带小干扰(si)RNA的重组腺相关病毒(AAV)沉默ERα(AAV-siRNA-ERα)或ERβ(AAV-siRNA-ERβ),以研究不同ER的区域特异性亚型在醛固酮(醛固酮)诱发的高血压中对雌激素的保护作用中。选择性ERβ激动剂二芳基丙腈或选择性ERα激动剂丙基吡唑三醇的脑室内灌注可减轻卵巢切除大鼠的Aldo / NaCl诱导的高血压。相反,脑室内注射siRNA-ERα或siRNA-ERβ会增加完整女性的Aldo诱发的高血压。 siRNA-ERβ的部位特异性脑室旁核(PVN)或rostroventrolateral延髓(RVLM)注射增加Aldo诱发的高血压。然而,PVN或RVLM注射siRNA-ERα的大鼠并没有明显增加Aldo诱发的血压。 siRNA注射的大鼠的PVN和RVLM的实时聚合酶链反应分析证实了ERα和ERβ表达的明显降低。在培养的PVN神经元中,通过与siRNA-ERα或siRNA-ERβ培养PVN神经元使ERα或ERβ沉默,可以增强Aldo诱导的活性氧的产生。 Aldo输注后的神经节阻滞显示ERβ敲低大鼠的交感神经活动增加。这些结果表明,PVN和RVLMERβ都参与了雌激素对Aldo诱发的高血压的保护作用,而这些核中的ERα却没有。还需要确定负责雌激素与ERα相互作用对Aldo诱发的高血压的保护作用的大脑区域。

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