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首页> 美国卫生研究院文献>American Journal of Physiology - Regulatory Integrative and Comparative Physiology >Central Control of Fluid and Electrolyte Homeostasis: Norepinephrine-evoked salt-sensitive hypertension requires impaired renal sodium chloride cotransporter activity in Sprague-Dawley rats
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Central Control of Fluid and Electrolyte Homeostasis: Norepinephrine-evoked salt-sensitive hypertension requires impaired renal sodium chloride cotransporter activity in Sprague-Dawley rats

机译:流体和电解质稳态的中央控制:去甲肾上腺素诱发的盐敏感性高血压需要在Sprague-Dawley大鼠中损害肾氯化钠共转运蛋白的活性

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Recent studies have implicated a role of norepinephrine (NE) in the activation of the sodium chloride cotransporter (NCC) to drive the development of salt-sensitive hypertension. However, the interaction between NE and increased salt intake on blood pressure remains to be fully elucidated. This study examined the impact of a continuous NE infusion on sodium homeostasis and blood pressure in conscious Sprague-Dawley rats challenged with a normal (NS; 0.6% NaCl) or high-salt (HS; 8% NaCl) diet for 14 days. Naïve and saline-infused Sprague-Dawley rats remained normotensive when placed on HS and exhibited dietary sodium-evoked suppression of peak natriuresis to hydrochlorothiazide. NE infusion resulted in the development of hypertension, which was exacerbated by HS, demonstrating the development of the salt sensitivity of blood pressure [MAP (mmHg) NE+NS: 151 ± 3 vs. NE+HS: 172 ± 4; P < 0.05]. In these salt-sensitive animals, increased NE prevented dietary sodium-evoked suppression of peak natriuresis to hydrochlorothiazide, suggesting impaired NCC activity contributes to the development of salt sensitivity [peak natriuresis to hydrochlorothiazide (μeq/min) Naïve+NS: 9.4 ± 0.2 vs. Naïve+HS: 7 ± 0.1; P < 0.05; NE+NS: 11.1 ± 1.1; NE+HS: 10.8 ± 0.4). NE infusion did not alter NCC expression in animals maintained on NS; however, dietary sodium-evoked suppression of NCC expression was prevented in animals challenged with NE. Chronic NCC antagonism abolished the salt-sensitive component of NE-mediated hypertension, while chronic ANG II type 1 receptor antagonism significantly attenuated NE-evoked hypertension without restoring NCC function. These data demonstrate that increased levels of NE prevent dietary sodium-evoked suppression of the NCC, via an ANG II-independent mechanism, to stimulate the development of salt-sensitive hypertension.
机译:最近的研究表明去甲肾上腺素(NE)在氯化钠共转运蛋白(NCC)的活化中的作用,以驱动盐敏感性高血压的发展。但是,NE和盐摄入量增加与血压之间的相互作用尚待充分阐明。这项研究检查了连续NE输注对正常饮食(NS; 0.6%NaCl)或高盐饮食(HS; 8%NaCl)攻击14天的清醒Sprague-Dawley大鼠钠稳态和血压的影响。幼稚和生理盐水注射的Sprague-Dawley大鼠在置于HS上后仍保持血压正常,并且饮食中钠诱导的钠利尿峰值抑制了氢氯噻嗪。 NE输注导致高血压的发展,HS加剧了高血压的发展,表明血压对盐敏感性的发展[MAP(mmHg)NE + NS:151±3 vs. NE + HS:172±4; P <0.05]。在这些对盐敏感的动物中,NE的增加阻止了饮食中钠引起的钠利尿对氢氯噻嗪的抑制,这表明NCC活性降低有助于盐敏感性的发展[对氢氯噻嗪的利钠峰值(μeq/ min)天真的+ NS:9.4±0.2 vs朴素+ HS:7±0.1; P <0.05; NE + NS:11.1±1.1; NE + HS:10.8±0.4)。在维持NS的动物中,NE输注不会改变NCC的表达。然而,在用NE攻击的动物中,饮食中钠引起的NCC表达抑制被阻止。慢性NCC拮抗作用消除了NE介导的高血压的盐敏感性成分,而慢性ANG II 1型受体拮抗作用则在不恢复NCC功能的情况下显着减轻了NE诱发的高血压。这些数据表明,增加的NE水平可通过独立于ANG II的机制阻止饮食中钠引起的NCC抑制,从而刺激盐敏感性高血压的发生。

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