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首页> 美国卫生研究院文献>The Journal of Physiology >Contracting human skeletal muscle maintains the ability to blunt α1-adrenergic vasoconstriction during KIR channel and Na+/K+-ATPase inhibition
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Contracting human skeletal muscle maintains the ability to blunt α1-adrenergic vasoconstriction during KIR channel and Na+/K+-ATPase inhibition

机译:收缩人体骨骼肌可在KIR通道和Na + / K + -ATPase抑制过程中保持钝化α1-肾上腺素能血管收缩的能力

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Sympathetic vasoconstriction in contracting skeletal muscle is blunted relative to that which occurs in resting tissue; however, the mechanisms underlying this ‘functional sympatholysis’ remain unclear in humans. We tested the hypothesis that α1-adrenergic vasoconstriction is augmented during exercise following inhibition of inwardly rectifying potassium (KIR) channels and Na+/K+-ATPase (BaCl2 + ouabain). In young healthy humans, we measured forearm blood flow (Doppler ultrasound) and calculated forearm vascular conductance (FVC) at rest, during steady-state stimulus conditions (pre-phenylephrine), and after 2 min of phenylephrine (PE; an α1-adrenoceptor agonist) infusion via brachial artery catheter in response to two different stimuli: moderate (15% maximal voluntary contraction) rhythmic handgrip exercise or adenosine infusion. In Protocol 1 (n = 11 subjects) a total of six trials were performed in three conditions: control (saline), combined enzymatic inhibition of nitric oxide (NO) and prostaglandin (PG) synthesis (l-NMMA + ketorolac) and combined inhibition of NO, PGs, KIR channels and Na+/K+-ATPase (l-NMMA + ketorolac + BaCl2 + ouabain). In Protocol 2 (n = 6) a total of four trials were performed in two conditions: control (saline), and combined KIR channel and Na+/K+-ATPase inhibition. All trials occurred after local β-adrenoceptor blockade (propranolol). PE-mediated vasoconstriction was calculated (%ΔFVC) in each condition. Contrary to our hypothesis, despite attenuated exercise hyperaemia of ∼30%, inhibition of KIR channels and Na+/K+-ATPase, combined with inhibition of NO and PGs (Protocol 1) or alone (Protocol 2) did not enhance α1-mediated vasoconstriction during exercise (Protocol 1: −27 ± 3%; P = 0.2 vs. control, P = 0.4 vs.l-NMMA + ketorolac; Protocol 2: −21 ± 7%; P = 0.9 vs. control). Thus, contracting human skeletal muscle maintains the ability to blunt α1-adrenergic vasoconstriction during combined KIR channel and Na+/K+-ATPase inhibition.
机译:收缩骨骼肌的交感性血管收缩相对于静止组织中的收缩。然而,这种“功能性交感神经”的机制在人类中仍然不清楚。我们测试了以下假设,即在运动过程中,内向整流钾(KIR)通道和Na + / K + -ATPase(BaCl2 +哇巴因)被抑制后,α1-肾上腺素血管收缩增加。在年轻健康的人类中,我们测量了静息时,稳态刺激条件下(去氧肾上腺素前)和去氧肾上腺素2分钟后(PE;α1-肾上腺素受体)后的前臂血流(多普勒超声)并计算了前臂血管电导(FVC)。激动剂)通过肱动脉导管对两种不同的刺激做出反应:有规律的(最大自愿收缩为15%)节律性手法锻炼或腺苷输注。在方案1(n = 11个受试者)中,总共在三个条件下进行了六项试验:对照(盐水),一氧化氮(NO)和前列腺素(PG)合成的酶促联合抑制(1-NMMA +酮咯酸)和联合抑制NO,PG,KIR通道和Na + / K + -ATPase(1-NMMA +酮咯酸+ BaCl2 +哇巴因)的含量。在方案2(n = 6)中,总共在两个条件下进行了四项试验:对照(盐水),并结合了KIR通道和Na + / K + -ATPase抑制。所有试验均在局部β-肾上腺素受体阻滞剂(普萘洛尔)后进行。在每种情况下计算PE介导的血管收缩(%ΔFVC)。与我们的假设相反,尽管运动性充血减轻了约30%,但抑制了KIR通道和Na + / K + -ATPase,并同时抑制了NO和PGs(协议1)或单独使用(协议2)在运动期间未增强α1介导的血管收缩(协议1:−27±3%; P = 0.2 vs.对照,P = 0.4 vs.1-NMMA +酮咯酸;方案2:−21 ±7%; P = 0.9 vs.因此,收缩人体骨骼肌可在联合KIR通道和Na + / K + -ATPase抑制作用期间保持钝化α1-肾上腺素能血管收缩的能力。

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