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Electrical dynamics of isolated cerebral and skeletal muscle endothelial tubes: Differential roles of G‐protein‐coupled receptors and K+ channels

机译:分离的大脑和骨骼肌内皮管的电动力学:G蛋白偶联受体和K +通道的差异作用

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摘要

Electrical dynamics of freshly isolated cerebral endothelium have not been determined independently of perivascular nerves and smooth muscle. We tested the hypothesis that endothelium of cerebral and skeletal muscle arteries differentially utilizes purinergic and muscarinic signaling pathways to activate endothelium‐derived hyperpolarization. Changes in membrane potential (V m) were recorded in intact endothelial tubes freshly isolated from posterior cerebral and superior epigastric arteries of male and female C57BL/6 mice (age: 3‐8 months). V m was measured in response to activation of purinergic (P2Y) and muscarinic (M3) receptors in addition to small‐ and intermediate‐conductance Ca2+‐activated K+ (SKC a/IKC a) and inward rectifying K+ (KIR) channels using ATP (100 μmol·L−1), acetylcholine (ACh; 10 μmol·L−1), NS309 (0.01‐10 μmol·L−1), and 15 mmol·L−1 KCl, respectively. Intercellular coupling was demonstrated via transfer of propidium iodide dye and electrical current (±0.5‐3 nA) through gap junctions. With similarities observed across gender, peak hyperpolarization to ATP and ACh in skeletal muscle endothelial tubes was ~twofold and ~sevenfold higher, respectively, vs cerebral endothelial tubes, whereas responses to NS309 were similar (from resting V m ~−30 mV to maximum ~−80 mV). Hyperpolarization (~8 mV) occurred during 15 mmol·L−1 KCl treatment in cerebral but not skeletal muscle endothelial tubes. Despite weaker hyperpolarization during endothelial style="fixed-case">GPCR stimulation in cerebral vs skeletal muscle endothelium, the capability for robust style="fixed-case">SKC a/ style="fixed-case">IKC a activity is preserved across brain and skeletal muscle. As vascular reactivity decreases with aging and cardiovascular disease, endothelial K+ channel activity may be calibrated to restore blood flow to respective organs regardless of gender.
机译:尚未独立于血管周围神经和平滑肌确定新鲜分离的脑内皮的电动力学。我们测试了大脑和骨骼肌动脉内皮差异利用嘌呤能和毒蕈碱信号通路激活内皮衍生的超极化的假说。在刚从雄性和雌性C57BL / 6小鼠的大脑后部和上腹上动脉新鲜分离的完整内皮管中记录了膜电位(V m)的变化(年龄:3-8个月)。除了小和中等电导的Ca 2 + -活化的K + (除了嘌呤能(P2Y)和毒蕈碱(M3)受体的激活外,还测量了V m SKC a / IKC a)并使用ATP(100μmol·L -1 ),乙酰胆碱(ACh;10μmol·L + (KIR)通道> -1 ),NS309(0.01-10μmol·L -1 )和15mmol·L -1 KCl。通过间隙连接转移碘化丙啶染料和电流(±0.5-3nA)证明了细胞间的偶联。跨性别观察到的相似,骨骼肌内皮管对ATP和ACh的超极化峰值分别比脑内皮管高约两倍和约七倍,而对NS309的响应相似(从静息V m〜-30 mV到最大〜 −80 mV)。 15mmol·L −1 KCl治疗期间在大脑而非骨骼肌内皮管中发生超极化(〜8 mV)。尽管在大脑vs骨骼肌内皮细胞中,在内皮 style =“ fixed-case”> GPCR 刺激过程中超极化较弱,但强大的 style =“ fixed-case”> SKC a / <跨大脑和骨骼肌保留了一种活动。随着衰老和心血管疾病的发生,血管反应性降低,因此可以校准内皮K + 通道活性以恢复流向各个器官的血液,而不论性别。

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