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U46619、内皮素-1或去氧肾上腺素诱导的细胞钙轮廓变化及对大鼠加压阻力动脉收缩的钙致敏作用的比较。

Comparison of U46619-, endothelin-1- or phenylephrine-induced changes in cellular Ca2+ profiles and Ca2+ sensitisation of constriction of pressurised rat resistance arteries.

作者信息

Shaw Linda, O'Neill Stephen, Jones Carolyn J P, Austin Clare, Taggart Michael J

机构信息

Smooth Muscle Physiology Group, Cardiovascular Research, University of Manchester, Manchester.

出版信息

Br J Pharmacol. 2004 Feb;141(4):678-88. doi: 10.1038/sj.bjp.0705647. Epub 2004 Jan 26.

Abstract
  1. In pressurised rat mesenteric small arteries (50 mmHg), we examined the effects of stimulation with U46619, endothelin-1 (ET-1) or phenylephrine (PE) on changes in vessel diameter, global Ca(2+), individual smooth muscle cell Ca(2+) and Ca(2+)-sensitisation of contraction. 2. U46619 or ET-1 gave tonic diameter reductions, whereas PE-stimulated vessels gave tonic contractions or initial vasoconstrictions followed by diameter oscillations. Global Ca(2+) changes were transient for each agonist, with tonic constrictions being accompanied by maintained submaximal global Ca(2+) levels. 3. U46619, ET-1 or PE tonic constrictions were accompanied by apparently asynchronous Ca(2+) waves in individual smooth muscle cells of the vessel wall, as examined by confocal fluorescent microscopy. In vessels exhibiting vasomotion to PE, some apparent synchrony of activation of individual cells was evident; however, this was incomplete with many cells responding out of phase with their neighbours. 4. In alpha-toxin-permeabilised preparations, agonist-induced Ca(2+)-sensitisation of constriction at submaximal Ca(2+) (pCa6.7) in the presence of GTP was greater with U46619 or ET than PE. 5. We conclude that, in pressurised mesenteric arteries, (i) a general feature of receptor-coupled constriction is the generation of periodic smooth muscle Ca(2+) waves; (ii) complete synchrony of Ca(2+) oscillations between smooth muscle cells is not a prerequisite for receptor-coupled vasomotion; (iii) varied Ca(2+)-sensitising actions of agonists may partly determine tonic or phasic vessel responses to different stimuli.
摘要
  1. 在压力为50 mmHg的大鼠肠系膜小动脉中,我们研究了用U46619、内皮素-1(ET-1)或去氧肾上腺素(PE)刺激对血管直径变化、整体细胞内钙离子浓度(Ca(2+))、单个平滑肌细胞内钙离子浓度(Ca(2+))以及收缩的钙敏化作用的影响。2. U46619或ET-1引起血管直径持续性减小,而PE刺激的血管则产生持续性收缩或初始血管收缩,随后出现直径振荡。每种激动剂引起的整体细胞内钙离子浓度变化都是短暂的,持续性收缩伴随着整体细胞内钙离子浓度维持在亚最大水平。3. 通过共聚焦荧光显微镜检查发现,U46619、ET-1或PE引起的持续性收缩伴随着血管壁单个平滑肌细胞内明显不同步的钙离子波。在对PE产生血管运动的血管中,单个细胞激活存在一定的同步性;然而,这种同步并不完全,许多细胞与相邻细胞的反应不同步。4. 在α-毒素通透的标本中,在存在GTP的情况下,U46619或ET引起的激动剂诱导的亚最大钙离子浓度(pCa6.7)下收缩的钙敏化作用比PE更强。5. 我们得出结论,在压力作用下的肠系膜动脉中,(i)受体偶联收缩的一个普遍特征是产生周期性的平滑肌细胞内钙离子波;(ii)平滑肌细胞之间钙离子振荡的完全同步不是受体偶联血管运动的先决条件;(iii)激动剂不同的钙敏化作用可能部分决定血管对不同刺激的持续性或阶段性反应。

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