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无钾溶液诱导的离体动脉中去甲肾上腺素的释放。

Norepinephrine release in isolated arteries induced by K-free solution.

作者信息

Bonaccorsi A, Hermsmeyer K, Smith C B, Bohr D F

出版信息

Am J Physiol. 1977 Feb;232(2):H140-5. doi: 10.1152/ajpheart.1977.232.2.H140.

Abstract

Helical strips from arteries with a rich sympathetic innervation (rat tail and femoral, and dog mesenteric arteries) develop a sustained contracture when exposed to a K-free physiological salt solution (PSS). The contracture can be blocked by phentolamine and does not occur in arteries whose nerve terminals have been destroyed with 6-hydroxydopamine. The temporal relationship between force development and efflux of NE was determined. Helical strips of rat tail arteries or dog mesenteric arteries were incubated in PSS containing 1-norepinephrine-7-3H([3H]NE). They were then transferred to a superfusion system which allowed isometric recordings and collection of the superfusate for the estimation of [3H]NE content. Following exposure to a K-free PSS force development paralleled NE release and both parameters were potentiated by ouabain. These data demonstrate that this neurogenic mechanism plays a most important role in the K-free contracture of the vascular smooth muscle studied. It is in accord with the observation that NE is released by adrenergic nerves following inhibition of Na+-K+-ATPase.

摘要

来自具有丰富交感神经支配的动脉(大鼠尾巴动脉、股动脉以及犬肠系膜动脉)的螺旋条带,在暴露于无钾生理盐溶液(PSS)时会产生持续性挛缩。这种挛缩可被酚妥拉明阻断,并且在其神经末梢已被6-羟基多巴胺破坏的动脉中不会发生。测定了力量发展与去甲肾上腺素(NE)流出之间的时间关系。将大鼠尾巴动脉或犬肠系膜动脉的螺旋条带在含有1-去甲肾上腺素-7-3H([3H]NE)的PSS中孵育。然后将它们转移到一个超级灌注系统中,该系统允许进行等长记录并收集超级灌注液以估计[3H]NE含量。暴露于无钾PSS后,力量发展与NE释放平行,并且这两个参数都被哇巴因增强。这些数据表明,这种神经源性机制在所研究的血管平滑肌的无钾挛缩中起最重要作用。这与以下观察结果一致,即钠钾ATP酶受抑制后,肾上腺素能神经会释放NE。

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