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血管活性肠肽是某些脑和脑外颅动脉舒张递质的证据。

Evidence that vasoactive intestinal polypeptide is a dilator transmitter to some cerebral and extracerebral cranial arteries.

作者信息

Bevan J A, Moscowitz M, Said S I, Buga G

出版信息

Peptides. 1984 Mar-Apr;5(2):385-8. doi: 10.1016/0196-9781(84)90239-0.

Abstract

Many arteries of the head upon electrical stimulation of the non-adrenergic nerve terminals present in their wall exhibit dilation that is only partially reduced by atropine. The results of three types of experiments are presented that tend to implicate vasoactive intestinal polypeptide (VIP) a known vasodilator, as an atropine-resistant dilator transmitter. VIP activity is high in vessels that exhibit neurogenic dilation and low in those that do not. It is released from two arteries that show such dilation upon neurogenic field stimulation and VIP antiserum reduces neurogenic dilation. It is proposed that VIP as well as acetylcholine are released from the innervation of some cranial arteries and together in a number of animals of least are responsible for part of the complex neurogenic dilation witnessed in these vessels. Although substance P is present in nerves found within the wall of cerebral and other cranial blood vessels, it is either ineffective as a dilator in vessels that show a sizeable dilation to electrical stimulation, or else exhibits marked, rapid, persistent tachyphylaxis.

摘要

对头部许多动脉壁上存在的非肾上腺素能神经末梢进行电刺激时,这些动脉会出现扩张,而阿托品只能部分减弱这种扩张。本文展示了三种类型的实验结果,这些结果倾向于表明血管活性肠肽(VIP)(一种已知的血管扩张剂)是一种抗阿托品的扩张递质。在表现出神经源性扩张的血管中,VIP活性较高,而在未表现出神经源性扩张的血管中,VIP活性较低。它从两条在神经源性场刺激时会出现这种扩张的动脉中释放出来,并且VIP抗血清会减弱神经源性扩张。有人提出,VIP以及乙酰胆碱是从一些颅动脉的神经支配中释放出来的,至少在一些动物中,它们共同负责这些血管中所观察到的部分复杂神经源性扩张。尽管P物质存在于脑和其他颅血管壁内的神经中,但它要么在对电刺激有明显扩张反应的血管中作为扩张剂无效,要么表现出明显、快速、持续的快速耐受性。

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