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气道平滑肌的神经支配。传出机制。

Innervation of airway smooth muscle. Efferent mechanisms.

作者信息

Andersson R G, Grundström N

出版信息

Pharmacol Ther. 1987;32(2):107-30. doi: 10.1016/0163-7258(87)90055-6.

Abstract

The classical view, with one excitatory (cholinergic) and one inhibitory (noradrenergic) component, of the innervation of airway smooth muscle is incomplete and at least two other, possibly peptidergic, types of innervation must be included when the innervation of airways is considered. A summary of these neuronal components is given in Fig. 1 and their possible origin is outlined. Besides the inhibitory noradrenergic innervation of the airways observed in some species, an inhibitory NANC (i-NANC) innervation has been demonstrated. The polypeptide, VIP, seems to be the most likely candidate for the neurotransmitter in the i-NANC innervation of the airways. The excitatory cholinergic innervation is present in the airways from the trachea down to the peripheral bronchi. In the guinea-pig bronchi an excitatory NANC (e-NANC) innervation has been demonstrated as well. The e-NANC nerves may correspond to chemosensitive primary afferent nerves with substance P or a related tachykinin as transmitter. When the innervation of airway smooth muscle of different mammalian species is compared it is evident that all nerve components except the cholinergic, show a considerable variability among species. The cholinergic innervation seems to be present in all mammalian species whereas the other components may be completely absent from some species. Distinct regional variations in the innervation of the airways may occur, which is exemplified by the distribution of the autonomic innervation in the guinea-pig tracheo-bronchial tree. Cholinergic neurotransmission in for example the guinea-pig and human airways can be modulated by NA via prejunctional inhibitory alpha 2-adrenoceptors. Furthermore, the e-NANC neurotransmission in the guinea-pig airways may be modulated by NA or by selective alpha 2-adrenoceptor agonists, acting via prejunctional inhibitory alpha 2-adrenoceptors. The clinical importance of the NANC innervation in relation to asthma is discussed. The i-NANC nerves may exert a modulating effect on bronchoconstriction, and a functional defect would presumably lead to an exaggerated response to constrictor stimuli. The e-NANC nerves in the airways may also be clinically relevant since the transmitter (tachykinins) from these nerves can produce bronchoconstriction and promote inflammation of the airway epithelium, either by direct mechanisms or indirectly by activation of mast cells, and thus contribute to the features of asthma.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

关于气道平滑肌神经支配的传统观点,即由一个兴奋性(胆碱能)和一个抑制性(去甲肾上腺素能)成分构成,是不完整的。在考虑气道神经支配时,必须纳入至少另外两种可能为肽能的神经支配类型。图1总结了这些神经成分,并概述了它们可能的起源。除了在某些物种中观察到的气道抑制性去甲肾上腺素能神经支配外,还证实了一种抑制性非肾上腺素能非胆碱能(i-NANC)神经支配。多肽血管活性肠肽(VIP)似乎是气道i-NANC神经支配中神经递质的最可能候选者。兴奋性胆碱能神经支配存在于从气管到外周支气管的气道中。在豚鼠支气管中也证实了一种兴奋性非肾上腺素能非胆碱能(e-NANC)神经支配。e-NANC神经可能对应于以P物质或相关速激肽作为递质的化学敏感初级传入神经。当比较不同哺乳动物物种气道平滑肌的神经支配时,很明显除胆碱能外的所有神经成分在物种间存在相当大的变异性。胆碱能神经支配似乎存在于所有哺乳动物物种中,而其他成分在某些物种中可能完全不存在。气道神经支配可能会出现明显的区域差异,豚鼠气管支气管树中自主神经支配的分布就是一个例子。例如,豚鼠和人类气道中的胆碱能神经传递可通过节前抑制性α2肾上腺素能受体被去甲肾上腺素(NA)调节。此外,豚鼠气道中的e-NANC神经传递可能被NA或选择性α2肾上腺素能受体激动剂通过节前抑制性α2肾上腺素能受体调节。讨论了NANC神经支配与哮喘相关的临床重要性。i-NANC神经可能对支气管收缩发挥调节作用,功能缺陷可能会导致对收缩刺激的过度反应。气道中的e-NANC神经在临床上可能也相关,因为这些神经的递质(速激肽)可通过直接机制或通过激活肥大细胞间接产生支气管收缩并促进气道上皮炎症,从而导致哮喘症状。(摘要截短至400字)

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