首页> 外文期刊>Autonomic neuroscience: basic & clinical >Sensory receptors in the airways: neurochemical coding of smooth muscle-associated airway receptors and pulmonary neuroepithelial body innervation.
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Sensory receptors in the airways: neurochemical coding of smooth muscle-associated airway receptors and pulmonary neuroepithelial body innervation.

机译:气道中的感觉受体:平滑肌相关气道受体和肺神经上皮体神经支配的神经化学编码。

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Mainly due to the lack of conclusive morphological data, correlation between functionally and morphologically defined lung receptors has so far been unsatisfactory. In the present study, multiple immunocytochemical stainings with a panel of markers for (mechanso)sensory nerve fibres were performed in order to visualise putative receptor terminals in rat intrapulmonary airways. We first focussed on determining the location, morphology and neurochemical coding of subepithelial receptor-like structures that have been sporadically reported in the wall of large diameter airways. Immunostaining with antibodies against Na+/K+-ATPase alpha3, vesicular glutamate transporter 1 (VGLUT1) and VGLUT2 revealed branching laminar subepithelial receptor endings associated with airway smooth muscle. The latter nerve terminals appeared to further express calbindin D28k (CB), and the ATP receptor P2X3, but were calcitonin gene-related peptide (CGRP)-negative. The nerve fibres that give rise to these terminals were shown tobe myelinated and have a vagal sensory origin. Because of the close association between the laminar terminals of this receptor-like structures and airway smooth muscle, we will further refer to these clearly morphologically identifiable sensory end organs as 'smooth muscle-associated airway receptors (SMARs)'. Secondly, we further explored the sensory innervation of pulmonary neuroepithelial bodies (NEBs). NEBs are intraepithelial groups of neuroendocrine cells, contacted by several nerve fibre populations, at least three of which are sensory. The spinal sensory innervation of NEBs expresses CGRP and substance P, contacts NEBs at their basal pole, and is capsaicin-sensitive. The intraepithelial vagal sensory innervation of NEBs, on the other hand, appears to be myelinated and could be labelled by antibodies against VGLUT1, VGLUT2, CB and P2X3 receptors. Na+/K+-ATPase alpha3 immunostaining additionally labelled part of the vagal sensory innervation of rat pulmonary NEBs. The neurochemical coding and receptor-like appearance of SMARs and of the complex vagal sensory innervation of NEBs appeared to be almost identical and reminiscent of mechanosensors. Both SMARs and vagal nodose nerve terminals in NEBs therefore likely represent the morphological counterparts of subgroups of the extensive population of physiologically characterised myelinated vagal airway receptors, the majority of which are mechanosensitive. Electrophysiological data based on 'local' stimuli should be interpreted with caution, because of the regular close apposition of SMARs and NEBs and the very similar characteristics of their nerve terminals.
机译:主要由于缺乏确定的形态学数据,迄今为止,在功能上和形态学上定义的肺受体之间的相关性还不能令人满意。在本研究中,进行了多种(细胞)感觉神经纤维标记物的免疫细胞化学染色,以观察大鼠肺气道中假定的受体末端。我们首先集中于确定上皮下受体样结构的位置,形态和神经化学编码,这些结构在大口径气道壁中偶发报道。用抗Na + / K + -ATPaseα3,水泡谷氨酸转运蛋白1(VGLUT1)和VGLUT2的抗体进行免疫染色,发现与气道平滑肌相关的分支层上皮下受体末端。后者的神经末梢似乎进一步表达钙结合蛋白D28k(CB)和ATP受体P2X3,但降钙素基因相关肽(CGRP)阴性。导致这些末端的神经纤维显示出髓鞘,并具有迷走感官起源。由于这种受体样结构的层状末端与气道平滑肌之间的紧密联系,我们将进一步将这些在形态学上可明确识别的感觉末端器官称为“平滑肌相关气道受体(SMARs)”。其次,我们进一步探讨了肺神经上皮体(NEBs)的感觉神经支配。 NEB是神经内分泌细胞的上皮内群,通过数个神经纤维群体接触,其中至少三个是感觉的。 NEB的脊髓感觉神经表达CGRP和P物质,在其基极接触NEB,并且对辣椒素敏感。另一方面,NEB的上皮内迷走神经感觉神经似乎是髓鞘化的,可以用针对VGLUT1,VGLUT2,CB和P2X3受体的抗体标记。 Na + / K + -ATPaseα3免疫染色另外标记了大鼠肺NEB迷走神经的神经支配部分。 SMARs和NEBs的迷走神经感觉神经支配的神经化学编码和受体样外观似乎几乎相同,让人联想到机械传感器。因此,NEB中的SMAR和迷走性结节神经末梢都可能代表了生理学特征的带髓鞘的迷走神经气道受体的广泛人群的亚型的形态对应物,其中大多数是机械敏感的。基于SMAR和NEB的经常紧密并置以及其神经末梢的特征非常相似,应谨慎解释基于“局部”刺激的电生理数据。

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