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首页> 外文期刊>The European Journal of Neuroscience >Nonselective innervation of lamina I projection neurons by cocaine- and amphetamine-regulated transcript peptide (CART)-immunoreactive fibres in the rat spinal dorsal horn.
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Nonselective innervation of lamina I projection neurons by cocaine- and amphetamine-regulated transcript peptide (CART)-immunoreactive fibres in the rat spinal dorsal horn.

机译:大鼠脊髓背角中可卡因和苯丙胺调节的转录肽(CART)免疫反应性纤维对层状I投射神经元的非选择性神经支配。

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摘要

Cocaine- and amphetamine-regulated transcript (CART) peptides have been implicated in spinal pain transmission. A dense plexus of CART-immunoreactive fibres has been described in the superficial laminae of the spinal cord, which are key areas in sensory information and pain processing. We demonstrated previously that the majority of these fibres originate from nociceptive primary afferents. Using tract tracing, multiple immunofluorescent labelling and electronmicroscopy we determined the proportion of peptidergic primary afferents expressing CART, looked for evidence for coexistence of CART with galanin in these afferents in lamina I and examined their targets. Almost all (97.9%) randomly selected calcitonin gene-related peptide (CGRP)-immunoreactive terminals were substance P (SP)-positive (+) and CART was detected in approximately half (48.6%) of them. Most (81.4%) of the CGRP/SPergic boutons were galanin+ and approximately half (49.0%) of these contained CART. Many (72.9%) of the CARTergic boutons which expressed CGRP were also immunoreactive for galanin, while only 8.6% of the CARTergic terminals were galanin+ without CGRP. Electron microscopy showed that most of the CART terminals formed asymmetrical synapses, mainly with dendrites. All different morphological and neurochemical subtypes of spinoparabrachial projection neurons in the lamina I received contacts from CART-immunoreactive nociceptive afferents. The innervation density from these boutons did not differ significantly between either the different neurochemical or the morphological subclasses of these cells. This suggests a nonselective innervation of lamina I projection neurons from a subpopulation of CGRP/SP afferents containing CART peptide. These results provide anatomical evidence for involvement of CART peptide in spinal pain transmission.
机译:可卡因和苯丙胺调节的转录(CART)肽已牵涉到脊髓痛的传递。在脊髓的浅层中已经描述了CART免疫反应性纤维的致密丛,这是感觉信息和疼痛处理的关键区域。我们以前证明了这些纤维的大部分来自伤害性的初级传入神经。使用道追踪,多重免疫荧光标记和电子显微镜,我们确定了表达CART的肽能性初级传入者的比例,寻找层状I中这些传入者中CART与甘丙肽共存的证据。几乎所有(97.9%)随机选择的降钙素基因相关肽(CGRP)免疫反应性末端均是P(SP)阳性(+)物质,其中约一半(48.6%)检出了CART。大部分(81.4%)的CGRP / SPergic bouton是甘丙肽+,其中约一半(49.0%)包含CART。许多(72.9%)表达CGRP的CARTergic钮扣也对甘丙肽具有免疫反应性,而只有8.6%的CARTergic末端是无CGRP的甘丙肽+。电子显微镜显示,大多数CART末端形成不对称突触,主要与树突有关。我的椎板中臂旁臂突神经元的所有不同形态和神经化学亚型都接受了来自CART免疫反应性伤害感受传入的接触。这些钮扣的神经支配密度在这些细胞的不同神经化学或形态亚类之间没有显着差异。这表明来自包含CART肽的CGRP / SP传入亚群的层I投射神经元的非选择性神经支配。这些结果为CART肽参与脊髓痛传递提供了解剖学证据。

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