首页> 外文OA文献 >Localization of neurones expressing the gap junction protein Connexin45 within the adult spinal dorsal horn: a study using Cx45-eGFP reporter mice.
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Localization of neurones expressing the gap junction protein Connexin45 within the adult spinal dorsal horn: a study using Cx45-eGFP reporter mice.

机译:在成年脊髓背角内表达间隙连接蛋白Connexin45的神经元的定位:使用Cx45-eGFp报道小鼠的研究。

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摘要

Connexin (Cx) proteins localized to neuronal and glial syncytia provide the ultrastructural components for intercellular communication via gap junctions. In this study, a Cx45 reporter mouse model in which the Cx45 coding sequence is substituted for enhanced green fluorescent protein (eGFP) was used to characterize Cx45 expressing neurones within adult mouse spinal cord. eGFP-immunoreactive (eGFP-IR) cells were localized at all rostro-caudal levels to laminae I-III of the dorsal horn (DH), areas associated with nociception. The neuronal rather than glial phenotype of these cells in DH was confirmed by co-localisation of eGFP-IR with the neuronal marker NeuN. Further immunohistochemical studies revealed that eGFP-IR interneurones co-express the calcium-binding protein calbindin, and to a lesser extent calretinin. In contrast, eGFP-IR profiles did not co-localize with either parvalbumin or GAD-67, both of which are linked to inhibitory interneurones. Staining with the primary afferent markers isolectin-B4 (IB4) and calcitonin gene-related peptide revealed that eGFP-IR somata within laminae I-III receive close appositions from the former, presumed non-peptidergic nociceptive afferents of peripheral origin. The presence of 5-HT terminals in close apposition to eGFP-IR interneuronal somata suggests modulation via descending pathways. These data demonstrate a highly localized expression of Cx45 in a population of interneurones within the mouse superficial dorsal horn. The implications of these data in the context of the putative role of Cx45 and gap junctions in spinal somatosensory processing and pain are discussed.
机译:连接蛋白(Cx)蛋白质位于神经元和神经胶质合胞体提供了通过间隙连接的细胞间通讯的超微结构组件。在这项研究中,其中Cx45编码序列被增强的绿色荧光蛋白(eGFP)取代的Cx45报告基因小鼠模型用于表征成年小鼠脊髓内表达Cx45的神经元。 eGFP免疫反应性(eGFP-IR)细胞在所有尾all水平均定位于背角(DH)的薄片I-III,即与伤害感受相关的区域。这些细胞在DH中的神经元而不是神经胶质表型通过eGFP-IR与神经元标记NeuN的共定位得到证实。进一步的免疫组织化学研究表明,eGFP-IR中间神经元共表达钙结合蛋白calbindin,并在较小程度上共表达calretinin。相比之下,eGFP-IR图谱与小白蛋白或GAD-67均未共定位,两者均与抑制性中间神经元有关。用主要传入标记isolectin-B4(IB4)和降钙素基因相关肽染色显示,层I-III内的eGFP-IR体细胞与周围的前者(假定为非肽能的伤害性传入)相似。 5-HT末端与eGFP-IR神经元间躯体紧密并存的存在提示通过递减途径进行调节。这些数据表明在小鼠浅背角内的interneurones人口中的Cx45高度本地化的表达。讨论了这些数据在Cx45和间隙连接在脊髓体感加工和疼痛中的假定作用的背景下的含义。

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