Colomer Claude, Olivos Ore Luis A, Coutry Nathalie, Mathieu Marie-Noëlle, Arthaud Sébastien, Fontanaud Pierre, Iankova Irena, Macari Françoise, Thouënnon Erwan, Yon Laurent, Anouar Youssef, Guérineau Nathalie C
Institute of Functional Genomics, 34094 Montpellier, France.
J Neurosci. 2008 Jun 25;28(26):6616-26. doi: 10.1523/JNEUROSCI.5597-07.2008.
An increase in circulating catecholamine levels represents one of the mechanisms whereby organisms cope with stress. In the periphery, catecholamines mainly originate from the sympathoadrenal system. As we reported, in addition to the central control through cholinergic innervation, a local gap junction-delineated route between adrenal chromaffin cells contributes to catecholamine exocytosis. Here, we investigated whether this intercellular communication is modified when the hormonal demand is increased as observed during cold stress. Our results show that in cold exposed rats, gap-junctional communication undergoes a functional plasticity, as evidenced by an increased number of dye-coupled cells. Of a physiological interest is that this upregulation of gap-junctional coupling results in the appearance of a robust electrical coupling between chromaffin cells that allows the transmission of action potentials between coupled cells. This enhancement of gap-junctional communication parallels an increase in expression levels of connexin36 (Cx36) and connexin43 (Cx43) proteins. Both transcriptional and posttranslational mechanisms are involved because Cx36 transcripts are increased in stressed rats and the expression of the scaffolding protein zonula occludens-1, known to interact with both Cx36 and Cx43, is also upregulated. Consistent with an upregulated coupling extent in stressed rats, the cytosolic Ca(2+) concentration rises triggered in a single cell by an iontophoretic application of nicotine occur simultaneously in several neighboring cells. These results describe for the first time a functional plasticity of junctional coupling between adult chromaffin cells that should be crucial for adaptation to stress or sensitization to subsequent stressors.
循环儿茶酚胺水平升高是生物体应对压力的机制之一。在外周,儿茶酚胺主要源自交感肾上腺系统。正如我们所报道的,除了通过胆碱能神经支配进行中枢控制外,肾上腺嗜铬细胞之间由局部缝隙连接界定的途径也有助于儿茶酚胺的胞吐作用。在此,我们研究了在冷应激期间观察到的激素需求增加时,这种细胞间通讯是否会发生改变。我们的结果表明,在冷暴露的大鼠中,缝隙连接通讯经历了功能可塑性,这表现为染料偶联细胞数量增加。从生理学角度来看,缝隙连接偶联的这种上调导致嗜铬细胞之间出现强大的电偶联,从而允许动作电位在偶联细胞之间传递。缝隙连接通讯的这种增强与连接蛋白36(Cx36)和连接蛋白43(Cx43)蛋白表达水平的增加平行。转录和翻译后机制均参与其中,因为应激大鼠中Cx36转录本增加,并且已知与Cx36和Cx43都相互作用的支架蛋白紧密连接蛋白-1的表达也上调。与应激大鼠中偶联程度上调一致,通过离子电渗法施加尼古丁在单个细胞中引发的胞质Ca(2+)浓度升高会在几个相邻细胞中同时发生。这些结果首次描述了成年嗜铬细胞之间连接偶联的功能可塑性,这对于适应压力或对后续应激源的敏化应该至关重要。