首页> 外文期刊>American Journal of Physiology >Heterogeneous distribution of basal cyclic guanosine monophosphate within distinct neuronal populations in the hypothalamic paraventricular nucleus.
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Heterogeneous distribution of basal cyclic guanosine monophosphate within distinct neuronal populations in the hypothalamic paraventricular nucleus.

机译:下丘脑室旁核中不同神经元群体中基底环鸟苷单磷酸的异质分布。

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摘要

The supraoptic (SON) and the paraventricular (PVN) hypothalamic nuclei constitute major neuronal substrates underlying nitric oxide (NO) effects on autonomic and neuroendocrine control. Within these nuclei, constitutively produced NO restrains the firing activity of magnocellular neurosecretory and preautonomic neurons, actions thought to be mediated by a cGMP-dependent enhancement of GABAergic inhibitory transmission. In the present study, we expanded on this knowledge by performing a detailed anatomical characterization of constitutive NO-receptive, cGMP-producing neurons within the PVN. To this end, we combined tract-tracing techniques and immunohistochemistry to visualize cGMP immunoreactivity within functionally, neurochemically, and topographically discrete PVN neuronal populations in Wistar rats. Basal cGMP immunoreactivity was readily observed in the PVN, both in neuronal and vascular profiles. The incidence of cGMP immunoreactivity was significantly higher in magnocellular (69%) compared with preautonomic ( approximately 10%) neuronal populations (P < 0.01). No differences were observed between oxytocin (OT) and vasopressin (VP) magnocellular neurons. In preautonomic neurons, the incidence of cGMP was independent of their subnuclei distribution, innervated target (i.e., intermediolateral cell column, nucleus tractus solitarii, or rostral ventrolateral medulla) or their neurochemical phenotype (i.e., OT or VP). Finally, high levels of cGMP immunoreactivity were observed in GABAergic somata and terminals within the PVN of eGFP-GAD67 transgenic mice. Altogether, these data support a highly heterogeneous distribution of basal cGMP levels within the PVN and further support the notion that constitutive NO actions in the PVN involve intricate cell-cell interactions, as well as heterogeneous signaling modalities.
机译:视上丘脑(SON)和室下丘脑(PVN)构成主要的神经元底物,一氧化氮(NO)对自主神经和神经内分泌的控制作用。在这些核内,组成性产生的NO抑制了大细胞神经分泌和前自主神经元的放电活性,这些动作被认为是由cGMP依赖性GABA能抑制性传递的增强介导的。在本研究中,我们通过对PVN内组成型NO受体,产生cGMP的神经元进行详细的解剖学表征,扩展了这一知识。为此,我们结合了追踪技术和免疫组化技术,以观察Wistar大鼠在功能,神经化学和地形上离散的PVN神经元群体中的cGMP免疫反应性。在神经元和血管分布中,PVN中都容易观察到基础cGMP免疫反应性。与自主神经前群体(约10%)相比,大细胞中cGMP免疫反应的发生率(69%)显着更高(P <0.01)。催产素(OT)和加压素(VP)巨细胞神经元之间未观察到差异。在自主神经元中,cGMP的发生与它们的亚核分布,神经支配的靶标(即中间外侧细胞柱,孤核,或腹侧腹侧延髓)或神经化学表型(即OT或VP)无关。最后,在eGFP-GAD67转基因小鼠的GABA能性体细胞和PVN末端观察到高水平的cGMP免疫反应性。总而言之,这些数据支持PVN内基础cGMP水平的高度异质分布,并进一步支持PVN中本构性NO作用涉及复杂的细胞-细胞相互作用以及异质信号传递方式的观点。

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