首页> 外文期刊>The European Journal of Neuroscience >Homeostatic plasticity induced by chronic block of AMPA/kainate receptors modulates the generation of rhythmic bursting in rat spinal cord organotypic cultures.
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Homeostatic plasticity induced by chronic block of AMPA/kainate receptors modulates the generation of rhythmic bursting in rat spinal cord organotypic cultures.

机译:由AMPA /海藻酸酯受体的慢性阻滞诱导的稳态可塑性调节大鼠脊髓器官型培养物中节律性爆发的产生。

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摘要

Generation of spontaneous rhythmic activity is a distinct feature of developing spinal networks. We report that rat embryo organotypic spinal cultures contain the basic circuits responsible for pattern generation. In this preparation rhythmic activity can be recorded from ventral interneurons and is developmentally regulated. When chronically grown in the presence of an AMPA/kainate receptor blocker, this circuit expresses long-term plasticity consisting largely of increased frequency of fast synaptic activity and reduction in slow GABAergic events. We examined whether, once this form of homeostatic plasticity is established, the network could still exhibit rhythmicity with properties similar to controls. Control or chronically treated ventral interneurons spontaneously generated (with similar probability) irregular, network-driven bursts over a background of ongoing synaptic activity. In control cultures increasing network excitability by strychnine plus bicuculline, or by raising [K(+)](o), induced rapid-onset, regular rhythmic bursts. In treated cultures the same pharmacological block of Cl(-)-mediated transmission or high-K(+) application also induced regular patterned activity, although significantly faster and, in the case of high K(+), characterized by slow onset due to postsynaptic current summation. Enhancing GABAergic transmission by pentobarbital surprisingly accelerated the high-K(+) rhythm of control cells (though depressing background activity), whereas it slowed it down in chronically treated cells. This contrasting effect of pentobarbital suggests that, to preserve bursting ability, chronic slices developed a distinct GABAergic inhibitory control on over-expressed bursting circuits. Conversely, in control slices GABAergic transmission depressed spontaneous activity but it facilitated bursting frequency. Thus, even after homeostatic rearrangement, developing mammalian spinal networks still generate rhythmic activity.
机译:自发的节律活动的产生是发展中的脊髓网络的明显特征。我们报告说,大鼠胚胎器官型脊柱文化包含负责模式生成的基本电路。在该制剂中,可以从腹间神经元记录节律性活动并对其进行调节。当在存在AMPA /海藻酸酯受体阻滞剂的情况下长期生长时,该电路会表现出长期可塑性,主要由快速突触活动的频率增加和缓慢的GABA能事件减少组成。我们检查了一旦建立了这种形式的稳态可塑性,该网络是否仍可以表现出具有与对照相似的特性的节律性。在进行性突触活动的背景下,对照或经慢性治疗的腹腔神经元自发地(以相似的概率)产生不规则的,网络驱动的爆发。在对照培养物中,通过士的宁加双瓜氨酸或通过升高[K(+)](o)来增加网络兴奋性,从而诱导快速发作,规律的节律性爆发。在经过处理的培养物中,Cl(-)介导的传播或高K(+)应用的相同药理学阻滞也诱导了规律的模式活性,尽管明显更快,并且在高K(+)的情况下,其特征在于起效缓慢突触后电流求和。戊巴比妥增强GABA能传递的速度出人意料地加快了对照细胞的高K(+)节律(尽管降低了背景活性),而在经过长期治疗的细胞中却减慢了它的生长速度。戊巴比妥的这种对比作用表明,为了保留爆发力,慢性切片在过度表达的爆发电路上形成了独特的GABA能抑制控制。相反,在控制切片中,GABA能传递抑制了自发活动,但促进了爆发频率。因此,即使在体内平衡重排后,发展中的哺乳动物脊髓网络仍会产生节律性活动。

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