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首页> 外文期刊>The Journal of Physiology >Profound regulation of neonatal CA1 rat hippocampal GABAergic transmission by functionally distinct kainate receptor populations.
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Profound regulation of neonatal CA1 rat hippocampal GABAergic transmission by functionally distinct kainate receptor populations.

机译:功能上不同的海藻酸盐受体群体对新生CA1大鼠海马GABA能传递的深刻调节。

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Neonatal hippocampus exhibits distinct patterns of network activity that are dependent on the interaction between inhibitory and excitatory transmission. Kainate receptors are ideally positioned to regulate this activity by virtue of their ability to regulate presynaptic function in GABAergic interneurones. Indeed, kainate receptors are highly expressed in neonatal hippocampal interneurones, yet the role and mechanisms by which they might regulate neonatal circuitry are unexplored. To address this we investigated the kainate receptor-dependent regulation of GABAergic transmission onto neonatal CA1 pyramidal neurones. Kainate receptor activation produced two distinct opposing effects, a very large increase in the frequency of spontaneous IPSCs, and a robust depression of evoked GABAergic transmission. The up-regulation of spontaneous transmission was due to activation of somatodendritic and axonal receptors while the depression of evoked transmission could be fully accounted for by a direct regulation of GABA release by kainate receptors located at the terminals. None of the effects of kainate receptor agonists were sensitive to GABAB receptor antagonists, nor was there any postsynaptic kainate receptor-dependent effects observed in CA1 pyramidal cells that could account for our findings. Our data demonstrate that kainate receptors profoundly regulate neonatal CA1 GABAergic circuitry by two distinct opposing mechanisms, and indicate that these two effects are mediated by functionally distinct populations of receptors. Thus kainate receptors are strategically located to play a critical role in shaping early hippocampal network activity and by virtue of this have a key role in hippocampal development.
机译:新生的海马表现出独特的网络活动模式,这取决于抑制性和兴奋性传递之间的相互作用。由于其调节GABA能性神经元中突触前功能的能力,理想的位置是调节海藻酸盐受体以调节该活性。确实,海藻酸盐受体在新生儿海马中间神经元中高度表达,但尚未探讨其调节新生儿回路的作用和机制。为了解决这个问题,我们研究了对新生CA1锥体神经元的GABA能传递的海因酸酯受体依赖性调节。海藻酸酯受体的激活产生两种截然相反的作用,即自发IPSC频率的大幅增加,以及诱发的GABA能传递的强烈抑制。自发性传输的上调是由于躯体树突状和轴突受体的激活引起的,而诱发性传输的抑制则可以由末端的海藻酸盐受体直接调节GABA释放来完全解释。海藻酸盐受体激动剂的作用均不对GABAB受体拮抗剂敏感,在CA1锥体细胞中也未观察到任何突触后海藻酸盐受体依赖性作用,这可以解释我们的发现。我们的数据表明,海藻酸盐受体通过两种截然不同的相反机制深刻调节新生儿CA1 GABA能回路,并表明这两种作用是由功能不同的受体群体介导的。因此,海藻酸盐受体在战略上定位成在塑造早期海马网络活动中起关键作用,并因此在海马发育中起关键作用。

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