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睫状神经肽信号动态调节出生后新皮层锥体神经元中的兴奋性突触。

Ciliary neuropeptidergic signaling dynamically regulates excitatory synapses in postnatal neocortical pyramidal neurons.

机构信息

Department of Biology, Brandeis University, Waltham, United States.

出版信息

Elife. 2021 Mar 2;10:e65427. doi: 10.7554/eLife.65427.

Abstract

Primary cilia are compartmentalized sensory organelles present on the majority of neurons in the mammalian brain throughout adulthood. Recent evidence suggests that cilia regulate multiple aspects of neuronal development, including the maintenance of neuronal connectivity. However, whether ciliary signals can dynamically modulate postnatal circuit excitability is unknown. Here we show that acute cell-autonomous knockdown of ciliary signaling rapidly strengthens glutamatergic inputs onto cultured rat neocortical pyramidal neurons and increases spontaneous firing. This increased excitability occurs without changes to passive neuronal properties or intrinsic excitability. Further, the neuropeptide receptor somatostatin receptor 3 (SSTR3) is localized nearly exclusively to excitatory neuron cilia both and in culture, and pharmacological manipulation of SSTR3 signaling bidirectionally modulates excitatory synaptic inputs onto these neurons. Our results indicate that ciliary neuropeptidergic signaling dynamically modulates excitatory synapses and suggest that defects in this regulation may underlie a subset of behavioral and cognitive disorders associated with ciliopathies.

摘要

初级纤毛是哺乳动物大脑中大多数神经元在成年期存在的分隔感觉细胞器。最近的证据表明,纤毛调节神经元发育的多个方面,包括神经元连接的维持。然而,纤毛信号是否可以动态调节出生后的回路兴奋性尚不清楚。在这里,我们显示急性细胞自主敲低纤毛信号迅速增强培养的大鼠新皮层锥体神经元上的谷氨酸能输入,并增加自发放电。这种兴奋性增加发生在没有改变被动神经元特性或内在兴奋性的情况下。此外,神经肽受体生长抑素受体 3(SSTR3)几乎仅定位于兴奋性神经元纤毛中, 和在培养物中,SSTR3 信号的药理学操纵双向调节这些神经元上的兴奋性突触输入。我们的结果表明,纤毛神经肽信号动态调节兴奋性突触,并表明这种调节的缺陷可能是与纤毛病相关的一系列行为和认知障碍的基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4387/7952091/f8aced136c1d/elife-65427-fig1.jpg

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