首页> 美国卫生研究院文献>The Journal of Neuroscience >Synaptic Activity Induces Dramatic Changes in the Geometry of the Cell Nucleus: Interplay between Nuclear Structure Histone H3 Phosphorylation and Nuclear Calcium Signaling
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Synaptic Activity Induces Dramatic Changes in the Geometry of the Cell Nucleus: Interplay between Nuclear Structure Histone H3 Phosphorylation and Nuclear Calcium Signaling

机译:突触活动引起细胞核几何结构的戏剧性变化:核结构组蛋白H3磷酸化和核钙信号之间的相互作用。

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摘要

Synaptic activity initiates many adaptive responses in neurons. Here we report a novel form of structural plasticity in dissociated hippocampal cultures and slice preparations. Using a recently developed algorithm for three-dimensional image reconstruction and quantitative measurements of cell organelles, we found that many nuclei from hippocampal neurons are highly infolded and form unequally sized nuclear compartments. Nuclear infoldings are dynamic structures, which can radically transform the geometry of the nucleus in response to neuronal activity. Action potential bursting causing synaptic NMDA receptor activation dramatically increases the number of infolded nuclei via a process that requires the ERK-MAP kinase pathway and new protein synthesis. In contrast, death-signaling pathways triggered by extrasynaptic NMDA receptors cause a rapid loss of nuclear infoldings. Compared with near-spherical nuclei, infolded nuclei have a larger surface and increased nuclear pore complex immunoreactivity. Nuclear calcium signals evoked by cytosolic calcium transients are larger in small nuclear compartments than in the large compartments of the same nucleus; moreover, small compartments are more efficient in temporally resolving calcium signals induced by trains of action potentials in the theta frequency range (5 Hz). Synaptic activity-induced phosphorylation of histone H3 on serine 10 was more robust in neurons with infolded nuclei compared with neurons with near-spherical nuclei, suggesting a functional link between nuclear geometry and transcriptional regulation. The translation of synaptic activity-induced signaling events into changes in nuclear geometry facilitates the relay of calcium signals to the nucleus, may lead to the formation of nuclear signaling microdomains, and could enhance signal-regulated transcription.
机译:突触活动引发神经元的许多适应性反应。在这里我们报告分离海马文化和切片准备中的一种新形式的结构可塑性。使用最近开发的算法进行三维图像重建和细胞器的定量测量,我们发现海马神经元的许多核高度折叠并形成大小不等的核区室。核折叠是动态结构,可以响应神经元活动从根本上改变核的几何形状。通过需要ERK-MAP激酶途径和新蛋白质合成的过程,引起突触NMDA受体活化的动作电位爆发极大地增加了核折叠的数量。相反,由突触外NMDA受体触发的死亡信号通路导致核折叠的快速丧失。与近球形的核相比,折叠的核具有更大的表面并增加了核孔复合物的免疫反应性。小核区室中胞浆钙瞬变引起的核钙信号比相同核的大区室大。此外,小隔室在时间上分辨由theta频率范围(5 Hz)中的一系列动作电位引起的钙信号更有效。与具有近球形核的神经元相比,在具有折叠核的神经元中,突触活动诱导的丝氨酸10上组蛋白H3的磷酸化更强健,表明核几何与转录调控之间存在功能联系。突触活动诱导的信号事件转化为核几何形状的变化有助于钙信号向核的传递,可能导致核信号微域的形成,并可以增强信号调节的转录。

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