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NMDA 受体 GluN2B 和 GluN2D 在躯体感觉发育和成熟中的相反作用。

Opposing role of NMDA receptor GluN2B and GluN2D in somatosensory development and maturation.

机构信息

Department of Anatomy, Hokkaido University Graduate School of Medicine, Sapporo 060-8638, Japan.

Department of Anatomy, Hokkaido University Graduate School of Medicine, Sapporo 060-8638, Japan, Department of Pediatric Dentistry, Hokkaido University Graduate School of Dental Medicine, Sapporo 060-8586, Japan.

出版信息

J Neurosci. 2014 Aug 27;34(35):11534-48. doi: 10.1523/JNEUROSCI.1811-14.2014.

Abstract

Development of correct topographical connections between peripheral receptors and central somatosensory stations requires activity-dependent synapse refinement, in which the NMDA type of glutamate receptors plays a key role. Here we compared functional roles of GluN2B (GluRε2 or NR2B) and GluN2D (GluRε4 or NR2D), two major regulatory subunits of neonatal NMDA receptors, in development of whisker-related patterning at trigeminal relay stations. Compared with control littermates, both the appearance of whisker-related patterning and the termination of the critical period, as assessed by unilateral infraorbital nerve transection, were delayed by nearly a day in the somatosensory cortex of GluN2B(+/-) mice but advanced by nearly a day in GluN2D(-/-) mice. Similar temporal shifts were found at subcortical relay stations in the thalamus and brainstem of GluN2B(+/-) and GluN2D(-/-) mice. In comparison, the magnitude of lesion-induced critical period plasticity in the somatosensory cortex, as assessed following row-C whisker removal, was normal in both mutants. Thus, GluN2B and GluN2D play counteractive roles in temporal development and maturation of somatosensory maps without affecting the magnitude of critical period plasticity. To understand the opposing action, we then examined neuronal and synaptic expressions of the two subunits along the trigeminal pathway. At each trigeminal station, GluN2B was predominant at asymmetrical synapses of non-GABAergic neurons, whereas GluN2D was selective to asymmetrical synapses of GABAergic neurons. Together, our findings suggest that GluN2B expressed at glutamatergic synapses on glutamatergic projection neurons facilitates refinement of ascending pathway synapses directly, whereas GluN2D expressed at glutamatergic synapses on GABAergic interneurons delays it indirectly.

摘要

外周受体与中枢感觉站之间正确的拓扑连接的发展需要活性依赖的突触细化,其中 NMDA 型谷氨酸受体发挥关键作用。在这里,我们比较了 GluN2B(GluRε2 或 NR2B)和 GluN2D(GluRε4 或 NR2D)这两种新生儿 NMDA 受体主要调节亚基在三叉神经中继站中与胡须相关模式形成中的功能作用。与对照同窝仔相比,GluN2B(+/-) 小鼠感觉皮层中的胡须相关模式的出现和关键期的结束(通过单侧眶下神经切断术评估)延迟了近一天,而 GluN2D(-/-) 小鼠则提前了近一天。在丘脑和脑干的皮层下中继站中也发现了类似的时间推移GluN2B(+/-) 和 GluN2D(-/-) 小鼠。相比之下,在感觉皮层中,通过去除第 C 排胡须来评估的损伤诱导的关键期可塑性的幅度在两种突变体中均正常。因此,GluN2B 和 GluN2D 在不影响关键期可塑性幅度的情况下,在感觉图谱的时间发育和成熟中发挥拮抗作用。为了理解相反的作用,我们随后检查了两种亚基沿三叉神经通路的神经元和突触表达。在每个三叉神经站,GluN2B 主要在非 GABA 能神经元的非对称突触上表达,而 GluN2D 选择性地在 GABA 能神经元的非对称突触上表达。总之,我们的发现表明,在谷氨酸能投射神经元上表达的 GluN2B 直接促进了上行通路突触的细化,而在 GABA 能中间神经元上表达的 GluN2D 则间接地延迟了它。

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