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Obligatory role for the immediate early gene NARP in critical period plasticity

机译:立即早期NARP在关键时期可塑性中的强制性作用

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摘要

The immediate early gene neuronal activity-regulated pentraxin (NARP) is an α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding protein that is specifically enriched at excitatory synapses onto fast-spiking parvalbumin-positive interneurons (FS [PV] INs). Here, we show that transgenic deletion of NARP decreases the number of excitatory synaptic inputs onto FS (PV) INs and reduces net excitatory synaptic drive onto FS (PV) INs. Accordingly, the visual cortex of NARP-/- mice is hyperexcitable and unable to express ocular dominance plasticity, although many aspects of visual function are unimpaired. Importantly, the number and strength of inhibitory synaptic contacts from FS (PV) INs onto principle neurons in the visual cortex is normal in NARP-/- mice, and enhancement of thisoutput recovers the expression of experience-dependent synaptic plasticity. Thus the recruitment of inhibition from FS (PV) INs plays a central role in enabling the critical period for ocular dominance plasticity.
机译:立即早期基因神经元活性调节的五味素(NARP)是一种α-氨基-3-羟基-5-甲基-4-异恶唑丙酸受体(AMPAR)结合蛋白,在兴奋性突触中特异富集到速加的小白蛋白阳性中间神经元(FS [PV] INs)。在这里,我们显示NARP的转基因删除减少了对FS(PV)IN的兴奋性突触输入的数量,并减少了对FS(PV)IN的净兴奋性突触驱动。因此,尽管视觉功能的许多方面没有受到损害,但是NARP-/-小鼠的视觉皮层是过度兴奋的,不能表达眼部优势可塑性。重要的是,在NARP-/-小鼠中,从FS(PV)IN到视皮层中的主要神经元的抑制性突触接触的数量和强度在NARP-/-小鼠中是正常的,并且该输出的增强恢复了经验依赖性突触可塑性的表达。因此,FS(PV)INs抑制物的募集在使眼部优势可塑性达到关键时期起着核心作用。

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