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首页> 外文期刊>Neuron >Serum response factor mediates NGF-dependent target innervation by embryonic DRG sensory neurons.
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Serum response factor mediates NGF-dependent target innervation by embryonic DRG sensory neurons.

机译:血清反应因子通过胚胎DRG感觉神经元介导NGF依赖的靶标神经。

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摘要

Serum response factor (SRF) is a prototypic transcription factor that mediates stimulus-dependent gene expression. Here, we show that SRF mediates NGF signaling, axonal growth, branching, and target innervation by embryonic DRG sensory neurons. Conditional deletion of the murine SRF gene in DRGs results in no deficits in neuronal viability or differentiation but causes defects in extension and arborization of peripheral axonal projections in the target field in vivo, similar to the target innervation defects observed in mice lacking NGF. Moreover, SRF is both necessary and sufficient for NGF-dependent axonal outgrowth in vitro, and NGF regulates SRF-dependent gene expression and axonal outgrowth through activation of both MEK/ERK and MAL signaling pathways. These findings show that SRF is a major effector of both MEK/ERK and MAL signaling by NGF and that SRF is a key mediator of NGF-dependent target innervation by embryonic sensory neurons.
机译:血清反应因子(SRF)是介导刺激依赖性基因表达的原型转录因子。在这里,我们显示SRF通过胚胎DRG感觉神经元介导NGF信号传导,轴突生长,分支和靶标神经支配。有条件地删除DRGs中的鼠SRF基因不会导致神经元活力或分化缺陷,但会导致体内靶标区域周围轴突投射的延伸和乔化缺陷,类似于在缺乏NGF的小鼠中观察到的靶标神经分布缺陷。而且,SRF对于体外依赖于NGF的轴突生长是必需的和充分的,并且NGF通过激活MEK / ERK和MAL信号通路来调节依赖于SRF的基因表达和轴突生长。这些发现表明,SRF是NGF引起的MEK / ERK和MAL信号的主要效应物,并且SRF是胚胎感觉神经元依赖NGF的靶标神经支配的关键介质。

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