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首页> 外文期刊>Development >Abnormal sympathetic nervous system development and physiological dysautonomia in Egr3-deficient mice.
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Abnormal sympathetic nervous system development and physiological dysautonomia in Egr3-deficient mice.

机译:Egr3缺陷小鼠的交感神经系统发育异常和生理自主神经异常。

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Sympathetic nervous system development depends upon many factors that mediate neuron migration, differentiation and survival. Target tissue-derived nerve growth factor (NGF) signaling-induced gene expression is required for survival, differentiation and target tissue innervation of post-migratory sympathetic neurons. However, the transcriptional regulatory mechanisms mediated by NGF signaling are very poorly defined. Here, we identify Egr3, a member of the early growth response (Egr) family of transcriptional regulators, as having an important role in sympathetic nervous system development. Egr3 is regulated by NGF signaling and it is expressed in sympathetic neurons during development when they depend upon NGF for survival and target tissue innervation. Egr3-deficient mice have severe sympathetic target tissue innervation abnormalities and profound physiological dysautonomia. Unlike NGF, which is essential for sympathetic neuron survival and for axon branching within target tissues, Egr3 is required for normal terminal axon extension and branching, but not for neuron survival. The results indicate that Egr3 is a novel NGF signaling effector that regulates sympathetic neuron gene expression required for normal target tissue innervation and function. Egr3-deficient mice have a phenotype that is remarkably similar to humans with sympathetic nervous system disease, raising the possibility that it may have a role in some forms of human dysautonomia, most of which have no known cause.
机译:交感神经系统的发育取决于许多介导神经元迁移,分化和存活的因素。迁移后交感神经元的存活,分化和目标组织神经支配需要目标组织来源的神经生长因子(NGF)信号传导诱导的基因表达。但是,由NGF信号传导介导的转录调控机制的定义非常差。在这里,我们确定Egr3,转录调节器的早期生长反应(Egr)家族的成员,在交感神经系统发育中具有重要作用。 Egr3受NGF信号传导调节,在发育过程中,当它们依赖NGF生存和靶向组织神经支配时,它在交感神经元中表达。 Egr3缺陷小鼠具有严重的交感性靶组织神经支配异常和严重的生理自主神经失调。与NGF不同,NGF对于交感神经元存活和目标组织内的轴突分支必不可少,而Egr3对于正常的终末轴突延伸和分支却不是神经元存活所必需的。结果表明,Egr3是一种新型NGF信号传导效应子,可调节正常目标组织神经支配和功能所需的交感神经元基因表达。 Egr3缺陷型小鼠的表型与交感神经系统疾病的人非常相似,这增加了它可能在某些形式的人类自主神经失调中起作用的可能性,其中大多数原因尚不明。

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