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首页> 外文期刊>Brain research. Molecular brain research >The upstream regulatory region of the gene for the human homologue of the adhesion molecule TAG-1 contains elements driving neural specific expression in vivo.
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The upstream regulatory region of the gene for the human homologue of the adhesion molecule TAG-1 contains elements driving neural specific expression in vivo.

机译:粘附分子TAG-1的人类同源物基因的上游调节区域包含驱动体内神经特异性表达的元件。

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摘要

Cell adhesion molecules (CAMs) of the immunoglobulin superfamily (IgSF) exhibit restricted spatial and temporal expression profiles requiring a tight regulatory program during development. The rodent glycoprotein TAG-1 and its orthologs TAX-1 in the human and axonin-1 in chick are cell adhesion molecules belonging to the contactin/F3 subgroup of the IgSF. TAG-1 is expressed in restricted subsets of central and peripheral neurons, not only during development but also in adulthood, and is implicated in neurite outgrowth, axon guidance and fasciculation, as well as neuronal migration. In an attempt to identify the regulatory elements that guide the neuronal expression of TAG-1, we have isolated genomic clones containing 4 kb of the TAX-1 upstream sequence and used them to drive the expression of the LacZ reporter gene in transgenic mice. We demonstrate that this sequence includes elements not only sufficient to restrict expression to the nervous system, but also to recapitulate to a great extent the endogenous pattern of the TAG-1 expression in the developing CNS.
机译:免疫球蛋白超家族(IgSF)的细胞粘附分子(CAM)表现出受限的时空表达特征,在开发过程中需要严格的调节程序。人中的啮齿动物糖蛋白TAG-1及其直系同源物TAX-1和小鸡的轴突蛋白1是细胞粘附分子,属于IgSF的contactin / F3亚组。 TAG-1不仅在发育过程中而且在成年期中都在中枢和周围神经元的受限子集中表达,并且与神经突生长,轴突引导和束缚以及神经元迁移有关。为了确定指导TAG-1神经元表达的调控元件,我们分离了含有4 kb TAX-1上游序列的基因组克隆,并用它们来驱动LacZ报告基因在转基因小鼠中的表达。我们证明该序列不仅包括足以限制表达到神经系统的元素,而且在很大程度上概括了发展中国家CNS中TAG-1表达的内源性模式。

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