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Structure of the gene encoding VGF, a nervous system-specific mRNA that is rapidly and selectively induced by nerve growth factor in PC12 cells.

机译:编码VGF的基因的结构,VGF是PC12细胞中神经生长因子快速选择性诱导的神经系统特异性mRNA。

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摘要

Nerve growth factor (NGF) plays a critical role in the development and survival of neurons in the peripheral nervous system. Following treatment with NGF but not epidermal growth factor, rat pheochromocytoma (PC12) cells undergo neural differentiation. We have cloned a nervous system-specific mRNA, NGF33.1, that is rapidly and relatively selectively induced by treatment of PC12 cells with NGF and basic fibroblast growth factor in comparison with epidermal growth factor. Analysis of the nucleic acid and predicted amino acid sequences of the NGF33.1 cDNA clone suggested that this clone corresponded to the NGF-inducible mRNA called VGF (A. Levi, J. D. Eldridge, and B. M. Paterson, Science 229:393-395, 1985; R. Possenti, J. D. Eldridge, B. M. Paterson, A. Grasso, and A. Levi, EMBO J. 8:2217-2223, 1989). We have used the NGF33.1 cDNA clone to isolate and characterize the VGF gene, and in this paper we report the complete sequence of the VGF gene, including 853 bases of 5' flank revealed TATAA and CCAAT elements, several GC boxes, and a consensus cyclic AMP response element-binding protein binding site. The VGF promoter contains sequences homologous to other NGF-inducible, neuronal promoters. We further show that VGF mRNA is induced in PC12 cells to a greater extent by depolarization and by phorbol-12-myristate-13-acetate treatment than by 8-bromo-cyclic AMP treatment. By Northern (RNA) and RNase protection analysis, VGF mRNA is detectable in embryonic and postnatal central and peripheral nervous tissues but not in a number of nonneural tissues. In the cascade of events which ultimately leads to the neural differentiation of NGF-treated PC12 cells, the VGF gene encodes the most rapidly and selectively regulated, nervous-system specific mRNA yet identified.
机译:神经生长因子(NGF)在周围神经系统中神经元的发育和存活中起关键作用。用NGF而非表皮生长因子治疗后,大鼠嗜铬细胞瘤(PC12)细胞经历神经分化。我们已经克隆了神经系统特异性mRNA,NGF33.1,与表皮生长因子相比,可以通过用NGF和碱性成纤维细胞生长因子治疗PC12细胞来快速而相对选择性地诱导。对NGF33.1 cDNA克隆的核酸和预测的氨基酸序列的分析表明,该克隆对应于称为VGF的NGF诱导型mRNA(A.Levi,JD Eldridge和BM Paterson,Science 229:393-395,1985 ; R.Possenti,JD Eldridge,BM Paterson,A.Grasso,和A.Levi,EMBO J.8:2217-2223,1989)。我们已经使用NGF33.1 cDNA克隆来分离和表征VGF基因,并且在本文中我们报告了VGF基因的完整序列,包括853个5'侧翼碱基,揭示了TATAA和CCAAT元素,几个GC框和一个共有环AMP反应元件结合蛋白结合位点。 VGF启动子包含与其他NGF可诱导的神经元启动子同源的序列。我们进一步表明,与通过8-溴环AMP处理相比,通过去极化和佛波12-肉豆蔻酸13-乙酸酯处理,VGF mRNA在PC12细胞中的诱导程度更高。通过Northern(RNA)和RNase保护分析,VGF mRNA在胚胎和出生后的中枢和外周神经组织中可检测到,但在许多非神经组织中则不可检测到。在最终导致NGF处理的PC12细胞神经分化的一系列事件中,VGF基因编码迄今已鉴定的最快速和选择性调节的神经系统特异性mRNA。

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