首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >A bi-functional activator/repressor element required for transcriptional activity of the human UCH-L1 gene assembles a neuron-specific protein: single-strand DNA complex.
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A bi-functional activator/repressor element required for transcriptional activity of the human UCH-L1 gene assembles a neuron-specific protein: single-strand DNA complex.

机译:人UCH-L1基因转录活性所需的双功能激活因子/阻遏因子元件可组装神经元特异性蛋白:单链DNA复合物。

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摘要

The ubiquitin C-terminal hydrolase (UCH)-L1 gene is expressed in a tissue- and cell-specific manner with expression restricted to neurons and neuroendocrine cells. Regulatory DNA sequences from the 5' untranscribed region of the human UCH-L1 gene will promote neuron specific transcription providing that a 59 bp sequence located between nucleotides -182 and -123 is present in reporter gene constructs. We show that this 59 bp sequence is a bi-functional regulator of transcription, acting as an activator in human neuroblastoma cells (SH-SY5Y) and a strong repressor in HeLa cells. The sense strand of the UCH-L1 activator/repressor element can interact with nuclear proteins that recognize single stranded DNA in a sequence specific manner. Nuclear extracts from neuroblastoma cells generate a protein:ssDNA interaction called complex 1B could be converted into a lower mobility complex (1A) by increasing the protein:DNA ratio. This conversion was not observed when using nuclear extracts from HeLa cells. Formation of neuron specific complex 1A could be prevented by incubation of protein:ssDNA complexes at 2 degrees C or in the presence of mM concentrations of MgCl2. In conclusion, we have identified a novel bi-functional regulatory DNA element in the promoter of the human UCH-L1 gene that contributes to neuron-restricted transcription and which can assemble a neuron specific protein:ssDNA complex on its sense strand.
机译:泛素C末端水解酶(UCH)-L1基因以组织和细胞特异性方式表达,且表达仅限于神经元和神经内分泌细胞。来自人类UCH-L1基因5'非转录区的调控DNA序列将促进神经元特异性转录,条件是在报告基因构建体中位于核苷酸-182和-123之间的59 bp序列。我们显示,这59 bp的序列是转录的双功能调节剂,在人类神经母细胞瘤细胞(SH-SY5Y)和HeLa细胞中具有强大的阻遏物作用。 UCH-L1激活物/阻遏物元件的有义链可以与核蛋白相互作用,这些核蛋白以序列特异性方式识别单链DNA。来自神经母细胞瘤细胞的核提取物产生一种蛋白质:ssDNA相互作用,称为复合物1B,可以通过增加蛋白质:DNA的比例转化为低迁移率的复合物(1A)。使用HeLa细胞的核提取物时未观察到这种转化。通过在2°C或存在mM浓度的MgCl2的条件下孵育蛋白质:ssDNA复合物,可以防止神经元特异性复合物1A的形成。总之,我们已经在人UCH-L1基因的启动子中鉴定了一种新型的双功能调节DNA元件,该元件有助于神经元限制性转录,并且可以在其有义链上组装神经元特异性蛋白质:ssDNA复合物。

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