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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Involvement of NF-Y and Sp1 in basal and cAMP-stimulated transcriptional activation of the tryptophan hydroxylase (TPH ) gene in the pineal gland.
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Involvement of NF-Y and Sp1 in basal and cAMP-stimulated transcriptional activation of the tryptophan hydroxylase (TPH ) gene in the pineal gland.

机译:NF-Y和Sp1参与松果体色氨酸羟化酶(TPH)基因的基础和cAMP刺激的转录激活。

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The expression of the tryptophan hydroxylase (TPH) gene, encoding the rate-limiting enzyme of serotonin biosynthesis, is tightly regulated both at the transcriptional and at the post-transcriptional levels. In the pineal gland, transcription of the gene is activated in response to an intracellular circadian increase of the cAMP concentration. We have previously shown that transcription of a 2.1-kb fragment of the human TPH promoter is induced by cAMP, although it lacks the canonical cAMP responsive element, CRE. The minimal promoter (-73/+29) has only weak transcriptional activity but is responsive to cAMP. It contains an inverted CCAAT box, which was demonstrated to be involved in this response. Here, we have extended our investigation to the functional features of the inverted CCAAT box in the -252/+29 TPH promoter, which has a higher basal activity. We show that an additional cis -acting sequence, the adjacent GC-rich region, cooperates with the inverted CCAAT box for the full activation of basal transcription, and that both elements are essential for the full cAMP response. We also show that in pinealocytes, NF-Y and Sp1 transactivators bind the inverted CCAAT box and GC-rich-region, respectively. These factors participate in a novel pathway for the cAMP-mediated response of the TPH promoter, which is independent of the canonical CRE-mediated response.
机译:色氨酸羟化酶(TPH)基因的编码,编码5-羟色胺生物合成的限速酶,其表达在转录水平和转录后水平均受到严格调节。在松果体中,响应细胞内昼夜节律中cAMP浓度的增加,基因的转录被激活。先前我们已经表明,人TPH启动子的2.1-kb片段的转录是由cAMP诱导的,尽管它缺乏典型的cAMP响应元件CRE。最小启动子(-73 / + 29)仅具有弱转录活性,但对cAMP有反应。它包含一个倒置的CCAAT框,该框已被证明参与了此响应。在这里,我们将研究扩展到-252 / + 29 TPH启动子中倒置CCAAT框的功能特征,它具有较高的基础活性。我们表明,一个额外的顺式作用序列,即邻近的富含GC的区域,与反向CCAAT框协同作用,可完全激活基础转录,并且这两个元素对于完整的cAMP反应都是必不可少的。我们还显示,在松果体细胞中,NF-Y和Sp1反式激活因子分别结合了反向CCAAT框和GC富集区域。这些因素参与了cAMP介导的TPH启动子应答的新途径,该途径独立于规范的CRE介导的应答。

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