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Transcriptional Activation of the Cholecystokinin Gene by DJ-1 through Interaction of DJ-1 with RREB1 and the Effect of DJ-1 on the Cholecystokinin Level in Mice

机译:DJ-1通过RREB1与DJ-1相互作用来激活DJ-1激活胆囊收缩素基因,以及DJ-1对小鼠胆囊收缩素水平的影响

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摘要

DJ-1 is an oncogene and also causative gene for familial Parkinson’s disease. DJ-1 has multiple functions, including transcriptional regulation. DJ-1 acts as a coactivator that binds to various transcription factors, resulting in stimulation or repression of the expression of their target genes. In this study, we found that the cholecystokinin (CCK) gene is a transcriptional target gene for DJ-1. CCK is a peptide hormone and plays roles in contraction of the gallbladder and in promotion of secretion of pancreatic fluid. CCK is co-localized with dopamine in the substantia nigra to regulate release of dopamine. Reduced expression of CCK mRNA was observed in DJ-1-knockdown cells. The Ras-responsive element (RRE) and Sp1 site were essential for promoter activity, and DJ-1 stimulated promoter activity by binding to RRE-binding protein 1 (RREBP1). The complex of DJ-1 with RREB1 but not with Sp1 bound to the RRE. Furthermore, the reduced CCK level in the serum from DJ-1-knockout mice compared to that from wild-type mice was observed. This is the first report showing that DJ-1 participates in peptide hormone synthesis.
机译:DJ-1是家族性帕金森氏病的致癌基因,也是致病基因。 DJ-1具有多种功能,包括转录调控。 DJ-1充当与各种转录因子结合的共激活因子,从而刺激或抑制其靶基因的表达。在这项研究中,我们发现胆囊收缩素(CCK)基因是DJ-1的转录靶基因。 CCK是一种肽激素,在胆囊收缩和促进胰液分泌中起作用。 CCK与多巴胺在黑质中共定位,以调节多巴胺的释放。在DJ-1敲低细胞中观察到CCK mRNA的表达降低。 Ras反应元件(RRE)和Sp1位点对于启动子活性必不可少,DJ-1通过与RRE结合蛋白1(RREBP1)结合来刺激启动子活性。 DJ-1与RREB1而不与Sp1的复合体绑定到RRE。此外,观察到与野生型小鼠相比,DJ-1基因敲除小鼠血清中CCK水平降低。这是第一份表明DJ-1参与肽激素合成的报告。

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