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一种包含冷休克结构域(Y盒)和多嘧啶序列结合蛋白的多蛋白复合物在血管内皮生长因子信使核糖核酸上形成。在信使核糖核酸稳定中可能发挥的作用。

A multi-protein complex containing cold shock domain (Y-box) and polypyrimidine tract binding proteins forms on the vascular endothelial growth factor mRNA. Potential role in mRNA stabilization.

作者信息

Coles Leeanne S, Bartley M Antonetta, Bert Andrew, Hunter Julie, Polyak Steven, Diamond Peter, Vadas Mathew A, Goodall Gregory J

机构信息

Division of Human Immunology, The Hanson Institute, Institute of Medical and Veterinary Science, Adelaide, South Australia, Australia.

出版信息

Eur J Biochem. 2004 Feb;271(3):648-60. doi: 10.1111/j.1432-1033.2003.03968.x.

Abstract

Vascular endothelial growth factor (VEGF) is a key regulator of angiogenesis and post-transcriptional regulation plays a major role in VEGF expression. Both the 5'- and 3'-UTR are required for VEGF post-transcriptional regulation but factors binding to functional sequences within the 5'-UTR have not been fully characterized. We report here the identification of complexes, binding to the VEGFmRNA 5'- and 3'-UTR, that contain cold shock domain (CSD) and polypyrimidine tract binding (PTB) RNA binding proteins. Analysis of the CSD/PTB binding sites revealed a potential role in VEGF mRNA stability, in both noninduced and induced conditions, demonstrating a general stabilizing function. Such a stabilizing mechanism had not been reported previously for the VEGF gene. We further found that the CSD/PTB-containing complexes are large multiprotein complexes that are most likely preformed in solution and we demonstrate that PTB is associated with the VEGF mRNA in vivo. Complex formation between CSD proteins and PTB has not been reported previously. Analysis of the CSD/PTB RNA binding sites revealed a novel CSD protein RNA recognition site and also demonstrated that CSD proteins may direct the binding of CSD/PTB complexes. We found the same complexes binding to an RNA-stabilizing element of another growth factor gene, suggesting a broader functional role for the CSD/PTB complexes. Finally, as the VEGF gene is also regulated at the transcriptional level by CSD proteins, we propose a combined transcriptional/post-transcriptional role for these proteins in VEGF and other growth factor gene regulation.

摘要

血管内皮生长因子(VEGF)是血管生成的关键调节因子,转录后调控在VEGF表达中起主要作用。VEGF的转录后调控需要5'-和3'-非翻译区(UTR),但与5'-UTR内功能序列结合的因子尚未完全明确。我们在此报告了与VEGF mRNA的5'-和3'-UTR结合的复合物的鉴定,这些复合物包含冷休克结构域(CSD)和多嘧啶序列结合(PTB)RNA结合蛋白。对CSD/PTB结合位点的分析揭示了其在非诱导和诱导条件下对VEGF mRNA稳定性的潜在作用,表明其具有普遍的稳定功能。此前尚未有关于VEGF基因这种稳定机制的报道。我们进一步发现,含CSD/PTB的复合物是大型多蛋白复合物,很可能在溶液中预先形成,并且我们证明PTB在体内与VEGF mRNA相关联。此前尚未报道过CSD蛋白与PTB之间形成复合物。对CSD/PTB RNA结合位点的分析揭示了一个新的CSD蛋白RNA识别位点,还表明CSD蛋白可能指导CSD/PTB复合物的结合。我们发现相同的复合物与另一个生长因子基因的RNA稳定元件结合,这表明CSD/PTB复合物具有更广泛的功能作用。最后,由于VEGF基因在转录水平上也受CSD蛋白调控,我们提出这些蛋白在VEGF和其他生长因子基因调控中具有转录/转录后联合作用。

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