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VEGF-A mRNA processing stability and translation: a paradigm for intricate regulation of gene expression at the post-transcriptional level

机译:VEGF-A mRNA的加工稳定性和翻译:转录后水平上复杂调控基因表达的范例

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摘要

Vascular Endothelial Growth Factor A (VEGF-A) is a potent secreted mitogen crucial for physiological and pathological angiogenesis. Post-transcriptional regulation of VEGF-A occurs at multiple levels. Firstly, alternative splicing gives rise to different transcript variants encoding diverse isoforms that exhibit distinct biological properties with regard to receptor binding and extra-cellular localization. Secondly, VEGF-A mRNA stability is regulated by effectors such as hypoxia or growth factors through the binding of stabilizing and destabilizing proteins at AU-rich elements located in the 3′-untranslated region. Thirdly, translation of VEGF-A mRNA is a controlled process involving alternative initiation codons, internal ribosome entry sites (IRESs), an upstream open reading frame (uORF), miRNA targeting and a riboswitch in the 3′ untranslated region. These different levels of regulation cooperate for the crucial fine-tuning of the expression of VEGF-A variants. This review will be focused on our current knowledge of the complex post-transcriptional regulatory switches that modulate the cellular VEGF-A level, a paradigmatic model of post-transcriptional regulation.
机译:血管内皮生长因子A(VEGF-A)是一种强力分泌的促有丝分裂原,对生理和病理性血管生成至关重要。 VEGF-A的转录后调控发生在多个水平。首先,选择性剪接产生编码不同同工型的不同转录本变体,这些同工型在受体结合和细胞外定位方面表现出独特的生物学特性。其次,VEGF-A mRNA的稳定性由诸如缺氧或生长因子等效应子通过稳定和去稳定蛋白在位于3'非翻译区的富含AU的元件的结合来调节。第三,VEGF-A mRNA的翻译是一个受控过程,涉及3'非翻译区的替代起始密码子,内部核糖体进入位点(IRESs),上游开放阅读框(uORF),miRNA靶向和核糖开关。这些不同水平的调节共同作用于VEGF-A变体表达的关键微调。这篇综述将集中于我们目前对复杂的转录后调控开关的了解,该开关调控细胞的VEGF-A水平,是转录后调控的典范模型。

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