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Role of 3’-untranslated region translational control in cancer development diagnostics and treatment

机译:3-非翻译区翻译控制在癌症发展诊断和治疗中的作用

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摘要

The messenger RNA 3’-untranslated region (3’UTR) plays an important role in regulation of gene expression on the posttranscriptional level. The 3’UTR controls gene expression via orchestrated interaction between the structural components of mRNAs (cis-element) and the specific trans-acting factors (RNA binding proteins and non-coding RNAs). The crosstalk of these factors is based on the binding sequences and/or direct protein-protein interaction, or just functional interaction. Much new evidence that has accumulated supports the idea that several RNA binding factors can bind to common mRNA targets: to the non-overlapping binding sites or to common sites in a competitive fashion. Various factors capable of binding to the same RNA can cooperate or be antagonistic in their actions. The outcome of the collective function of all factors bound to the same mRNA 3’UTR depends on many circumstances, such as their expression levels, affinity to the binding sites, and localization in the cell, which can be controlled by various physiological conditions. Moreover, the functional and/or physical interactions of the factors binding to 3’UTR can change the character of their actions. These interactions vary during the cell cycle and in response to changing physiological conditions. Abnormal functioning of the factors can lead to disease. In this review we will discuss how alterations of these factors or their interaction can affect cancer development and promote or enhance the malignant phenotype of cancer cells. Understanding these alterations and their impact on 3’UTR-directed posttranscriptional gene regulation will uncover promising new targets for therapeutic intervention and diagnostics. We will also discuss emerging new tools in cancer diagnostics and therapy based on 3’UTR binding factors and approaches to improve them.
机译:信使RNA 3'非翻译区(3'UTR)在转录后水平上对基因表达的调节起着重要作用。 3’UTR通过mRNA的结构成分(顺式元件)与特定反式作用因子(RNA结合蛋白和非编码RNA)之间的协调相互作用来控制基因表达。这些因素的串扰基于结合序列和/或直接的蛋白质-蛋白质相互作用,或仅基于功能相互作用。积累的许多新证据支持以下观点:几种RNA结合因子可以与常见的mRNA靶结合:以竞争的方式与非重叠结合位点或与共同位点结合。能够结合相同RNA的各种因素在其作用上可以相互配合或拮抗。绑定到同一mRNA 3’UTR的所有因子的集体功能的结果取决于许多情况,例如它们的表达水平,对结合位点的亲和力以及细胞内的定位,这些可以通过各种生理条件来控制。此外,与3’UTR结合的因子的功能和/或物理相互作用可以改变其行为的特征。这些相互作用在细胞周期中和响应于变化的生理条件而变化。这些因素的功能异常会导致疾病。在这篇综述中,我们将讨论这些因素的改变或它们之间的相互作用如何影响癌症的发展并促进或增强癌细胞的恶性表型。了解这些改变及其对3’UTR定向转录后基因调控的影响,将为治疗干预和诊断发现有希望的新靶标。我们还将讨论基于3’UTR结合因子的癌症诊断和治疗中正在出现的新工具及其改进方法。

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