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首页> 外文期刊>Progress in nucleic acid research and molecular biology >The search for trans-acting factors controlling messenger RNA decay.
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The search for trans-acting factors controlling messenger RNA decay.

机译:寻找控制信使RNA衰变的反式作用因子。

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摘要

Control of mRNA turnover is an integral component of regulated gene expression. Individual mRNAs display a wide range of stabilities, which in many cases have been linked to discrete sequence elements. The most extensively characterized determinants of rapid constitutive mRNA turnover in mammalian systems are A + U-rich elements (AREs), first identified in the 3' untranslated regions of many cytokine/lymphokine and protooncogene mRNAs. In this article, we describe recent advances in the characterization of ARE-directed mRNA turnover, including links to deadenylation kinetics and functional heterogeneity among AREs from different mRNAs. We then describe strategies employed in the search for trans-acting factors interacting with these elements. Using such techniques, an ARE-binding activity capable of accelerating c-myc mRNA turnover in vitro was identified, and named AUF1. Subsequent cloning and characterization revealed that AUF1 exists as a family of four proteins formed by alternative splicing of a common pre-mRNA and appears to function as part of a multisubunit trans-acting complex to promote ARE-directed mRNA turnover. Investigations using several systems have demonstrated that AUF1 expression and/or activity correlate with rapid decay of ARE-containing mRNAs, and that both expression and activity of AUF1 are regulated by developmental and signal transduction mechanisms.
机译:mRNA更新的控制是调控基因表达的组成部分。单个mRNA表现出广泛的稳定性,在许多情况下,这些稳定性已与离散序列元件相关联。哺乳动物系统中快速组成性mRNA转换的最广泛表征的决定因素是富含A + U的元件(ARE),首先在许多细胞因子/淋巴因子和原癌基因mRNA的3'非翻译区中发现。在本文中,我们描述了ARE指导的mRNA转换特征的最新进展,包括来自不同mRNA的ARE之间的腺苷酸化动力学和功能异质性的链接。然后,我们描述搜索与这些元素相互作用的反式作用因子时所采用的策略。使用这样的技术,鉴定了能够在体外加速c-myc mRNA更新的ARE结合活性,并将其命名为AUF1。随后的克隆和表征表明,AUF1作为四种蛋白质的家族存在,这些蛋白质是由常见的pre-mRNA的可变剪接形成的,并且似乎起多亚基反作用复合物的一部分的作用,从而促进ARE定向的mRNA转换。使用几种系统的研究表明,AUF1的表达和/或活性与含有ARE的mRNA的快速衰减相关,并且AUF1的表达和活性均受发育和信号转导机制的调节。

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