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Intronless mRNA transport elements may affect multiple steps of pre-mRNA processing.

机译:无内含子的mRNA转运元件可能会影响前mRNA加工的多个步骤。

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摘要

We have reported recently that a small element within the mouse histone H2a-coding region permits efficient cytoplasmic accumulation of intronless beta-globin cDNA transcripts. This sequence lowers the levels of spliced products from intron-containing constructs and can functionally replace Rev and the Rev-responsive element (RRE) in the nuclear export of unspliced HIV-1-related mRNAs. In work reported here, we further investigate the molecular mechanisms by which this element might work. We demonstrate here through both in vivo and in vitro assays that, in addition to promoting mRNA nuclear export, this element acts as a polyadenylation enhancer and as a potent inhibitor of splicing. Surprisingly, two other described intronless mRNA transport elements (from the herpes simplex virus thymidine kinase gene and hepatitis B virus) appear to function in a similar manner. These findings prompt us to suggest that a general feature of intronless mRNA transport elements might be a collection of phenotypes, including the inhibition of splicing and the enhancement of both polyadenylation and mRNA export.
机译:我们最近报道,在小鼠组蛋白H2a编码区域内的一个小元件允许无内含子的β-珠蛋白cDNA转录物的有效胞质积累。该序列降低了含内含子构建体的剪接产物的水平,并且可以在未剪接的HIV-1相关mRNA的核输出中功能性地代替Rev和Rev响应元件(RRE)。在这里报道的工作中,我们进一步研究了该元素可能起作用的分子机制。我们在这里通过体内和体外试验证明,除了促进mRNA核输出外,该元件还作为聚腺苷酸增强剂和有效的剪接抑制剂。令人惊讶地,其他两个所述的无内含子mRNA转运元件(来自单纯疱疹病毒胸苷激酶基因和乙型肝炎病毒)似乎以相似的方式起作用。这些发现促使我们建议,无内含子的mRNA转运元件的一般特征可能是表型的集合,包括抑制剪接以及增强聚腺苷酸化和mRNA输出。

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