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Gene regulation by sense-antisense overlap of polyadenylation signals.

机译:通过聚腺苷酸化信号的反义重叠进行基因调控。

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We show here that expression of genes from convergent transcription units can be regulated by the formation of double-stranded RNA (dsRNA) in the region of overlapping polyadenylation signals. The model system employed is the mouse polyomavirus. The early and late genes of polyomavirus are transcribed from opposite strands of the circular viral genome. At early times after infection, the early genes are expressed predominantly. Late gene expression increases dramatically upon the onset of DNA replication, when a major defect in polyadenylation of the late primary transcripts generates multigenomic RNAs that are precursors to the mature late mRNAs. Embedded in these late pre-mRNAs are sequences complementary to the early RNAs that act to down-regulate early gene expression via A-to-I editing of dsRNAs. In this system, the defective polyadenylation, and consequently the production of multigenomic late RNAs, depends on the context, and perhaps also, on the A-to-I editing of the poly(A) signal that overlaps the 3'-end of early transcripts.
机译:我们在这里表明,可以通过重叠的多腺苷酸化信号区域中双链RNA(dsRNA)的形成来调节来自收敛转录单位的基因表达。使用的模型系统是小鼠多瘤病毒。多瘤病毒的早期和晚期基因从环状病毒基因组的相反链转录而来。在感染后的早期,主要表达早期基因。 DNA复制开始后,晚期初级转录物的聚腺苷酸化的主要缺陷会产生多基因组RNA,而后者是成熟晚期mRNA的前体,因此晚期基因表达会急剧增加。嵌入这些晚期pre-mRNA中的是与早期RNA互补的序列,这些序列通过dsRNA的A至I编辑来下调早期基因表达。在该系统中,有缺陷的聚腺苷酸化以及因此产生的多基因组晚期RNA取决于环境,也许还取决于与早期3'端重叠的poly(A)信号的A至I编辑成绩单。

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