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A viral microRNA functions as an orthologue of cellular miR-155

机译:病毒microRNA充当细胞miR-155的直系同源物

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摘要

All metazoan eukaryotes express microRNAs (miRNAs), roughly 22-nucleotide regulatory RNAs that can repress the expression of messenger RNAs bearing complementary sequences. Several DNA viruses also express miRNAs in infected cells, suggesting a role in viral replication and pathogenesis. Although specific viral miRNAs have been shown to autoregulate viral mRNAs or downregulate cellular mRNAs, the function of most viral miRNAs remains unknown. Here we report that the miR-K12-11 miRNA encoded by Kaposi's-sarcoma-associated herpes virus (KSHV) shows significant homology to cellular miR-155, including the entire miRNA 'seed' region. Using a range of assays, we show that expression of physiological levels of miR-K12-11 or miR-155 results in the downregulation of an extensive set of common mRNA targets, including genes with known roles in cell growth regulation. Our findings indicate that viral miR-K12-11 functions as an orthologue of cellular miR-155 and probably evolved to exploit a preexisting gene regulatory pathway in B cells. Moreover, the known aetiological role of miR-155 in B-cell transformation suggests that miR-K12-11 may contribute to the induction of KSHV-positive B-cell tumours in infected patients.
机译:所有后生真核生物均表达microRNA(miRNA),约22个核苷酸的调节性RNA,可抑制带有互补序列的信使RNA的表达。几种DNA病毒还在受感染的细胞中表达miRNA,提示在病毒复制和发病机理中起作用。尽管已经显示出特定的病毒miRNA可以自动调节病毒mRNA或下调细胞mRNA,但是大多数病毒miRNA的功能仍然未知。在这里,我们报道由卡波西氏肉瘤相关疱疹病毒(KSHV)编码的miR-K12-11 miRNA与细胞miR-155具有显着的同源性,包括整个miRNA“种子”区域。使用一系列分析方法,我们显示了miR-K12-11或miR-155生理水平的表达导致广泛的一组常见mRNA目标的下调,包括在细胞生长调节中具有已知作用的基因。我们的发现表明,病毒miR-K12-11充当细胞miR-155的直向同源物,并且可能进化为利用B细胞中预先存在的基因调控途径。此外,miR-155在B细胞转化中的已知病因学作用表明,miR-K12-11可能有助于在感染患者中诱导KSHV阳性B细胞肿瘤。

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