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Potential physiological roles of the 31/32-nucleotide Y4-RNA fragment in human plasma

机译:31/32核苷酸Y4-RNA片段在人血浆中的潜在生理作用

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摘要

The 31- and 32-nt 5′-fragments of Y4-RNA (Y4RNAfr) exist abundantly in human plasma. The Y4RNAfr can function as 5′-half-tRNA-type sgRNA for tRNase Z , although we do not know yet what its physiological roles are and what cellular RNAs are its genuine targets. In this paper, we analyzed the effects of the Y4RNAfr on cell viability and transcriptomes using HL60, RPMI-8226, and HEK293 cells, and Y4RNAfr-binding RNAs in A549 cells. Although the Y4RNAfr hardly affected the viability of HL60, RPMI-8226, and HEK293 cells, it significantly affected their transcriptome. The DAVID analysis for > 2-fold upregulated and downregulated genes suggested that the Y4RNAfr may affect various KEGG pathways. We obtained 108 Y4RNAfr-binding RNAs in A549 cells, searched potential secondary structures of complexes between theY4RNAfr and its binding RNAs for the pre-tRNA-like structure, and found many such structures. One of the five best fitted structures was for the MKI67 mRNA, suggesting that the Y4RNAfr can decrease the cellular MKI67 level through guiding the cleavage of the MKI67 mRNA by tRNase Z . This may be one of the underlying mechanisms for the reported observation that the Y4RNAfr suppresses the proliferation of A549 cells.
机译:Y4-RNA(Y4RNAfr)的31和32 nt 5'片段在人体血浆中大量存在。 Y4RNAfr可以作为tRNase Z的5'-half-tRNA型sgRNA,尽管我们尚不清楚其生理作用是什么,什么细胞RNA是其真正的靶标。在本文中,我们使用HL60,RPMI-8226和HEK293细胞以及A549细胞中的Y4RNAfr结合RNA分析了Y4RNAfr对细胞活力和转录组的影响。尽管Y4RNAfr几乎不会影响HL60,RPMI-8226和HEK293细胞的活力,但会显着影响其转录组。超过2倍的上调和下调基因的DAVID分析表明,Y4RNAfr可能影响各种KEGG途径。我们在A549细胞中获得了108个与Y4RNAfr结合的RNA,搜索了Y4RNAfr及其结合RNA之间的复合物的潜在二级结构,以获得pre-tRNA样结构,并发现了许多这样的结构。五个最合适的结构之一是MKI67 mRNA,这表明Y4RNAfr可以通过指导tRNase Z切割MKI67 mRNA来降低细胞MKI67水平。这可能是报道的观察到的Y4RNAfr抑制A549细胞增殖的潜在机制之一。

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