4.6 Article

Universal and strain specific structure features of segment 8 genomic RNA of influenza A virus-application of 4-thiouridine photocrosslinking

期刊

JOURNAL OF BIOLOGICAL CHEMISTRY
卷 297, 期 6, 页码 -

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ELSEVIER
DOI: 10.1016/j.jbc.2021.101245

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资金

  1. National Science Centre [UMO-2020/01/0/NZ6/00137, UMO-2019/33/B/ST4/01422, UMO-2017/25/B/NZ1/02269]
  2. NIH/NIGMS [R00GM112877, R01GM133810]
  3. Roy J. Carver Charitable Trust

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In this study, RNA secondary structures of influenza A virus were determined using chemical mapping and 4-thiouridine (4sU) crosslinking, revealing both universal and unique features of different strains. The method highlighted the three-dimensional properties and allowed for proposing long-range interactions in the RNA secondary structure. The combination of 4sU mapping with chemical mapping and bioinformatic analysis could enhance RNA structure determination and target recognition for antisense strategies or viral RNA detection.
RNA structure in the influenza A virus (IAV) has been the focus of several studies that have shown connections between conserved secondary structure motifs and their biological function in the virus replication cycle. Questions have arisen on how to best recognize and understand the pandemic properties of IAV strains from an RNA perspective, but determination of the RNA secondary structure has been challenging. Herein, we used chemical mapping to determine the secondary structure of segment 8 viral RNA (vRNA) of the pandemic A/California/04/ 2009 (H1N1) strain of IAV. Additionally, this long, naturally occurring RNA served as a model to evaluate RNA mapping with 4-thiouridine (4sU) crosslinking. We explored 4-thiouridine as a probe of nucleotides in close proximity, through its incorporation into newly transcribed RNA and subsequent photoactivation. RNA secondary structural features both universal to type A strains and unique to the A/California/04/2009 (H1N1) strain were recognized. 4sU mapping confirmed and facilitated RNA structure prediction, according to several rules: 4sU photocross-linking forms efficiently in the double-stranded region of RNA with some flexibility, in the ends of helices, and across bulges and loops when their structural mobility is permitted. This method highlighted three-dimensional properties of segment 8 vRNA secondary structure motifs and allowed to propose several long-range three-dimensional interactions. 4sU mapping combined with chemical mapping and bioinformatic analysis could be used to enhance the RNA structure determination as well as recognition of target regions for antisense strategies or viral RNA detection.

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