ムービー
コントローラー
構造ビューア
万見文献について
+検索条件
-Structure paper
| タイトル | Flipped over U: structural basis for dsRNA cleavage by the SARS-CoV-2 endoribonuclease. |
|---|---|
| ジャーナル・号・ページ | Nucleic Acids Res, Vol. 50, Issue 14, Page 8290-8301, Year 2022 |
| 掲載日 | 2022年8月12日 |
 著者 | Meredith N Frazier / Isha M Wilson / Juno M Krahn / Kevin John Butay / Lucas B Dillard / Mario J Borgnia / Robin E Stanley |
| PubMed 要旨 | Coronaviruses generate double-stranded (ds) RNA intermediates during viral replication that can activate host immune sensors. To evade activation of the host pattern recognition receptor MDA5, ...Coronaviruses generate double-stranded (ds) RNA intermediates during viral replication that can activate host immune sensors. To evade activation of the host pattern recognition receptor MDA5, coronaviruses employ Nsp15, which is a uridine-specific endoribonuclease. Nsp15 is proposed to associate with the coronavirus replication-transcription complex within double-membrane vesicles to cleave these dsRNA intermediates. How Nsp15 recognizes and processes dsRNA is poorly understood because previous structural studies of Nsp15 have been limited to small single-stranded (ss) RNA substrates. Here we present cryo-EM structures of SARS-CoV-2 Nsp15 bound to a 52nt dsRNA. We observed that the Nsp15 hexamer forms a platform for engaging dsRNA across multiple protomers. The structures, along with site-directed mutagenesis and RNA cleavage assays revealed critical insight into dsRNA recognition and processing. To process dsRNA Nsp15 utilizes a base-flipping mechanism to properly orient the uridine within the active site for cleavage. Our findings show that Nsp15 is a distinctive endoribonuclease that can cleave both ss- and dsRNA effectively. |
 リンク | Nucleic Acids Res / PubMed:35801916 / PubMed Central |
| 手法 | EM (単粒子) |
| 解像度 | 3.2 - 3.43 Å |
| 構造データ | EMDB-25915, PDB-7tj2: EMDB-26073, PDB-7tqv: |
| 由来 |
|
 キーワード |  VIRAL PROTEIN/RNA (ウイルス性) / endoribonuclease / VIRAL PROTEIN (ウイルスタンパク質) / VIRAL PROTEIN-RNA complex (ウイルス性) |
