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The Hinge Region of the Israeli Acute Paralysis Virus Internal Ribosome Entry Site Directs Ribosomal Positioning, Translational Activity, and Virus Infection

J Virol. 2022-01; 
Mathew P Kirby, Ciara Stevenson, Liam J Worrall, Yihang Chen, Christina Young, Jisoo Youm, Natalie C J Strynadka, Douglas W Allan, Eric Jan
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Polyclonal Antibody Services … The TM IAPV IRES denotes mutations that disrupt all three pseudoknots (25). Shown are … VP2) rabbit polyclonal antibody (1:10000, Genscript) and mouse antitubulin antibody (1:1000; … Get A Quote

摘要

All viruses must usurp host ribosomes for viral protein synthesis. Dicistroviruses utilize an intergenic region internal ribosome entry site (IGR IRES) to directly recruit ribosomes and mediate translation initiation from a non-AUG start codon. The IGR IRES adopts a three-pseudoknot structure that comprises a ribosome binding domain of pseudoknot II and III (PKII and PKIII), and a tRNA-like anticodon domain (PKI) connected via a short, one to three nucleotide hinge region. Recent cryo-EM structural analysis of the dicistrovirus Taura syndrome virus (TSV) IGR IRES bound to the ribosome suggests that the hinge region may facilitate translocation of the IRES from the ribosomal A to P site. In this study, we provid... More

關鍵詞

IRES, Israeli acute paralysis virus, RNA, RNA structure, RNA virus, infectious clones, internal ribosome entry site, ribosome, translation, translational control, virus
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