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The mechanism of ribosomal recruitment during translation initiation on the Type 2 encephalomyocarditis virus IRES

The EMBO Journal. 2026-03; 
Sayan Bhattacharjee, Irina S Abaeva, Zuben P Brown, Yani Arhab, Hengameh Fallah, Christopher U T Hellen, Joachim Frank, Tatyana V Pestova
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Protein Electrophoresis and Western SurePAGE 4–12% Bis-Tris gels (GenScript) MES SDS Running buffer (GenScript) 373–1656 or EMCV nt. 373–987 (GenBank: M81861.1) inserted intopUC57, and mutants derived from these plasmids were made by GenScript Corp. Get A Quote
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摘要

The encephalomyocarditis virus (EMCV) internal ribosomal entry side (IRES) and other Type 2 IRESs favor translation of the viral genome during infection. The domains H-L of these IRESs specifically interact with the cellular translation initiation factors eIF4G/eIF4A through their essential JK domain. However, the JK domain is not sufficient for IRES activity, which also strictly requires the preceding domain I of unknown function. To identify interactions that drive ribosomal attachment to eIF4G/eIF4A-bound Type 2 IRESs, we determined the cryo-EM structure of 48S initiation complexes formed on the EMCV IRES. The apical cloverleaf of domain I contacts ribosomal proteins uS13 and uS19 via its subdomain Id, where... More

关键词

Cryo-EM; GNRA tetraloop; IRES; Picornavirus; Translation initiation.