Literature DB >> 31619563

Ribosomal Protein L13 Promotes IRES-Driven Translation of Foot-and-Mouth Disease Virus in a Helicase DDX3-Dependent Manner.

Shichong Han1,2, Shiqi Sun2, Pinghua Li2, Qun Liu1, Zhihui Zhang2, Hu Dong2, Mengmeng Sun1, Wenxue Wu1, Xiaojia Wang3, Huichen Guo4.   

Abstract

Internal ribosome entry site (IRES)-driven translation is a common strategy among positive-sense, single-stranded RNA viruses for bypassing the host cell requirement of a 5' cap structure. In the current study, we identified the ribosomal protein L13 (RPL13) as a critical regulator of IRES-driven translation of foot-and-mouth disease virus (FMDV) but found that it is not essential for cellular global translation. RPL13 is also a determinant for translation and infection of Seneca Valley virus (SVV) and classical swine fever virus (CSFV), and this suggests that its function may also be conserved in unrelated IRES-containing viruses. We further showed that depletion of DEAD box helicase DDX3 disrupts binding of RPL13 to the FMDV IRES, whereas the reduction in RPL13 expression impairs the ability of DDX3 to promote IRES-driven translation directly. DDX3 cooperates with RPL13 to support the assembly of 80S ribosomes for optimal translation initiation of viral mRNA. Finally, we demonstrated that DDX3 affects the recruitment of the eukaryotic initiation factor eIF3 subunits e and j to the viral IRES. This work provides the first connection between DDX3 and eIF3e/j and recognition of the role of RPL13 in modulating viral IRES-dependent translation. This previously uncharacterized process may be involved in selective mRNA translation.IMPORTANCE Accumulating evidence has unveiled the roles of ribosomal proteins (RPs) belonging to the large 60S subunit in regulating selective translation of specific mRNAs. The translation specificity of the large-subunit RPs in this process is thought provoking, given the role they play canonically in catalyzing peptide bond formation. Here, we have identified the ribosomal protein L13 (RPL13) as a critical regulator of IRES-driven translation during FMDV infection. Our study supports a model whereby the FMDV IRESs recruit helicase DDX3 recognizing RPL13 to facilitate IRES-driven translation, with the assistance of eIF3e and eIF3j. A better understanding of these specific interactions surrounding IRES-mediated translation initiation could have important implications for the selective translation of viral mRNA and thus for the development of effective prevention of viral infection.
Copyright © 2020 American Society for Microbiology.

Entities:  

Keywords:  DEAD box helicase 3; eukaryotic initiation factor 3; foot-and-mouth disease virus; internal ribosome entry site; ribosomal protein L13; translation initiation

Mesh:

Substances:

Year:  2020        PMID: 31619563      PMCID: PMC6955262          DOI: 10.1128/JVI.01679-19

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  90 in total

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Journal:  Trends Biochem Sci       Date:  2006-08-22       Impact factor: 13.807

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Journal:  Science       Date:  1997-03-07       Impact factor: 47.728

Review 3.  Viral IRES RNA structures and ribosome interactions.

Authors:  Jeffrey S Kieft
Journal:  Trends Biochem Sci       Date:  2008-05-28       Impact factor: 13.807

4.  Structure of the human 80S ribosome.

Authors:  Heena Khatter; Alexander G Myasnikov; S Kundhavai Natchiar; Bruno P Klaholz
Journal:  Nature       Date:  2015-04-22       Impact factor: 49.962

5.  Ribosomes take control.

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7.  The j-subunit of human translation initiation factor eIF3 is required for the stable binding of eIF3 and its subcomplexes to 40 S ribosomal subunits in vitro.

Authors:  Christopher S Fraser; Jennifer Y Lee; Greg L Mayeur; Martin Bushell; Jennifer A Doudna; John W B Hershey
Journal:  J Biol Chem       Date:  2003-12-19       Impact factor: 5.157

8.  The pathway of hepatitis C virus mRNA recruitment to the human ribosome.

Authors:  Christopher S Fraser; John W B Hershey; Jennifer A Doudna
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10.  The DEAD-box helicase DDX3X is a critical component of the TANK-binding kinase 1-dependent innate immune response.

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Journal:  EMBO J       Date:  2008-06-26       Impact factor: 11.598

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2.  Nucleolin Promotes IRES-Driven Translation of Foot-and-Mouth Disease Virus by Supporting the Assembly of Translation Initiation Complexes.

Authors:  Shichong Han; Xiaojia Wang; Junyong Guan; Jinen Wu; Yun Zhang; Pinghua Li; Zaixin Liu; Sahibzada Waheed Abdullah; Zhihui Zhang; Ye Jin; Shiqi Sun; Huichen Guo
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6.  The DDX23 Negatively Regulates Translation and Replication of Foot-and-Mouth Disease Virus and Is Degraded by 3C Proteinase.

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Review 7.  RNA Helicase DDX3: A Double-Edged Sword for Viral Replication and Immune Signaling.

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10.  Ribosomal Protein L13 Participates in Innate Immune Response Induced by Foot-and-Mouth Disease Virus.

Authors:  Junyong Guan; Shichong Han; Jin'en Wu; Yun Zhang; Manyuan Bai; Sahibzada Waheed Abdullah; Shiqi Sun; Huichen Guo
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