Literature DB >> 16014945

A peptide derived from RNA recognition motif 2 of human la protein binds to hepatitis C virus internal ribosome entry site, prevents ribosomal assembly, and inhibits internal initiation of translation.

Renuka Pudi1, Sudhamani S Ramamurthy, Saumitra Das.   

Abstract

Human La protein is known to interact with hepatitis C virus (HCV) internal ribosome entry site (IRES) and stimulate translation. Previously, we demonstrated that mutations within HCV SL IV lead to reduced binding to La-RNA recognition motif 2 (RRM2) and drastically affect HCV IRES-mediated translation. Also, the binding of La protein to SL IV of HCV IRES was shown to impart conformational alterations within the RNA so as to facilitate the formation of functional initiation complex. Here, we report that a synthetic peptide, LaR2C, derived from the C terminus of La-RRM2 competes with the binding of cellular La protein to the HCV IRES and acts as a dominant negative inhibitor of internal initiation of translation of HCV RNA. The peptide binds to the HCV IRES and inhibits the functional initiation complex formation. An Huh7 cell line constitutively expressing a bicistronic RNA in which both cap-dependent and HCV IRES-mediated translation can be easily assayed has been developed. The addition of purified TAT-LaR2C recombinant polypeptide that allows direct delivery of the peptide into the cells showed reduced expression of HCV IRES activity in this cell line. The study reveals valuable insights into the role of La protein in ribosome assembly at the HCV IRES and also provides the basis for targeting ribosome-HCV IRES interaction to design potent antiviral therapy.

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Year:  2005        PMID: 16014945      PMCID: PMC1181605          DOI: 10.1128/JVI.79.15.9842-9853.2005

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


  39 in total

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7.  Hepatitis C virus internal ribosome entry site-mediated translation is stimulated by specific interaction of independent regions of human La autoantigen.

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8.  A peptide from autoantigen La blocks poliovirus and hepatitis C virus cap-independent translation and reveals a single tyrosine critical for La RNA binding and translation stimulation.

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Journal:  J Virol       Date:  2004-04       Impact factor: 5.103

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Journal:  Nucleic Acids Res       Date:  2004-03-12       Impact factor: 16.971

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  10 in total

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3.  Structural determinant of human La protein critical for internal initiation of translation of hepatitis C virus RNA.

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4.  Proanthocyanidin from blueberry leaves suppresses expression of subgenomic hepatitis C virus RNA.

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5.  Specific sequence of a Beta turn in human la protein may contribute to species specificity of hepatitis C virus.

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Review 6.  Hepatitis C virus translation inhibitors targeting the internal ribosomal entry site.

Authors:  Sergey M Dibrov; Jerod Parsons; Maia Carnevali; Shu Zhou; Kevin D Rynearson; Kejia Ding; Emily Garcia Sega; Nicholas D Brunn; Mark A Boerneke; Maria P Castaldi; Thomas Hermann
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7.  Catalytic metallodrugs based on the LaR2C peptide target HCV SLIV IRES RNA.

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Review 10.  Exploring Internal Ribosome Entry Sites as Therapeutic Targets.

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  10 in total

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