Literature DB >> 12810915

The dynamic nature of the four-way junction of the hepatitis C virus IRES.

Sonya E Melcher1, Timothy J Wilson, David M J Lilley.   

Abstract

Translation is initiated within the RNA of the hepatitis C virus at the internal ribosome entry site (IRES). The IRES is a 341-nucleotide element that contains a four-way helical junction (IIIabc) as a functionally important element of the secondary structure. The junction has three additional, nonpaired nucleotides at the point of strand exchange on one diagonal. We have studied the global conformation and folding of this junction in solution, using comparative gel electrophoresis and steady-state and time-resolved fluorescence resonance energy transfer. In the absence of divalent metal ions, the junction adopts an extended-square structure, in contrast to perfect four-way RNA junctions, which retain coaxial helical stacking under all conditions. The IIIabc junction is induced to fold on addition of Mg(2+), by pairwise coaxial stacking of arms, into the conformer in which the unpaired bases are located on the exchanging strands. Fluorescence lifetime measurements indicate that in the presence of Mg(2+) ions, the IIIabc junction exists in a dynamic equilibrium comprising approximately equal populations of antiparallel and parallel species. These dynamic properties may be important in mediating interactions between the IRES and the ribosome and initiation factors.

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Year:  2003        PMID: 12810915      PMCID: PMC1370448          DOI: 10.1261/rna.5130703

Source DB:  PubMed          Journal:  RNA        ISSN: 1355-8382            Impact factor:   4.942


  31 in total

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Journal:  Methods Enzymol       Date:  1992       Impact factor: 1.600

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  15 in total

1.  Structure of the three-way helical junction of the hepatitis C virus IRES element.

Authors:  Jonathan Ouellet; Sonya Melcher; Asif Iqbal; Yiliang Ding; David M J Lilley
Journal:  RNA       Date:  2010-06-25       Impact factor: 4.942

2.  Crystal structure of the HCV IRES central domain reveals strategy for start-codon positioning.

Authors:  Katherine E Berry; Shruti Waghray; Stefanie A Mortimer; Yun Bai; Jennifer A Doudna
Journal:  Structure       Date:  2011-10-12       Impact factor: 5.006

3.  Structure of the full-length HCV IRES in solution.

Authors:  Julien Pérard; Cédric Leyrat; Florence Baudin; Emmanuel Drouet; Marc Jamin
Journal:  Nat Commun       Date:  2013       Impact factor: 14.919

4.  Interconversion between parallel and antiparallel conformations of a 4H RNA junction in domain 3 of foot-and-mouth disease virus IRES captured by dynamics simulations.

Authors:  Segun Jung; Tamar Schlick
Journal:  Biophys J       Date:  2014-01-21       Impact factor: 4.033

Review 5.  Hierarchy of RNA functional dynamics.

Authors:  Anthony M Mustoe; Charles L Brooks; Hashim M Al-Hashimi
Journal:  Annu Rev Biochem       Date:  2014-03-05       Impact factor: 23.643

6.  Analysis of four-way junctions in RNA structures.

Authors:  Christian Laing; Tamar Schlick
Journal:  J Mol Biol       Date:  2009-05-13       Impact factor: 5.469

7.  The kink-turn motif in RNA is dimorphic, and metal ion-dependent.

Authors:  Terry A Goody; Sonya E Melcher; David G Norman; David M J Lilley
Journal:  RNA       Date:  2004-02       Impact factor: 4.942

Review 8.  Structure and function of HCV IRES domains.

Authors:  Peter J Lukavsky
Journal:  Virus Res       Date:  2008-07-31       Impact factor: 3.303

9.  Induced fit of RNA on binding the L7Ae protein to the kink-turn motif.

Authors:  Ben Turner; Sonya E Melcher; Timothy J Wilson; David G Norman; David M J Lilley
Journal:  RNA       Date:  2005-06-29       Impact factor: 4.942

10.  Hepatitis-C-virus-like internal ribosome entry sites displace eIF3 to gain access to the 40S subunit.

Authors:  Yaser Hashem; Amedee des Georges; Vidya Dhote; Robert Langlois; Hstau Y Liao; Robert A Grassucci; Tatyana V Pestova; Christopher U T Hellen; Joachim Frank
Journal:  Nature       Date:  2013-11-03       Impact factor: 49.962

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