A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting

<p>Abstract</p> <p>Japanese encephalitis, West Nile, Usutu and Murray Valley encephalitis viruses form a tight subgroup within the larger <it>Flavivirus </it>genus. These viruses utilize a single-polyprotein expression strategy, resulting in ~10 mature proteins. Plottin...

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Main Authors: Atkins John F, Firth Andrew E
Format: Article
Language:English
Published: BMC 2009-02-01
Series:Virology Journal
Online Access:http://www.virologyj.com/content/6/1/14
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spelling doaj-26257858e359446aa87cebfd35d98c2f2020-11-24T21:44:39ZengBMCVirology Journal1743-422X2009-02-01611410.1186/1743-422X-6-14A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshiftingAtkins John FFirth Andrew E<p>Abstract</p> <p>Japanese encephalitis, West Nile, Usutu and Murray Valley encephalitis viruses form a tight subgroup within the larger <it>Flavivirus </it>genus. These viruses utilize a single-polyprotein expression strategy, resulting in ~10 mature proteins. Plotting the conservation at synonymous sites along the polyprotein coding sequence reveals strong conservation peaks at the very 5' end of the coding sequence, and also at the 5' end of the sequence encoding the NS2A protein. Such peaks are generally indicative of functionally important non-coding sequence elements. The second peak corresponds to a predicted stable pseudoknot structure whose biological importance is supported by compensatory mutations that preserve the structure. The pseudoknot is preceded by a conserved slippery heptanucleotide (Y CCU UUU), thus forming a classical stimulatory motif for -1 ribosomal frameshifting. We hypothesize, therefore, that the functional importance of the pseudoknot is to stimulate a portion of ribosomes to shift -1 nt into a short (45 codon), conserved, overlapping open reading frame, termed <it>foo</it>. Since cleavage at the NS1-NS2A boundary is known to require synthesis of NS2A in <it>cis</it>, the resulting transframe fusion protein is predicted to be NS1-NS2A<sup>N-term</sup>-FOO. We hypothesize that this may explain the origin of the previously identified NS1 'extension' protein in JEV-group flaviviruses, known as NS1'.</p> http://www.virologyj.com/content/6/1/14
collection DOAJ
language English
format Article
sources DOAJ
author Atkins John F
Firth Andrew E
spellingShingle Atkins John F
Firth Andrew E
A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
Virology Journal
author_facet Atkins John F
Firth Andrew E
author_sort Atkins John F
title A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
title_short A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
title_full A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
title_fullStr A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
title_full_unstemmed A conserved predicted pseudoknot in the NS2A-encoding sequence of West Nile and Japanese encephalitis flaviviruses suggests NS1' may derive from ribosomal frameshifting
title_sort conserved predicted pseudoknot in the ns2a-encoding sequence of west nile and japanese encephalitis flaviviruses suggests ns1' may derive from ribosomal frameshifting
publisher BMC
series Virology Journal
issn 1743-422X
publishDate 2009-02-01
description <p>Abstract</p> <p>Japanese encephalitis, West Nile, Usutu and Murray Valley encephalitis viruses form a tight subgroup within the larger <it>Flavivirus </it>genus. These viruses utilize a single-polyprotein expression strategy, resulting in ~10 mature proteins. Plotting the conservation at synonymous sites along the polyprotein coding sequence reveals strong conservation peaks at the very 5' end of the coding sequence, and also at the 5' end of the sequence encoding the NS2A protein. Such peaks are generally indicative of functionally important non-coding sequence elements. The second peak corresponds to a predicted stable pseudoknot structure whose biological importance is supported by compensatory mutations that preserve the structure. The pseudoknot is preceded by a conserved slippery heptanucleotide (Y CCU UUU), thus forming a classical stimulatory motif for -1 ribosomal frameshifting. We hypothesize, therefore, that the functional importance of the pseudoknot is to stimulate a portion of ribosomes to shift -1 nt into a short (45 codon), conserved, overlapping open reading frame, termed <it>foo</it>. Since cleavage at the NS1-NS2A boundary is known to require synthesis of NS2A in <it>cis</it>, the resulting transframe fusion protein is predicted to be NS1-NS2A<sup>N-term</sup>-FOO. We hypothesize that this may explain the origin of the previously identified NS1 'extension' protein in JEV-group flaviviruses, known as NS1'.</p>
url http://www.virologyj.com/content/6/1/14
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