HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators

Frameshifting during translation of viral or in rare cases cellular mRNA results in the synthesis of proteins from two overlapping reading frames within the same mRNA. In HIV-1 the protease, reverse transcriptase, and integrase enzymes are in a second reading frame relative to the structural group-s...

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Autores principales: Cardno, Tony S., Shimaki, Yosuke, Sleebs, Brad E., Lackovic, Kurt, Parisot, John P., Moss, Rebecca M., Crowe-McAuliffe, Caillan, Mathew, Suneeth F., Edgar, Christina D., Kleffmann, Torsten, Tate, Warren P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4598141/
https://www.ncbi.nlm.nih.gov/pubmed/26447468
http://dx.doi.org/10.1371/journal.pone.0139036
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author Cardno, Tony S.
Shimaki, Yosuke
Sleebs, Brad E.
Lackovic, Kurt
Parisot, John P.
Moss, Rebecca M.
Crowe-McAuliffe, Caillan
Mathew, Suneeth F.
Edgar, Christina D.
Kleffmann, Torsten
Tate, Warren P.
author_facet Cardno, Tony S.
Shimaki, Yosuke
Sleebs, Brad E.
Lackovic, Kurt
Parisot, John P.
Moss, Rebecca M.
Crowe-McAuliffe, Caillan
Mathew, Suneeth F.
Edgar, Christina D.
Kleffmann, Torsten
Tate, Warren P.
author_sort Cardno, Tony S.
collection PubMed
description Frameshifting during translation of viral or in rare cases cellular mRNA results in the synthesis of proteins from two overlapping reading frames within the same mRNA. In HIV-1 the protease, reverse transcriptase, and integrase enzymes are in a second reading frame relative to the structural group-specific antigen (gag), and their synthesis is dependent upon frameshifting. This ensures that a strictly regulated ratio of structural proteins and enzymes, which is critical for HIV-1 replication and viral infectivity, is maintained during protein synthesis. The frameshift element in HIV-1 RNA is an attractive target for the development of a new class of anti HIV-1 drugs. However, a number of examples are now emerging of human genes using −1 frameshifting, such as PEG10 and CCR5. In this study we have compared the HIV-1 and PEG10 frameshift elements and shown they have distinct functional characteristics. Frameshifting occurs at several points within each element. Moreover, frameshift modulators that were isolated by high-throughput screening of a library of 114,000 lead-like compounds behaved differently with the PEG10 frameshift element. The most effective compounds affecting the HIV-1 element enhanced frameshifting by 2.5-fold at 10 μM in two different frameshift reporter assay systems. HIV-1 protease:gag protein ratio was affected by a similar amount in a specific assay of virally-infected cultured cell, but the modulation of frameshifting of the first-iteration compounds was not sufficient to show significant effects on viral infectivity. Importantly, two compounds did not affect frameshifting with the human PEG10 element, while one modestly inhibited rather than enhanced frameshifting at the human element. These studies indicate that frameshift elements have unique characteristics that may allow targeting of HIV-1 and of other viruses specifically for development of antiviral therapeutic molecules without effect on human genes like PEG10 that use the same generic mechanism.
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spelling pubmed-45981412015-10-20 HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators Cardno, Tony S. Shimaki, Yosuke Sleebs, Brad E. Lackovic, Kurt Parisot, John P. Moss, Rebecca M. Crowe-McAuliffe, Caillan Mathew, Suneeth F. Edgar, Christina D. Kleffmann, Torsten Tate, Warren P. PLoS One Research Article Frameshifting during translation of viral or in rare cases cellular mRNA results in the synthesis of proteins from two overlapping reading frames within the same mRNA. In HIV-1 the protease, reverse transcriptase, and integrase enzymes are in a second reading frame relative to the structural group-specific antigen (gag), and their synthesis is dependent upon frameshifting. This ensures that a strictly regulated ratio of structural proteins and enzymes, which is critical for HIV-1 replication and viral infectivity, is maintained during protein synthesis. The frameshift element in HIV-1 RNA is an attractive target for the development of a new class of anti HIV-1 drugs. However, a number of examples are now emerging of human genes using −1 frameshifting, such as PEG10 and CCR5. In this study we have compared the HIV-1 and PEG10 frameshift elements and shown they have distinct functional characteristics. Frameshifting occurs at several points within each element. Moreover, frameshift modulators that were isolated by high-throughput screening of a library of 114,000 lead-like compounds behaved differently with the PEG10 frameshift element. The most effective compounds affecting the HIV-1 element enhanced frameshifting by 2.5-fold at 10 μM in two different frameshift reporter assay systems. HIV-1 protease:gag protein ratio was affected by a similar amount in a specific assay of virally-infected cultured cell, but the modulation of frameshifting of the first-iteration compounds was not sufficient to show significant effects on viral infectivity. Importantly, two compounds did not affect frameshifting with the human PEG10 element, while one modestly inhibited rather than enhanced frameshifting at the human element. These studies indicate that frameshift elements have unique characteristics that may allow targeting of HIV-1 and of other viruses specifically for development of antiviral therapeutic molecules without effect on human genes like PEG10 that use the same generic mechanism. Public Library of Science 2015-10-08 /pmc/articles/PMC4598141/ /pubmed/26447468 http://dx.doi.org/10.1371/journal.pone.0139036 Text en © 2015 Cardno et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Cardno, Tony S.
Shimaki, Yosuke
Sleebs, Brad E.
Lackovic, Kurt
Parisot, John P.
Moss, Rebecca M.
Crowe-McAuliffe, Caillan
Mathew, Suneeth F.
Edgar, Christina D.
Kleffmann, Torsten
Tate, Warren P.
HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title_full HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title_fullStr HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title_full_unstemmed HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title_short HIV-1 and Human PEG10 Frameshift Elements Are Functionally Distinct and Distinguished by Novel Small Molecule Modulators
title_sort hiv-1 and human peg10 frameshift elements are functionally distinct and distinguished by novel small molecule modulators
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4598141/
https://www.ncbi.nlm.nih.gov/pubmed/26447468
http://dx.doi.org/10.1371/journal.pone.0139036
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