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Anti-tetherin activities in Vpu-expressing primate lentiviruses

BACKGROUND: The anti-viral activity of the cellular restriction factor, BST-2/tetherin, was first observed as an ability to block the release of Vpu-minus HIV-1 from the surface of infected cells. However, tetherin restriction is also counteracted by primate lentiviruses that do not express a Vpu pr...

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Autores principales: Yang, Su Jung, Lopez, Lisa A, Hauser, Heiko, Exline, Colin M, Haworth, Kevin G, Cannon, Paula M
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2831821/
https://www.ncbi.nlm.nih.gov/pubmed/20167081
http://dx.doi.org/10.1186/1742-4690-7-13
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author Yang, Su Jung
Lopez, Lisa A
Hauser, Heiko
Exline, Colin M
Haworth, Kevin G
Cannon, Paula M
author_facet Yang, Su Jung
Lopez, Lisa A
Hauser, Heiko
Exline, Colin M
Haworth, Kevin G
Cannon, Paula M
author_sort Yang, Su Jung
collection PubMed
description BACKGROUND: The anti-viral activity of the cellular restriction factor, BST-2/tetherin, was first observed as an ability to block the release of Vpu-minus HIV-1 from the surface of infected cells. However, tetherin restriction is also counteracted by primate lentiviruses that do not express a Vpu protein, where anti-tetherin functions are provided by either the Env protein (HIV-2, SIVtan) or the Nef protein (SIVsm/mac and SIVagm). Within the primate lentiviruses, Vpu is also present in the genomes of SIVcpz and certain SIVsyk viruses. We asked whether, in these viruses, anti-tetherin activity was always a property of Vpu, or if it had selectively evolved in HIV-1 to perform this function. RESULTS: We found that despite the close relatedness of HIV-1 and SIVcpz, the chimpanzee viruses use Nef instead of Vpu to counteract tetherin. Furthermore, SIVcpz Nef proteins had activity against chimpanzee but not human tetherin. This specificity mapped to a short sequence that is present in the cytoplasmic tail of primate but not human tetherins, and this also accounts for the specificity of SIVsm/mac Nef for primate but not human tetherins. In contrast, Vpu proteins from four diverse members of the SIVsyk lineage all displayed an anti-tetherin activity that was active against macaque tetherin. Interestingly, Vpu from a SIVgsn isolate was also found to have activity against human tetherin. CONCLUSIONS: Primate lentiviruses show a high degree of flexibility in their use of anti-tetherin factors, indicating a strong selective pressure to counteract tetherin restriction. The identification of an activity against human tetherin in SIVgsn Vpu suggests that the presence of Vpu in the ancestral SIVmus/mon/gsn virus believed to have contributed the 3' half of the HIV-1 genome may have played a role in the evolution of viruses that could counteract human tetherin and infect humans.
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spelling pubmed-28318212010-03-04 Anti-tetherin activities in Vpu-expressing primate lentiviruses Yang, Su Jung Lopez, Lisa A Hauser, Heiko Exline, Colin M Haworth, Kevin G Cannon, Paula M Retrovirology Research BACKGROUND: The anti-viral activity of the cellular restriction factor, BST-2/tetherin, was first observed as an ability to block the release of Vpu-minus HIV-1 from the surface of infected cells. However, tetherin restriction is also counteracted by primate lentiviruses that do not express a Vpu protein, where anti-tetherin functions are provided by either the Env protein (HIV-2, SIVtan) or the Nef protein (SIVsm/mac and SIVagm). Within the primate lentiviruses, Vpu is also present in the genomes of SIVcpz and certain SIVsyk viruses. We asked whether, in these viruses, anti-tetherin activity was always a property of Vpu, or if it had selectively evolved in HIV-1 to perform this function. RESULTS: We found that despite the close relatedness of HIV-1 and SIVcpz, the chimpanzee viruses use Nef instead of Vpu to counteract tetherin. Furthermore, SIVcpz Nef proteins had activity against chimpanzee but not human tetherin. This specificity mapped to a short sequence that is present in the cytoplasmic tail of primate but not human tetherins, and this also accounts for the specificity of SIVsm/mac Nef for primate but not human tetherins. In contrast, Vpu proteins from four diverse members of the SIVsyk lineage all displayed an anti-tetherin activity that was active against macaque tetherin. Interestingly, Vpu from a SIVgsn isolate was also found to have activity against human tetherin. CONCLUSIONS: Primate lentiviruses show a high degree of flexibility in their use of anti-tetherin factors, indicating a strong selective pressure to counteract tetherin restriction. The identification of an activity against human tetherin in SIVgsn Vpu suggests that the presence of Vpu in the ancestral SIVmus/mon/gsn virus believed to have contributed the 3' half of the HIV-1 genome may have played a role in the evolution of viruses that could counteract human tetherin and infect humans. BioMed Central 2010-02-18 /pmc/articles/PMC2831821/ /pubmed/20167081 http://dx.doi.org/10.1186/1742-4690-7-13 Text en Copyright ©2010 Yang et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Yang, Su Jung
Lopez, Lisa A
Hauser, Heiko
Exline, Colin M
Haworth, Kevin G
Cannon, Paula M
Anti-tetherin activities in Vpu-expressing primate lentiviruses
title Anti-tetherin activities in Vpu-expressing primate lentiviruses
title_full Anti-tetherin activities in Vpu-expressing primate lentiviruses
title_fullStr Anti-tetherin activities in Vpu-expressing primate lentiviruses
title_full_unstemmed Anti-tetherin activities in Vpu-expressing primate lentiviruses
title_short Anti-tetherin activities in Vpu-expressing primate lentiviruses
title_sort anti-tetherin activities in vpu-expressing primate lentiviruses
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2831821/
https://www.ncbi.nlm.nih.gov/pubmed/20167081
http://dx.doi.org/10.1186/1742-4690-7-13
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