Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms

BACKGROUND: A nef gene is present in all primate lentiviral genomes and is important for high viral loads and progression to AIDS in human or experimental macaque hosts of HIV or SIV, respectively. In these hosts, infection of the thymus results in a decreased output of naive T cells that may contri...

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Autores principales: Van Nuffel, Anouk, Ariën, Kevin K, Stove, Veronique, Schindler, Michael, O’Neill, Eduardo, Schmökel, Jan, Van de Walle, Inge, Naessens, Evelien, Vanderstraeten, Hanne, Van Landeghem, Kathleen, Taghon, Tom, Pulkkinen, Kati, Saksela, Kalle, Garcia, J Victor, Fackler, Oliver T, Kirchhoff, Frank, Verhasselt, Bruno
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3906981/
https://www.ncbi.nlm.nih.gov/pubmed/24237970
http://dx.doi.org/10.1186/1742-4690-10-137
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author Van Nuffel, Anouk
Ariën, Kevin K
Stove, Veronique
Schindler, Michael
O’Neill, Eduardo
Schmökel, Jan
Van de Walle, Inge
Naessens, Evelien
Vanderstraeten, Hanne
Van Landeghem, Kathleen
Taghon, Tom
Pulkkinen, Kati
Saksela, Kalle
Garcia, J Victor
Fackler, Oliver T
Kirchhoff, Frank
Verhasselt, Bruno
author_facet Van Nuffel, Anouk
Ariën, Kevin K
Stove, Veronique
Schindler, Michael
O’Neill, Eduardo
Schmökel, Jan
Van de Walle, Inge
Naessens, Evelien
Vanderstraeten, Hanne
Van Landeghem, Kathleen
Taghon, Tom
Pulkkinen, Kati
Saksela, Kalle
Garcia, J Victor
Fackler, Oliver T
Kirchhoff, Frank
Verhasselt, Bruno
author_sort Van Nuffel, Anouk
collection PubMed
description BACKGROUND: A nef gene is present in all primate lentiviral genomes and is important for high viral loads and progression to AIDS in human or experimental macaque hosts of HIV or SIV, respectively. In these hosts, infection of the thymus results in a decreased output of naive T cells that may contribute to the development of immunodeficiency. We have previously shown that HIV-1 subtype B Nef proteins can block human T-cell development. However, the underlying mechanism(s) and the conservation of this Nef function between different groups of HIV and SIV remained to be determined. RESULTS: We investigated whether reduction of thymic output is a conserved function of highly divergent lentiviral Nef proteins including those from both types of human immunodeficiency viruses (HIV-1 and HIV-2), their direct simian counterparts (SIVcpz, SIVgor and SIVsmm, respectively), and some additional SIV strains. We found that expression of most of these nef alleles in thymocyte progenitors impaired T-cell development and reduced thymic output. For HIV-1 Nef, binding to active p21 protein (Cdc42/Rac)-activated kinase (PAK2) was a major determinant of this function. In contrast, selective disruption of PAK2 binding did not eliminate the effect on T-cell development of SIVmac239 Nef, as was shown by expressing mutants in a newly discovered PAK2 activating structural motif (PASM) constituted by residues I117, H121, T218 and Y221, as well as previously described mutants. Rather, down-modulation of cell surface CD3 was sufficient for reduced thymic output by SIVmac Nef, while other functions of SIV Nefs contributed. CONCLUSIONS: Our results indicate that primate lentiviral Nef proteins impair development of thymocyte precursors into T cells in multiple ways. The interaction of HIV-1 Nef with active PAK2 by HIV-1 seem to be most detrimental, and downregulation of CD3 by HIV-2 and most SIV Nef proteins sufficient for reduced thymic output. Since the reduction of thymic output by Nef is a conserved property of divergent lentiviruses, it is likely to be relevant for peripheral T-cell depletion in poorly adapted primate lentiviral infections.
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spelling pubmed-39069812014-01-31 Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms Van Nuffel, Anouk Ariën, Kevin K Stove, Veronique Schindler, Michael O’Neill, Eduardo Schmökel, Jan Van de Walle, Inge Naessens, Evelien Vanderstraeten, Hanne Van Landeghem, Kathleen Taghon, Tom Pulkkinen, Kati Saksela, Kalle Garcia, J Victor Fackler, Oliver T Kirchhoff, Frank Verhasselt, Bruno Retrovirology Research BACKGROUND: A nef gene is present in all primate lentiviral genomes and is important for high viral loads and progression to AIDS in human or experimental macaque hosts of HIV or SIV, respectively. In these hosts, infection of the thymus results in a decreased output of naive T cells that may contribute to the development of immunodeficiency. We have previously shown that HIV-1 subtype B Nef proteins can block human T-cell development. However, the underlying mechanism(s) and the conservation of this Nef function between different groups of HIV and SIV remained to be determined. RESULTS: We investigated whether reduction of thymic output is a conserved function of highly divergent lentiviral Nef proteins including those from both types of human immunodeficiency viruses (HIV-1 and HIV-2), their direct simian counterparts (SIVcpz, SIVgor and SIVsmm, respectively), and some additional SIV strains. We found that expression of most of these nef alleles in thymocyte progenitors impaired T-cell development and reduced thymic output. For HIV-1 Nef, binding to active p21 protein (Cdc42/Rac)-activated kinase (PAK2) was a major determinant of this function. In contrast, selective disruption of PAK2 binding did not eliminate the effect on T-cell development of SIVmac239 Nef, as was shown by expressing mutants in a newly discovered PAK2 activating structural motif (PASM) constituted by residues I117, H121, T218 and Y221, as well as previously described mutants. Rather, down-modulation of cell surface CD3 was sufficient for reduced thymic output by SIVmac Nef, while other functions of SIV Nefs contributed. CONCLUSIONS: Our results indicate that primate lentiviral Nef proteins impair development of thymocyte precursors into T cells in multiple ways. The interaction of HIV-1 Nef with active PAK2 by HIV-1 seem to be most detrimental, and downregulation of CD3 by HIV-2 and most SIV Nef proteins sufficient for reduced thymic output. Since the reduction of thymic output by Nef is a conserved property of divergent lentiviruses, it is likely to be relevant for peripheral T-cell depletion in poorly adapted primate lentiviral infections. BioMed Central 2013-11-15 /pmc/articles/PMC3906981/ /pubmed/24237970 http://dx.doi.org/10.1186/1742-4690-10-137 Text en Copyright © 2013 Van Nuffel 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
Van Nuffel, Anouk
Ariën, Kevin K
Stove, Veronique
Schindler, Michael
O’Neill, Eduardo
Schmökel, Jan
Van de Walle, Inge
Naessens, Evelien
Vanderstraeten, Hanne
Van Landeghem, Kathleen
Taghon, Tom
Pulkkinen, Kati
Saksela, Kalle
Garcia, J Victor
Fackler, Oliver T
Kirchhoff, Frank
Verhasselt, Bruno
Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title_full Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title_fullStr Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title_full_unstemmed Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title_short Primate lentiviral Nef proteins deregulate T-cell development by multiple mechanisms
title_sort primate lentiviral nef proteins deregulate t-cell development by multiple mechanisms
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3906981/
https://www.ncbi.nlm.nih.gov/pubmed/24237970
http://dx.doi.org/10.1186/1742-4690-10-137
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