Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function

BACKGROUND: The Nef protein of HIV facilitates virus replication and disease progression in infected patients. This role as pathogenesis factor depends on several genetically separable Nef functions that are mediated by interactions of highly conserved protein-protein interaction motifs with differe...

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Autores principales: Meuwissen, Pieter J, Stolp, Bettina, Iannucci, Veronica, Vermeire, Jolien, Naessens, Evelien, Saksela, Kalle, Geyer, Matthias, Vanham, Guido, Arien, Kevin K, Fackler, Oliver T, Verhasselt, Bruno
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3476393/
https://www.ncbi.nlm.nih.gov/pubmed/22537596
http://dx.doi.org/10.1186/1742-4690-9-34
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author Meuwissen, Pieter J
Stolp, Bettina
Iannucci, Veronica
Vermeire, Jolien
Naessens, Evelien
Saksela, Kalle
Geyer, Matthias
Vanham, Guido
Arien, Kevin K
Fackler, Oliver T
Verhasselt, Bruno
author_facet Meuwissen, Pieter J
Stolp, Bettina
Iannucci, Veronica
Vermeire, Jolien
Naessens, Evelien
Saksela, Kalle
Geyer, Matthias
Vanham, Guido
Arien, Kevin K
Fackler, Oliver T
Verhasselt, Bruno
author_sort Meuwissen, Pieter J
collection PubMed
description BACKGROUND: The Nef protein of HIV facilitates virus replication and disease progression in infected patients. This role as pathogenesis factor depends on several genetically separable Nef functions that are mediated by interactions of highly conserved protein-protein interaction motifs with different host cell proteins. By studying the functionality of a series of nef alleles from clinical isolates, we identified a dysfunctional HIV group O Nef in which a highly conserved valine-glycine-phenylalanine (VGF) region, which links a preceding acidic cluster with the following proline-rich motif into an amphipathic surface was deleted. In this study, we aimed to study the functional importance of this VGF region. RESULTS: The dysfunctional HIV group O8 nef allele was restored to the consensus sequence, and mutants of canonical (NL4.3, NA-7, SF2) and non-canonical (B2 and C1422) HIV-1 group M nef alleles were generated in which the amino acids of the VGF region were changed into alanines (VGF→AAA) and tested for their capacity to interfere with surface receptor trafficking, signal transduction and enhancement of viral replication and infectivity. We found the VGF motif, and each individual amino acid of this motif, to be critical for downregulation of MHC-I and CXCR4. Moreover, Nef’s association with the cellular p21-activated kinase 2 (PAK2), the resulting deregulation of cofilin and inhibition of host cell actin remodeling, and targeting of Lck kinase to the trans-golgi-network (TGN) were affected as well. Of particular interest, VGF integrity was essential for Nef-mediated enhancement of HIV virion infectivity and HIV replication in peripheral blood lymphocytes. For targeting of Lck kinase to the TGN and viral infectivity, especially the phenylalanine of the triplet was essential. At the molecular level, the VGF motif was required for the physical interaction of the adjacent proline-rich motif with Hck. CONCLUSION: Based on these findings, we propose that this highly conserved three amino acid VGF motif together with the acidic cluster and the proline-rich motif form a previously unrecognized amphipathic surface on Nef. This surface appears to be essential for the majority of Nef functions and thus represents a prime target for the pharmacological inhibition of Nef.
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spelling pubmed-34763932012-10-20 Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function Meuwissen, Pieter J Stolp, Bettina Iannucci, Veronica Vermeire, Jolien Naessens, Evelien Saksela, Kalle Geyer, Matthias Vanham, Guido Arien, Kevin K Fackler, Oliver T Verhasselt, Bruno Retrovirology Research BACKGROUND: The Nef protein of HIV facilitates virus replication and disease progression in infected patients. This role as pathogenesis factor depends on several genetically separable Nef functions that are mediated by interactions of highly conserved protein-protein interaction motifs with different host cell proteins. By studying the functionality of a series of nef alleles from clinical isolates, we identified a dysfunctional HIV group O Nef in which a highly conserved valine-glycine-phenylalanine (VGF) region, which links a preceding acidic cluster with the following proline-rich motif into an amphipathic surface was deleted. In this study, we aimed to study the functional importance of this VGF region. RESULTS: The dysfunctional HIV group O8 nef allele was restored to the consensus sequence, and mutants of canonical (NL4.3, NA-7, SF2) and non-canonical (B2 and C1422) HIV-1 group M nef alleles were generated in which the amino acids of the VGF region were changed into alanines (VGF→AAA) and tested for their capacity to interfere with surface receptor trafficking, signal transduction and enhancement of viral replication and infectivity. We found the VGF motif, and each individual amino acid of this motif, to be critical for downregulation of MHC-I and CXCR4. Moreover, Nef’s association with the cellular p21-activated kinase 2 (PAK2), the resulting deregulation of cofilin and inhibition of host cell actin remodeling, and targeting of Lck kinase to the trans-golgi-network (TGN) were affected as well. Of particular interest, VGF integrity was essential for Nef-mediated enhancement of HIV virion infectivity and HIV replication in peripheral blood lymphocytes. For targeting of Lck kinase to the TGN and viral infectivity, especially the phenylalanine of the triplet was essential. At the molecular level, the VGF motif was required for the physical interaction of the adjacent proline-rich motif with Hck. CONCLUSION: Based on these findings, we propose that this highly conserved three amino acid VGF motif together with the acidic cluster and the proline-rich motif form a previously unrecognized amphipathic surface on Nef. This surface appears to be essential for the majority of Nef functions and thus represents a prime target for the pharmacological inhibition of Nef. BioMed Central 2012-04-27 /pmc/articles/PMC3476393/ /pubmed/22537596 http://dx.doi.org/10.1186/1742-4690-9-34 Text en Copyright ©2012 Meuwissen 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
Meuwissen, Pieter J
Stolp, Bettina
Iannucci, Veronica
Vermeire, Jolien
Naessens, Evelien
Saksela, Kalle
Geyer, Matthias
Vanham, Guido
Arien, Kevin K
Fackler, Oliver T
Verhasselt, Bruno
Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title_full Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title_fullStr Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title_full_unstemmed Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title_short Identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for HIV-1 Nef function
title_sort identification of a highly conserved valine-glycine-phenylalanine amino acid triplet required for hiv-1 nef function
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3476393/
https://www.ncbi.nlm.nih.gov/pubmed/22537596
http://dx.doi.org/10.1186/1742-4690-9-34
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