HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3

BACKGROUND: HIV-1 Vif promotes the degradation of host anti-retroviral factor family, APOBEC3 proteins via the recruitment of a multi-subunit E3 ubiquitin ligase complex. The complex is composed of a scaffold protein, Cullin 5 (Cul5), RING-box protein (Rbx), a SOCS box binding protein complex, Elong...

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Autores principales: Evans, Sean L, Schön, Arne, Gao, Qimeng, Han, Xue, Zhou, Xiaohong, Freire, Ernesto, Yu, Xiao-Fang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3937519/
https://www.ncbi.nlm.nih.gov/pubmed/24422669
http://dx.doi.org/10.1186/1742-4690-11-4
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author Evans, Sean L
Schön, Arne
Gao, Qimeng
Han, Xue
Zhou, Xiaohong
Freire, Ernesto
Yu, Xiao-Fang
author_facet Evans, Sean L
Schön, Arne
Gao, Qimeng
Han, Xue
Zhou, Xiaohong
Freire, Ernesto
Yu, Xiao-Fang
author_sort Evans, Sean L
collection PubMed
description BACKGROUND: HIV-1 Vif promotes the degradation of host anti-retroviral factor family, APOBEC3 proteins via the recruitment of a multi-subunit E3 ubiquitin ligase complex. The complex is composed of a scaffold protein, Cullin 5 (Cul5), RING-box protein (Rbx), a SOCS box binding protein complex, Elongins B/C (Elo B/C), as well as newly identified host co-factor, core binding factor beta (CBF-β). Cul5 has previously been shown to bind amino acids within an HCCH domain as well as a PPLP motif at the C–terminus of Vif; however, it is unclear whether Cul5 binding requires additional regions of the Vif polypeptide. RESULTS: Here, we provide evidence that an amino terminal region of full length Vif is necessary for the Vif-Cul5 interaction. Single alanine replacement of select amino acids spanning residues 25–30 ((25)VXHXMY(30)) reduced the ability for Vif to bind Cul5, but not CBF-β or Elo B/C in pull-down experiments. In addition, recombinant Vif mutants had a reduced binding affinity for Cul5 compared to wild-type as measured by isothermal titration calorimetry. N-terminal mutants that demonstrated reduced Cul5 binding were also unable to degrade APOBEC3G as well as APOBEC3F and were unable to restore HIV infectivity, in the presence of APOBEC3G. Although the Vif N-terminal amino acids were necessary for Cul5 interaction, the mutation of each residue to alanine induced a change in the secondary structure of the Vif-CBF-β-Elo B/C complex as suggested by results from circular dichroism spectroscopy and size-exclusion chromatography experiments. Surprisingly, the replacement of His108 to alanine also contributed to the Vif structure. Thus, it is unclear whether the amino acids contribute to a direct interaction with Cul5 or whether the amino acids are responsible for the structural organization of the Vif protein that promotes Cul5 binding. CONCLUSIONS: Taken together, we propose a novel Vif N-terminal motif that is responsible for Vif recruitment of Cul5. Motifs in Vif that are absent from cellular proteins represent attractive targets for future HIV pharmaceutical design.
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spelling pubmed-39375192014-03-01 HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3 Evans, Sean L Schön, Arne Gao, Qimeng Han, Xue Zhou, Xiaohong Freire, Ernesto Yu, Xiao-Fang Retrovirology Research BACKGROUND: HIV-1 Vif promotes the degradation of host anti-retroviral factor family, APOBEC3 proteins via the recruitment of a multi-subunit E3 ubiquitin ligase complex. The complex is composed of a scaffold protein, Cullin 5 (Cul5), RING-box protein (Rbx), a SOCS box binding protein complex, Elongins B/C (Elo B/C), as well as newly identified host co-factor, core binding factor beta (CBF-β). Cul5 has previously been shown to bind amino acids within an HCCH domain as well as a PPLP motif at the C–terminus of Vif; however, it is unclear whether Cul5 binding requires additional regions of the Vif polypeptide. RESULTS: Here, we provide evidence that an amino terminal region of full length Vif is necessary for the Vif-Cul5 interaction. Single alanine replacement of select amino acids spanning residues 25–30 ((25)VXHXMY(30)) reduced the ability for Vif to bind Cul5, but not CBF-β or Elo B/C in pull-down experiments. In addition, recombinant Vif mutants had a reduced binding affinity for Cul5 compared to wild-type as measured by isothermal titration calorimetry. N-terminal mutants that demonstrated reduced Cul5 binding were also unable to degrade APOBEC3G as well as APOBEC3F and were unable to restore HIV infectivity, in the presence of APOBEC3G. Although the Vif N-terminal amino acids were necessary for Cul5 interaction, the mutation of each residue to alanine induced a change in the secondary structure of the Vif-CBF-β-Elo B/C complex as suggested by results from circular dichroism spectroscopy and size-exclusion chromatography experiments. Surprisingly, the replacement of His108 to alanine also contributed to the Vif structure. Thus, it is unclear whether the amino acids contribute to a direct interaction with Cul5 or whether the amino acids are responsible for the structural organization of the Vif protein that promotes Cul5 binding. CONCLUSIONS: Taken together, we propose a novel Vif N-terminal motif that is responsible for Vif recruitment of Cul5. Motifs in Vif that are absent from cellular proteins represent attractive targets for future HIV pharmaceutical design. BioMed Central 2014-01-14 /pmc/articles/PMC3937519/ /pubmed/24422669 http://dx.doi.org/10.1186/1742-4690-11-4 Text en Copyright © 2014 Evans 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
Evans, Sean L
Schön, Arne
Gao, Qimeng
Han, Xue
Zhou, Xiaohong
Freire, Ernesto
Yu, Xiao-Fang
HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title_full HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title_fullStr HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title_full_unstemmed HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title_short HIV-1 Vif N-terminal Motif is required for recruitment of Cul5 to Suppress APOBEC3
title_sort hiv-1 vif n-terminal motif is required for recruitment of cul5 to suppress apobec3
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3937519/
https://www.ncbi.nlm.nih.gov/pubmed/24422669
http://dx.doi.org/10.1186/1742-4690-11-4
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