Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.

Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.

Most simian immunodeficiency viruses use Nef to counteract the tetherin proteins of their nonhuman primate hosts. Nef also downmodulates cell-surface CD4 and MHC class I (MHC I) molecules and enhances viral infectivity by counteracting SERINC5. We previously demonstrated that tetherin antagonism by...

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Main Authors: Aidin Tavakoli-Tameh, Sanath Kumar Janaka, Katie Zarbock, Shelby O'Connor, Kristin Crosno, Saverio Capuano, Hajime Uno, Jeffrey D Lifson, David T Evans
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-04-01
Series:PLoS Pathogens
Online Access:https://doi.org/10.1371/journal.ppat.1008487
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spelling doaj-b7803c4943094999a6d7b123419810b72021-05-15T04:31:07ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742020-04-01164e100848710.1371/journal.ppat.1008487Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.Aidin Tavakoli-TamehSanath Kumar JanakaKatie ZarbockShelby O'ConnorKristin CrosnoSaverio CapuanoHajime UnoJeffrey D LifsonDavid T EvansMost simian immunodeficiency viruses use Nef to counteract the tetherin proteins of their nonhuman primate hosts. Nef also downmodulates cell-surface CD4 and MHC class I (MHC I) molecules and enhances viral infectivity by counteracting SERINC5. We previously demonstrated that tetherin antagonism by SIV Nef is genetically separable from CD4- and MHC I-downmodulation. Here we show that disruption of tetherin antagonism by Nef impairs virus replication during acute SIV infection of rhesus macaques. A combination of mutations was introduced into the SIVmac239 genome resulting in three amino acid substitutions in Nef that impair tetherin antagonism, but not CD3-, CD4- or MHC I-downmodulation. Further characterization of this mutant (SIVmac239AAA) revealed that these changes also result in partial sensitivity to SERINC5. Separate groups of four rhesus macaques were infected with either wild-type SIVmac239 or SIVmac239AAA, and viral RNA loads in plasma and sequence changes in the viral genome were monitored. Viral loads were significantly lower during acute infection in animals infected with SIVmac239AAA than in animals infected with wild-type SIVmac239. Sequence analysis of the virus population in plasma confirmed that the substitutions in Nef were retained during acute infection; however, changes were observed by week 24 post-infection that fully restored anti-tetherin activity and partially restored anti-SERINC5 activity. These observations reveal overlap in the residues of SIV Nef required for counteracting tetherin and SERINC5 and selective pressure to overcome these restriction factors in vivo.https://doi.org/10.1371/journal.ppat.1008487
collection DOAJ
language English
format Article
sources DOAJ
author Aidin Tavakoli-Tameh
Sanath Kumar Janaka
Katie Zarbock
Shelby O'Connor
Kristin Crosno
Saverio Capuano
Hajime Uno
Jeffrey D Lifson
David T Evans
spellingShingle Aidin Tavakoli-Tameh
Sanath Kumar Janaka
Katie Zarbock
Shelby O'Connor
Kristin Crosno
Saverio Capuano
Hajime Uno
Jeffrey D Lifson
David T Evans
Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
PLoS Pathogens
author_facet Aidin Tavakoli-Tameh
Sanath Kumar Janaka
Katie Zarbock
Shelby O'Connor
Kristin Crosno
Saverio Capuano
Hajime Uno
Jeffrey D Lifson
David T Evans
author_sort Aidin Tavakoli-Tameh
title Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
title_short Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
title_full Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
title_fullStr Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
title_full_unstemmed Loss of tetherin antagonism by Nef impairs SIV replication during acute infection of rhesus macaques.
title_sort loss of tetherin antagonism by nef impairs siv replication during acute infection of rhesus macaques.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2020-04-01
description Most simian immunodeficiency viruses use Nef to counteract the tetherin proteins of their nonhuman primate hosts. Nef also downmodulates cell-surface CD4 and MHC class I (MHC I) molecules and enhances viral infectivity by counteracting SERINC5. We previously demonstrated that tetherin antagonism by SIV Nef is genetically separable from CD4- and MHC I-downmodulation. Here we show that disruption of tetherin antagonism by Nef impairs virus replication during acute SIV infection of rhesus macaques. A combination of mutations was introduced into the SIVmac239 genome resulting in three amino acid substitutions in Nef that impair tetherin antagonism, but not CD3-, CD4- or MHC I-downmodulation. Further characterization of this mutant (SIVmac239AAA) revealed that these changes also result in partial sensitivity to SERINC5. Separate groups of four rhesus macaques were infected with either wild-type SIVmac239 or SIVmac239AAA, and viral RNA loads in plasma and sequence changes in the viral genome were monitored. Viral loads were significantly lower during acute infection in animals infected with SIVmac239AAA than in animals infected with wild-type SIVmac239. Sequence analysis of the virus population in plasma confirmed that the substitutions in Nef were retained during acute infection; however, changes were observed by week 24 post-infection that fully restored anti-tetherin activity and partially restored anti-SERINC5 activity. These observations reveal overlap in the residues of SIV Nef required for counteracting tetherin and SERINC5 and selective pressure to overcome these restriction factors in vivo.
url https://doi.org/10.1371/journal.ppat.1008487
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