N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.

The N-linked glycosylation motif at amino acid position 154-156 of the envelope (E) protein of West Nile virus (WNV) is linked to enhanced murine neuroinvasiveness, avian pathogenicity and vector competence. Naturally occurring isolates with altered E protein glycosylation patterns have been observe...

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Main Authors: Payal D Maharaj, Stanley A Langevin, Bethany G Bolling, Christy C Andrade, Xavier A Engle, Wanichaya N Ramey, Angela Bosco-Lauth, Richard A Bowen, Todd A Sanders, Claire Y-H Huang, William K Reisen, Aaron C Brault
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-07-01
Series:PLoS Neglected Tropical Diseases
Online Access:https://doi.org/10.1371/journal.pntd.0007473
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spelling doaj-c074d38fd0b049d9a322a42893c3e9d02021-04-21T23:54:07ZengPublic Library of Science (PLoS)PLoS Neglected Tropical Diseases1935-27271935-27352019-07-01137e000747310.1371/journal.pntd.0007473N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.Payal D MaharajStanley A LangevinBethany G BollingChristy C AndradeXavier A EngleWanichaya N RameyAngela Bosco-LauthRichard A BowenTodd A SandersClaire Y-H HuangWilliam K ReisenAaron C BraultThe N-linked glycosylation motif at amino acid position 154-156 of the envelope (E) protein of West Nile virus (WNV) is linked to enhanced murine neuroinvasiveness, avian pathogenicity and vector competence. Naturally occurring isolates with altered E protein glycosylation patterns have been observed in WNV isolates; however, the specific effects of these polymorphisms on avian host pathogenesis and vector competence have not been investigated before. In the present study, amino acid polymorphisms, NYT, NYP, NYF, SYP, SYS, KYS and deletion (A'DEL), were reverse engineered into a parental WNV (NYS) cDNA infectious clone to generate WNV glycosylation mutant viruses. These WNV glycosylation mutant viruses were characterized for in vitro growth, pH-sensitivity, temperature-sensitivity and host competence in American crows (AMCR), house sparrows (HOSP) and Culex quinquefasciatus. The NYS and NYT glycosylated viruses showed higher viral replication, and lower pH and temperature sensitivity than NYP, NYF, SYP, SYS, KYS and A'DEL viruses in vitro. Interestingly, in vivo results demonstrated asymmetric effects in avian and mosquito competence that were independent of the E-protein glycosylation status. In AMCRs and HOSPs, all viruses showed comparable viremias with the exception of NYP and KYS viruses that showed attenuated phenotypes. Only NYP showed reduced vector competence in both Cx. quinquefasciatus and Cx. tarsalis. Glycosylated NYT exhibited similar avian virulence properties as NYS, but resulted in higher mosquito oral infectivity than glycosylated NYS and nonglycosylated, NYP, NYF, SYP and KYS mutants. These data demonstrated that amino acid polymorphisms at E154/156 dictate differential avian host and vector competence phenotypes independent of E-protein glycosylation status.https://doi.org/10.1371/journal.pntd.0007473
collection DOAJ
language English
format Article
sources DOAJ
author Payal D Maharaj
Stanley A Langevin
Bethany G Bolling
Christy C Andrade
Xavier A Engle
Wanichaya N Ramey
Angela Bosco-Lauth
Richard A Bowen
Todd A Sanders
Claire Y-H Huang
William K Reisen
Aaron C Brault
spellingShingle Payal D Maharaj
Stanley A Langevin
Bethany G Bolling
Christy C Andrade
Xavier A Engle
Wanichaya N Ramey
Angela Bosco-Lauth
Richard A Bowen
Todd A Sanders
Claire Y-H Huang
William K Reisen
Aaron C Brault
N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
PLoS Neglected Tropical Diseases
author_facet Payal D Maharaj
Stanley A Langevin
Bethany G Bolling
Christy C Andrade
Xavier A Engle
Wanichaya N Ramey
Angela Bosco-Lauth
Richard A Bowen
Todd A Sanders
Claire Y-H Huang
William K Reisen
Aaron C Brault
author_sort Payal D Maharaj
title N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
title_short N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
title_full N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
title_fullStr N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
title_full_unstemmed N-linked glycosylation of the West Nile virus envelope protein is not a requisite for avian virulence or vector competence.
title_sort n-linked glycosylation of the west nile virus envelope protein is not a requisite for avian virulence or vector competence.
publisher Public Library of Science (PLoS)
series PLoS Neglected Tropical Diseases
issn 1935-2727
1935-2735
publishDate 2019-07-01
description The N-linked glycosylation motif at amino acid position 154-156 of the envelope (E) protein of West Nile virus (WNV) is linked to enhanced murine neuroinvasiveness, avian pathogenicity and vector competence. Naturally occurring isolates with altered E protein glycosylation patterns have been observed in WNV isolates; however, the specific effects of these polymorphisms on avian host pathogenesis and vector competence have not been investigated before. In the present study, amino acid polymorphisms, NYT, NYP, NYF, SYP, SYS, KYS and deletion (A'DEL), were reverse engineered into a parental WNV (NYS) cDNA infectious clone to generate WNV glycosylation mutant viruses. These WNV glycosylation mutant viruses were characterized for in vitro growth, pH-sensitivity, temperature-sensitivity and host competence in American crows (AMCR), house sparrows (HOSP) and Culex quinquefasciatus. The NYS and NYT glycosylated viruses showed higher viral replication, and lower pH and temperature sensitivity than NYP, NYF, SYP, SYS, KYS and A'DEL viruses in vitro. Interestingly, in vivo results demonstrated asymmetric effects in avian and mosquito competence that were independent of the E-protein glycosylation status. In AMCRs and HOSPs, all viruses showed comparable viremias with the exception of NYP and KYS viruses that showed attenuated phenotypes. Only NYP showed reduced vector competence in both Cx. quinquefasciatus and Cx. tarsalis. Glycosylated NYT exhibited similar avian virulence properties as NYS, but resulted in higher mosquito oral infectivity than glycosylated NYS and nonglycosylated, NYP, NYF, SYP and KYS mutants. These data demonstrated that amino acid polymorphisms at E154/156 dictate differential avian host and vector competence phenotypes independent of E-protein glycosylation status.
url https://doi.org/10.1371/journal.pntd.0007473
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