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Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein

Chikungunya virus (CHIKV) and related arboviruses have been responsible for large epidemic outbreaks with serious economic and social impact. The immune mechanisms, which control viral multiplication and dissemination, are not yet known. Here, we studied the antibody response against the CHIKV surfa...

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Autores principales: Kam, Yiu-Wing, Lum, Fok-Moon, Teo, Teck-Hui, Lee, Wendy W L, Simarmata, Diane, Harjanto, Sumitro, Chua, Chong-Long, Chan, Yoke-Fun, Wee, Jin-Kiat, Chow, Angela, Lin, Raymond T P, Leo, Yee-Sin, Le Grand, Roger, Sam, I-Ching, Tong, Joo-Chuan, Roques, Pierre, Wiesmüller, Karl-Heinz, Rénia, Laurent, Rötzschke, Olaf, Ng, Lisa F P
Formato: Online Artículo Texto
Lenguaje:English
Publicado: WILEY-VCH Verlag 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3376860/
https://www.ncbi.nlm.nih.gov/pubmed/22389221
http://dx.doi.org/10.1002/emmm.201200213
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author Kam, Yiu-Wing
Lum, Fok-Moon
Teo, Teck-Hui
Lee, Wendy W L
Simarmata, Diane
Harjanto, Sumitro
Chua, Chong-Long
Chan, Yoke-Fun
Wee, Jin-Kiat
Chow, Angela
Lin, Raymond T P
Leo, Yee-Sin
Le Grand, Roger
Sam, I-Ching
Tong, Joo-Chuan
Roques, Pierre
Wiesmüller, Karl-Heinz
Rénia, Laurent
Rötzschke, Olaf
Ng, Lisa F P
author_facet Kam, Yiu-Wing
Lum, Fok-Moon
Teo, Teck-Hui
Lee, Wendy W L
Simarmata, Diane
Harjanto, Sumitro
Chua, Chong-Long
Chan, Yoke-Fun
Wee, Jin-Kiat
Chow, Angela
Lin, Raymond T P
Leo, Yee-Sin
Le Grand, Roger
Sam, I-Ching
Tong, Joo-Chuan
Roques, Pierre
Wiesmüller, Karl-Heinz
Rénia, Laurent
Rötzschke, Olaf
Ng, Lisa F P
author_sort Kam, Yiu-Wing
collection PubMed
description Chikungunya virus (CHIKV) and related arboviruses have been responsible for large epidemic outbreaks with serious economic and social impact. The immune mechanisms, which control viral multiplication and dissemination, are not yet known. Here, we studied the antibody response against the CHIKV surface antigens in infected patients. With plasma samples obtained during the early convalescent phase, we showed that the naturally-acquired IgG response is dominated by IgG3 antibodies specific mostly for a single linear epitope ‘E2EP3’. E2EP3 is located at the N-terminus of the E2 glycoprotein and prominently exposed on the viral envelope. E2EP3-specific antibodies are neutralizing and their removal from the plasma reduced the CHIKV-specific antibody titer by up to 80%. Screening of E2EP3 across different patient cohorts and in non-human primates demonstrated the value of this epitope as a good serology detection marker for CHIKV infection already at an early stage. Mice vaccinated by E2EP3 peptides were protected against CHIKV with reduced viremia and joint inflammation, providing a pre-clinical basis for the design of effective vaccine against arthralgia-inducing CHIKV and other alphaviruses.
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spelling pubmed-33768602012-09-17 Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein Kam, Yiu-Wing Lum, Fok-Moon Teo, Teck-Hui Lee, Wendy W L Simarmata, Diane Harjanto, Sumitro Chua, Chong-Long Chan, Yoke-Fun Wee, Jin-Kiat Chow, Angela Lin, Raymond T P Leo, Yee-Sin Le Grand, Roger Sam, I-Ching Tong, Joo-Chuan Roques, Pierre Wiesmüller, Karl-Heinz Rénia, Laurent Rötzschke, Olaf Ng, Lisa F P EMBO Mol Med Research Article Chikungunya virus (CHIKV) and related arboviruses have been responsible for large epidemic outbreaks with serious economic and social impact. The immune mechanisms, which control viral multiplication and dissemination, are not yet known. Here, we studied the antibody response against the CHIKV surface antigens in infected patients. With plasma samples obtained during the early convalescent phase, we showed that the naturally-acquired IgG response is dominated by IgG3 antibodies specific mostly for a single linear epitope ‘E2EP3’. E2EP3 is located at the N-terminus of the E2 glycoprotein and prominently exposed on the viral envelope. E2EP3-specific antibodies are neutralizing and their removal from the plasma reduced the CHIKV-specific antibody titer by up to 80%. Screening of E2EP3 across different patient cohorts and in non-human primates demonstrated the value of this epitope as a good serology detection marker for CHIKV infection already at an early stage. Mice vaccinated by E2EP3 peptides were protected against CHIKV with reduced viremia and joint inflammation, providing a pre-clinical basis for the design of effective vaccine against arthralgia-inducing CHIKV and other alphaviruses. WILEY-VCH Verlag 2012-04 /pmc/articles/PMC3376860/ /pubmed/22389221 http://dx.doi.org/10.1002/emmm.201200213 Text en Copyright © 2012 EMBO Molecular Medicine
spellingShingle Research Article
Kam, Yiu-Wing
Lum, Fok-Moon
Teo, Teck-Hui
Lee, Wendy W L
Simarmata, Diane
Harjanto, Sumitro
Chua, Chong-Long
Chan, Yoke-Fun
Wee, Jin-Kiat
Chow, Angela
Lin, Raymond T P
Leo, Yee-Sin
Le Grand, Roger
Sam, I-Ching
Tong, Joo-Chuan
Roques, Pierre
Wiesmüller, Karl-Heinz
Rénia, Laurent
Rötzschke, Olaf
Ng, Lisa F P
Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title_full Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title_fullStr Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title_full_unstemmed Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title_short Early neutralizing IgG response to Chikungunya virus in infected patients targets a dominant linear epitope on the E2 glycoprotein
title_sort early neutralizing igg response to chikungunya virus in infected patients targets a dominant linear epitope on the e2 glycoprotein
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3376860/
https://www.ncbi.nlm.nih.gov/pubmed/22389221
http://dx.doi.org/10.1002/emmm.201200213
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