Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)

Respiratory syncytial virus (RSV) is a major cause of respiratory tract infection in infants and young children worldwide, but currently no safe and effective vaccine is available. The RSV G glycoprotein (RSVG), a major attachment protein, is an important target for the induction of protective immun...

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Autores principales: Cheon, In Su, Shim, Byoung-Shik, Park, Sung-Moo, Choi, Youngjoo, Jang, Ji Eun, Jung, Dae Im, Kim, Jae-Ouk, Chang, Jun, Yun, Cheol-Heui, Song, Man Ki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3988050/
https://www.ncbi.nlm.nih.gov/pubmed/24736750
http://dx.doi.org/10.1371/journal.pone.0094269
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author Cheon, In Su
Shim, Byoung-Shik
Park, Sung-Moo
Choi, Youngjoo
Jang, Ji Eun
Jung, Dae Im
Kim, Jae-Ouk
Chang, Jun
Yun, Cheol-Heui
Song, Man Ki
author_facet Cheon, In Su
Shim, Byoung-Shik
Park, Sung-Moo
Choi, Youngjoo
Jang, Ji Eun
Jung, Dae Im
Kim, Jae-Ouk
Chang, Jun
Yun, Cheol-Heui
Song, Man Ki
author_sort Cheon, In Su
collection PubMed
description Respiratory syncytial virus (RSV) is a major cause of respiratory tract infection in infants and young children worldwide, but currently no safe and effective vaccine is available. The RSV G glycoprotein (RSVG), a major attachment protein, is an important target for the induction of protective immune responses during RSV infection. However, it has been thought that a CD4(+) T cell epitope (a.a. 183–195) within RSVG is associated with pathogenic pulmonary eosinophilia. To develop safe and effective RSV vaccine using RSV G protein core fragment (Gcf), several Gcf variants resulting from modification to CD4(+) T cell epitope were constructed. Mice were immunized with each variant Gcf, and the levels of RSV-specific serum IgG were measured. At day 4 post-challenge with RSV subtype A or B, lung viral titers and pulmonary eosinophilia were determined and changes in body weight were monitored. With wild type Gcf derived from RSV A2 (wtAGcf), although RSV A subtype-specific immune responses were induced, vaccine-enhanced disease characterized by excessive pulmonary eosinophil recruitment and body weight loss were evident, whereas wtGcf from RSV B1 (wtBGcf) induced RSV B subtype-specific immune responses without the signs of vaccine-enhanced disease. Mice immunized with Th-mGcf, a fusion protein consisting CD4(+) T cell epitope from RSV F (F(51–66)) conjugated to mGcf that contains alanine substitutions at a.a. position 185 and 188, showed higher levels of RSV-specific IgG response than mice immunized with mGcf. Both wtAGcf and Th-mGcf provided complete protection against RSV A2 and partial protection against RSV B. Importantly, mice immunized with Th-mGcf did not develop vaccine-enhanced disease following RSV challenge. Immunization of Th-mGcf provided protection against RSV infection without the symptom of vaccine-enhanced disease. Our study provides a novel strategy to develop a safe and effective mucosal RSV vaccine by manipulating the CD4(+) T cell epitope within RSV G protein.
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spelling pubmed-39880502014-04-21 Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf) Cheon, In Su Shim, Byoung-Shik Park, Sung-Moo Choi, Youngjoo Jang, Ji Eun Jung, Dae Im Kim, Jae-Ouk Chang, Jun Yun, Cheol-Heui Song, Man Ki PLoS One Research Article Respiratory syncytial virus (RSV) is a major cause of respiratory tract infection in infants and young children worldwide, but currently no safe and effective vaccine is available. The RSV G glycoprotein (RSVG), a major attachment protein, is an important target for the induction of protective immune responses during RSV infection. However, it has been thought that a CD4(+) T cell epitope (a.a. 183–195) within RSVG is associated with pathogenic pulmonary eosinophilia. To develop safe and effective RSV vaccine using RSV G protein core fragment (Gcf), several Gcf variants resulting from modification to CD4(+) T cell epitope were constructed. Mice were immunized with each variant Gcf, and the levels of RSV-specific serum IgG were measured. At day 4 post-challenge with RSV subtype A or B, lung viral titers and pulmonary eosinophilia were determined and changes in body weight were monitored. With wild type Gcf derived from RSV A2 (wtAGcf), although RSV A subtype-specific immune responses were induced, vaccine-enhanced disease characterized by excessive pulmonary eosinophil recruitment and body weight loss were evident, whereas wtGcf from RSV B1 (wtBGcf) induced RSV B subtype-specific immune responses without the signs of vaccine-enhanced disease. Mice immunized with Th-mGcf, a fusion protein consisting CD4(+) T cell epitope from RSV F (F(51–66)) conjugated to mGcf that contains alanine substitutions at a.a. position 185 and 188, showed higher levels of RSV-specific IgG response than mice immunized with mGcf. Both wtAGcf and Th-mGcf provided complete protection against RSV A2 and partial protection against RSV B. Importantly, mice immunized with Th-mGcf did not develop vaccine-enhanced disease following RSV challenge. Immunization of Th-mGcf provided protection against RSV infection without the symptom of vaccine-enhanced disease. Our study provides a novel strategy to develop a safe and effective mucosal RSV vaccine by manipulating the CD4(+) T cell epitope within RSV G protein. Public Library of Science 2014-04-15 /pmc/articles/PMC3988050/ /pubmed/24736750 http://dx.doi.org/10.1371/journal.pone.0094269 Text en © 2014 Cheon et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Cheon, In Su
Shim, Byoung-Shik
Park, Sung-Moo
Choi, Youngjoo
Jang, Ji Eun
Jung, Dae Im
Kim, Jae-Ouk
Chang, Jun
Yun, Cheol-Heui
Song, Man Ki
Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title_full Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title_fullStr Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title_full_unstemmed Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title_short Development of Safe and Effective RSV Vaccine by Modified CD4 Epitope in G Protein Core Fragment (Gcf)
title_sort development of safe and effective rsv vaccine by modified cd4 epitope in g protein core fragment (gcf)
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3988050/
https://www.ncbi.nlm.nih.gov/pubmed/24736750
http://dx.doi.org/10.1371/journal.pone.0094269
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