Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response

BACKGROUND: The study of human B cell response to dengue virus (DENV) infection is critical to understand serotype-specific protection and the cross-reactive sub-neutralizing response. Whereas the first is beneficial and thus represents the ultimate goal of vaccination, the latter has been implicate...

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Autores principales: Godoy-Lozano, Elizabeth Ernestina, Téllez-Sosa, Juan, Sánchez-González, Gilberto, Sámano-Sánchez, Hugo, Aguilar-Salgado, Andrés, Salinas-Rodríguez, Aarón, Cortina-Ceballos, Bernardo, Vivanco-Cid, Héctor, Hernández-Flores, Karina, Pfaff, Jennifer M., Kahle, Kristen M., Doranz, Benjamin J., Gómez-Barreto, Rosa Elena, Valdovinos-Torres, Humberto, López-Martínez, Irma, Rodriguez, Mario H., Martínez-Barnetche, Jesús
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2016
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4766701/
https://www.ncbi.nlm.nih.gov/pubmed/26917418
http://dx.doi.org/10.1186/s13073-016-0276-1
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author Godoy-Lozano, Elizabeth Ernestina
Téllez-Sosa, Juan
Sánchez-González, Gilberto
Sámano-Sánchez, Hugo
Aguilar-Salgado, Andrés
Salinas-Rodríguez, Aarón
Cortina-Ceballos, Bernardo
Vivanco-Cid, Héctor
Hernández-Flores, Karina
Pfaff, Jennifer M.
Kahle, Kristen M.
Doranz, Benjamin J.
Gómez-Barreto, Rosa Elena
Valdovinos-Torres, Humberto
López-Martínez, Irma
Rodriguez, Mario H.
Martínez-Barnetche, Jesús
author_facet Godoy-Lozano, Elizabeth Ernestina
Téllez-Sosa, Juan
Sánchez-González, Gilberto
Sámano-Sánchez, Hugo
Aguilar-Salgado, Andrés
Salinas-Rodríguez, Aarón
Cortina-Ceballos, Bernardo
Vivanco-Cid, Héctor
Hernández-Flores, Karina
Pfaff, Jennifer M.
Kahle, Kristen M.
Doranz, Benjamin J.
Gómez-Barreto, Rosa Elena
Valdovinos-Torres, Humberto
López-Martínez, Irma
Rodriguez, Mario H.
Martínez-Barnetche, Jesús
author_sort Godoy-Lozano, Elizabeth Ernestina
collection PubMed
description BACKGROUND: The study of human B cell response to dengue virus (DENV) infection is critical to understand serotype-specific protection and the cross-reactive sub-neutralizing response. Whereas the first is beneficial and thus represents the ultimate goal of vaccination, the latter has been implicated in the development of severe disease, which occurs in a small, albeit significant, fraction of secondary DENV infections. Both primary and secondary infections are associated with the production of poly-reactive and cross-reactive IgG antibodies. METHODS: To gain insight into the effect of DENV infection on the B cell repertoire, we used VH region high-throughput cDNA sequencing of the peripheral blood IgG B cell compartment of 19 individuals during the acute phase of infection. For 11 individuals, a second sample obtained 6 months later was analyzed for comparison. Probabilities of sequencing antibody secreting cells or memory B cells were estimated using second-order Monte Carlo simulation. RESULTS: We found that in acute disease there is an increase in IgG B cell diversity and changes in the relative use of segments IGHV1-2, IGHV1-18, and IGHV1-69. Somewhat unexpectedly, an overall low proportion of somatic hypermutated antibody genes was observed during the acute phase plasmablasts, particularly in secondary infections and those cases with more severe disease. CONCLUSIONS: Our data are consistent with an innate-like antiviral recognition system mediated by B cells using defined germ-line coded B cell receptors, which could provide a rapid germinal center-independent antibody response during the early phase of infection. A model describing concurrent T-dependent and T-independent B cell responses in the context of DENV infection is proposed, which incorporates the selection of B cells using hypomutated IGHV segments and their potential role in poly/cross-reactivity. Its formal demonstration could lead to a definition of its potential implication in antibody-dependent enhancement, and may contribute to rational vaccine development efforts. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13073-016-0276-1) contains supplementary material, which is available to authorized users.
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spelling pubmed-47667012016-02-26 Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response Godoy-Lozano, Elizabeth Ernestina Téllez-Sosa, Juan Sánchez-González, Gilberto Sámano-Sánchez, Hugo Aguilar-Salgado, Andrés Salinas-Rodríguez, Aarón Cortina-Ceballos, Bernardo Vivanco-Cid, Héctor Hernández-Flores, Karina Pfaff, Jennifer M. Kahle, Kristen M. Doranz, Benjamin J. Gómez-Barreto, Rosa Elena Valdovinos-Torres, Humberto López-Martínez, Irma Rodriguez, Mario H. Martínez-Barnetche, Jesús Genome Med Research BACKGROUND: The study of human B cell response to dengue virus (DENV) infection is critical to understand serotype-specific protection and the cross-reactive sub-neutralizing response. Whereas the first is beneficial and thus represents the ultimate goal of vaccination, the latter has been implicated in the development of severe disease, which occurs in a small, albeit significant, fraction of secondary DENV infections. Both primary and secondary infections are associated with the production of poly-reactive and cross-reactive IgG antibodies. METHODS: To gain insight into the effect of DENV infection on the B cell repertoire, we used VH region high-throughput cDNA sequencing of the peripheral blood IgG B cell compartment of 19 individuals during the acute phase of infection. For 11 individuals, a second sample obtained 6 months later was analyzed for comparison. Probabilities of sequencing antibody secreting cells or memory B cells were estimated using second-order Monte Carlo simulation. RESULTS: We found that in acute disease there is an increase in IgG B cell diversity and changes in the relative use of segments IGHV1-2, IGHV1-18, and IGHV1-69. Somewhat unexpectedly, an overall low proportion of somatic hypermutated antibody genes was observed during the acute phase plasmablasts, particularly in secondary infections and those cases with more severe disease. CONCLUSIONS: Our data are consistent with an innate-like antiviral recognition system mediated by B cells using defined germ-line coded B cell receptors, which could provide a rapid germinal center-independent antibody response during the early phase of infection. A model describing concurrent T-dependent and T-independent B cell responses in the context of DENV infection is proposed, which incorporates the selection of B cells using hypomutated IGHV segments and their potential role in poly/cross-reactivity. Its formal demonstration could lead to a definition of its potential implication in antibody-dependent enhancement, and may contribute to rational vaccine development efforts. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13073-016-0276-1) contains supplementary material, which is available to authorized users. BioMed Central 2016-02-25 /pmc/articles/PMC4766701/ /pubmed/26917418 http://dx.doi.org/10.1186/s13073-016-0276-1 Text en © Godoy-Lozano et al. 2016 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Godoy-Lozano, Elizabeth Ernestina
Téllez-Sosa, Juan
Sánchez-González, Gilberto
Sámano-Sánchez, Hugo
Aguilar-Salgado, Andrés
Salinas-Rodríguez, Aarón
Cortina-Ceballos, Bernardo
Vivanco-Cid, Héctor
Hernández-Flores, Karina
Pfaff, Jennifer M.
Kahle, Kristen M.
Doranz, Benjamin J.
Gómez-Barreto, Rosa Elena
Valdovinos-Torres, Humberto
López-Martínez, Irma
Rodriguez, Mario H.
Martínez-Barnetche, Jesús
Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title_full Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title_fullStr Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title_full_unstemmed Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title_short Lower IgG somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent B cell response
title_sort lower igg somatic hypermutation rates during acute dengue virus infection is compatible with a germinal center-independent b cell response
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4766701/
https://www.ncbi.nlm.nih.gov/pubmed/26917418
http://dx.doi.org/10.1186/s13073-016-0276-1
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