Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold

Emergence of a new influenza strain leads to a rapid global spread of the virus due to minimal antibody immunity. Pre-existing CD8(+) T-cell immunity directed towards conserved internal viral regions can greatly ameliorate the disease. However, mutational escape within the T cell epitopes is a subst...

Descripción completa

Detalles Bibliográficos
Autores principales: Valkenburg, Sophie A., Gras, Stephanie, Guillonneau, Carole, La Gruta, Nicole L., Thomas, Paul G., Purcell, Anthony W., Rossjohn, Jamie, Doherty, Peter C., Turner, Stephen J., Kedzierska, Katherine
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2920842/
https://www.ncbi.nlm.nih.gov/pubmed/20711359
http://dx.doi.org/10.1371/journal.ppat.1001039
_version_ 1782185316686233600
author Valkenburg, Sophie A.
Gras, Stephanie
Guillonneau, Carole
La Gruta, Nicole L.
Thomas, Paul G.
Purcell, Anthony W.
Rossjohn, Jamie
Doherty, Peter C.
Turner, Stephen J.
Kedzierska, Katherine
author_facet Valkenburg, Sophie A.
Gras, Stephanie
Guillonneau, Carole
La Gruta, Nicole L.
Thomas, Paul G.
Purcell, Anthony W.
Rossjohn, Jamie
Doherty, Peter C.
Turner, Stephen J.
Kedzierska, Katherine
author_sort Valkenburg, Sophie A.
collection PubMed
description Emergence of a new influenza strain leads to a rapid global spread of the virus due to minimal antibody immunity. Pre-existing CD8(+) T-cell immunity directed towards conserved internal viral regions can greatly ameliorate the disease. However, mutational escape within the T cell epitopes is a substantial issue for virus control and vaccine design. Although mutations can result in a loss of T cell recognition, some variants generate cross-reactive T cell responses. In this study, we used reverse genetics to modify the influenza NP(336–374) peptide at a partially-solvent exposed residue (N->A, NPN3A mutation) to assess the availability, effectiveness and mechanism underlying influenza-specific cross-reactive T cell responses. The engineered virus induced a diminished CD8(+) T cell response and selected a narrowed T cell receptor (TCR) repertoire within two Vβ regions (Vβ8.3 and Vβ9). This can be partially explained by the H-2D(b)NPN3A structure that showed a loss of several contacts between the NPN3A peptide and H-2D(b), including a contact with His155, a position known to play an important role in mediating TCR-pMHC-I interactions. Despite these differences, common cross-reactive TCRs were detected in both the naïve and immune NPN3A-specific TCR repertoires. However, while the NPN3A epitope primes memory T-cells that give an equivalent recall response to the mutant or wild-type (wt) virus, both are markedly lower than wt->wt challenge. Such decreased CD8(+) responses elicited after heterologous challenge resulted in delayed viral clearance from the infected lung. Furthermore, mice first exposed to the wt virus give a poor, low avidity response following secondary infection with the mutant. Thus, the protective efficacy of cross-reactive CD8(+) T cells recognising mutant viral epitopes depend on peptide-MHC-I structural interactions and functional avidity. Our study does not support vaccine strategies that include immunization against commonly selected cross-reactive variants with mutations at partially-solvent exposed residues that have characteristics comparable to NPN3A.
format Text
id pubmed-2920842
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-29208422010-08-13 Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold Valkenburg, Sophie A. Gras, Stephanie Guillonneau, Carole La Gruta, Nicole L. Thomas, Paul G. Purcell, Anthony W. Rossjohn, Jamie Doherty, Peter C. Turner, Stephen J. Kedzierska, Katherine PLoS Pathog Research Article Emergence of a new influenza strain leads to a rapid global spread of the virus due to minimal antibody immunity. Pre-existing CD8(+) T-cell immunity directed towards conserved internal viral regions can greatly ameliorate the disease. However, mutational escape within the T cell epitopes is a substantial issue for virus control and vaccine design. Although mutations can result in a loss of T cell recognition, some variants generate cross-reactive T cell responses. In this study, we used reverse genetics to modify the influenza NP(336–374) peptide at a partially-solvent exposed residue (N->A, NPN3A mutation) to assess the availability, effectiveness and mechanism underlying influenza-specific cross-reactive T cell responses. The engineered virus induced a diminished CD8(+) T cell response and selected a narrowed T cell receptor (TCR) repertoire within two Vβ regions (Vβ8.3 and Vβ9). This can be partially explained by the H-2D(b)NPN3A structure that showed a loss of several contacts between the NPN3A peptide and H-2D(b), including a contact with His155, a position known to play an important role in mediating TCR-pMHC-I interactions. Despite these differences, common cross-reactive TCRs were detected in both the naïve and immune NPN3A-specific TCR repertoires. However, while the NPN3A epitope primes memory T-cells that give an equivalent recall response to the mutant or wild-type (wt) virus, both are markedly lower than wt->wt challenge. Such decreased CD8(+) responses elicited after heterologous challenge resulted in delayed viral clearance from the infected lung. Furthermore, mice first exposed to the wt virus give a poor, low avidity response following secondary infection with the mutant. Thus, the protective efficacy of cross-reactive CD8(+) T cells recognising mutant viral epitopes depend on peptide-MHC-I structural interactions and functional avidity. Our study does not support vaccine strategies that include immunization against commonly selected cross-reactive variants with mutations at partially-solvent exposed residues that have characteristics comparable to NPN3A. Public Library of Science 2010-08-12 /pmc/articles/PMC2920842/ /pubmed/20711359 http://dx.doi.org/10.1371/journal.ppat.1001039 Text en Valkenburg 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
Valkenburg, Sophie A.
Gras, Stephanie
Guillonneau, Carole
La Gruta, Nicole L.
Thomas, Paul G.
Purcell, Anthony W.
Rossjohn, Jamie
Doherty, Peter C.
Turner, Stephen J.
Kedzierska, Katherine
Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title_full Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title_fullStr Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title_full_unstemmed Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title_short Protective Efficacy of Cross-Reactive CD8(+) T Cells Recognising Mutant Viral Epitopes Depends on Peptide-MHC-I Structural Interactions and T Cell Activation Threshold
title_sort protective efficacy of cross-reactive cd8(+) t cells recognising mutant viral epitopes depends on peptide-mhc-i structural interactions and t cell activation threshold
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2920842/
https://www.ncbi.nlm.nih.gov/pubmed/20711359
http://dx.doi.org/10.1371/journal.ppat.1001039
work_keys_str_mv AT valkenburgsophiea protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT grasstephanie protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT guillonneaucarole protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT lagrutanicolel protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT thomaspaulg protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT purcellanthonyw protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT rossjohnjamie protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT dohertypeterc protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT turnerstephenj protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold
AT kedzierskakatherine protectiveefficacyofcrossreactivecd8tcellsrecognisingmutantviralepitopesdependsonpeptidemhcistructuralinteractionsandtcellactivationthreshold

Ejemplares similares