Quantification of epitope abundance reveals the effect of direct and cross-presentation on influenza CTL responses

Ting Wu; Jing Guan; Andreas Handel; David C. Tscharke; John Sidney; Alessandro Sette; Linda M. Wakim; Xavier Y.X. Sng; Paul G. Thomas; Nathan P. Croft; Anthony W. Purcell; Nicole L. La Gruta

doi:10.1038/s41467-019-10661-8

Quantification of epitope abundance reveals the effect of direct and cross-presentation on influenza CTL responses

Ting Wu, Jing Guan, Andreas Handel, David C. Tscharke, John Sidney, Alessandro Sette, Linda M. Wakim, Xavier Y.X. Sng, Paul G. Thomas, Nathan P. Croft^*, Anthony W. Purcell, Nicole L. La Gruta

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

77 Citations (Scopus)

Abstract

The magnitude of T cell responses to infection is a function of the naïve T cell repertoire combined with the context and duration of antigen presentation. Using mass spectrometry, we identify and quantify 21 class 1 MHC-restricted influenza A virus (IAV)-peptides following either direct or cross-presentation. All these peptides, including seven novel epitopes, elicit T cell responses in infected C57BL/6 mice. Directly presented IAV epitopes maintain their relative abundance across distinct cell types and reveal a broad range of epitope abundances. In contrast, cross-presented epitopes are more uniform in abundance. We observe a clear disparity in the abundance of the two key immunodominant IAV antigens, wherein direct infection drives optimal nucleoprotein (NP)_366–374 presentation, while cross-presentation is optimal for acid polymerase (PA)_224–233 presentation. The study demonstrates how assessment of epitope abundance in both modes of antigen presentation is necessary to fully understand the immunogenicity and response magnitude to T cell epitopes.

Original language	English
Article number	2846
Journal	Nature Communications
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-10661-8
Publication status	Published - 1 Dec 2019

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Wu, T., Guan, J., Handel, A., Tscharke, D. C., Sidney, J., Sette, A., Wakim, L. M., Sng, X. Y. X., Thomas, P. G., Croft, N. P., Purcell, A. W., & La Gruta, N. L. (2019). Quantification of epitope abundance reveals the effect of direct and cross-presentation on influenza CTL responses. Nature Communications, 10(1), Article 2846. https://doi.org/10.1038/s41467-019-10661-8

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abstract = "The magnitude of T cell responses to infection is a function of the na{\"i}ve T cell repertoire combined with the context and duration of antigen presentation. Using mass spectrometry, we identify and quantify 21 class 1 MHC-restricted influenza A virus (IAV)-peptides following either direct or cross-presentation. All these peptides, including seven novel epitopes, elicit T cell responses in infected C57BL/6 mice. Directly presented IAV epitopes maintain their relative abundance across distinct cell types and reveal a broad range of epitope abundances. In contrast, cross-presented epitopes are more uniform in abundance. We observe a clear disparity in the abundance of the two key immunodominant IAV antigens, wherein direct infection drives optimal nucleoprotein (NP)366–374 presentation, while cross-presentation is optimal for acid polymerase (PA)224–233 presentation. The study demonstrates how assessment of epitope abundance in both modes of antigen presentation is necessary to fully understand the immunogenicity and response magnitude to T cell epitopes.",

author = "Ting Wu and Jing Guan and Andreas Handel and Tscharke, {David C.} and John Sidney and Alessandro Sette and Wakim, {Linda M.} and Sng, {Xavier Y.X.} and Thomas, {Paul G.} and Croft, {Nathan P.} and Purcell, {Anthony W.} and {La Gruta}, {Nicole L.}",

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AU - Wu, Ting

AU - Guan, Jing

AU - Handel, Andreas

AU - Tscharke, David C.

AU - Sidney, John

AU - Sette, Alessandro

AU - Wakim, Linda M.

AU - Sng, Xavier Y.X.

AU - Thomas, Paul G.

AU - Croft, Nathan P.

AU - Purcell, Anthony W.

AU - La Gruta, Nicole L.

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AB - The magnitude of T cell responses to infection is a function of the naïve T cell repertoire combined with the context and duration of antigen presentation. Using mass spectrometry, we identify and quantify 21 class 1 MHC-restricted influenza A virus (IAV)-peptides following either direct or cross-presentation. All these peptides, including seven novel epitopes, elicit T cell responses in infected C57BL/6 mice. Directly presented IAV epitopes maintain their relative abundance across distinct cell types and reveal a broad range of epitope abundances. In contrast, cross-presented epitopes are more uniform in abundance. We observe a clear disparity in the abundance of the two key immunodominant IAV antigens, wherein direct infection drives optimal nucleoprotein (NP)366–374 presentation, while cross-presentation is optimal for acid polymerase (PA)224–233 presentation. The study demonstrates how assessment of epitope abundance in both modes of antigen presentation is necessary to fully understand the immunogenicity and response magnitude to T cell epitopes.

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Quantification of epitope abundance reveals the effect of direct and cross-presentation on influenza CTL responses

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