SARS-CoV-2 escapes CD8 T cell surveillance via mutations in MHC-I restricted epitopes

Benedikt Agerer,Maximilian Koblischke,Venugopal Gudipati,Mark J. Smyth,Alexandra Popa,Jakob-Wendelin Genger,Lukas Endler,David M. Florian,Vanessa Muehlgrabner,Alexander Lercher,Pia Gattinger,Ricard Torralba-Gombau,Thomas Penz,Ingrid Faé,S. Wenda,Marianna Traungott,Gernot Walder,Gottfried Fischer,Wolfgang Hoepler,Erich Pawelka,Alexander Zoufaly,Rudolf Valenta,Christoph Bock,Johannes B. Huppa,Judith H. Aberle,Andreas Bergthaler

SARS-CoV-2 escapes CD8 T cell surveillance via mutations in MHC-I restricted epitopes

2020

CD8+ T cell immunity to SARS-CoV-2 has been implicated in COVID-19 severity and virus control, though direct evidence has been lacking so far. Here, we identified non-synonymous mutations in MHC-I restricted CD8+ T cell epitopes after deep sequencing of 747 SARS-CoV- 2 virus isolates. Mutant peptides exhibited diminished or abrogated MHC-I binding, which was associated with a loss of recognition and functional responses by CD8+ T cells isolated from HLA-matched COVID-19 patients. Our findings highlight the capacity of SARS-CoV-2 to subvert CD8+ T cell surveillance through escape mutations in MHCI-restricted viral epitopes. This provides evolutionary evidence for CD8+ T cell immunity controlling SARS-CoV-2 with consequences for COVID-19 vaccine design.

Keywords:

Major histocompatibility complex
Virus
T cell
Epitope
Biology
MHC class I
Mutant
CD8
Cytotoxic T cell
Virology

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