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Clonal analysis of immunodominance and cross-reactivity of the CD4 T cell response to SARS-CoV-2
Author(s) -
Jun Siong Low,
Daniela Vaqueirinho,
Federico Mele,
Mathilde Foglierini,
Josipa Jerak,
Michela Perotti,
David Jarrossay,
Sandra Jovic,
Laurent Perez,
Rosalia Cacciatore,
Tatiana Terrot,
Alessandra Franzetti-Pellanda,
Maira Biggiogero,
Christian Garzoni,
Paolo Ferrari,
Alessandro Ceschi,
Antonio Lanzavecchia,
Federica Sallusto,
Antonino Cassotta
Publication year - 2021
Publication title -
science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 12.556
H-Index - 1186
eISSN - 1095-9203
pISSN - 0036-8075
DOI - 10.1126/science.abg8985
Subject(s) - immunodominance , epitope , virology , biology , cross reactivity , t cell , antigen , coronavirus , memory t cell , immunology , immune system , covid-19 , cross reactions , medicine , disease , pathology , infectious disease (medical specialty)
The identification of CD4 + T cell epitopes is instrumental for the design of subunit vaccines for broad protection against coronaviruses. Here, we demonstrate in COVID-19-recovered individuals a robust CD4 + T cell response to naturally processed severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) spike (S) protein and nucleoprotein (N), including effector, helper, and memory T cells. By characterizing 2943 S-reactive T cell clones from 34 individuals, we found that the receptor-binding domain (RBD) is highly immunogenic and that 33% of RBD-reactive clones and 94% of individuals recognized a conserved immunodominant S346-S365 region comprising nested human leukocyte antigen DR (HLA-DR)- and HLA-DP-restricted epitopes. Using pre- and post-COVID-19 samples and S proteins from endemic coronaviruses, we identified cross-reactive T cells targeting multiple S protein sites. The immunodominant and cross-reactive epitopes identified can inform vaccination strategies to counteract emerging SARS-CoV-2 variants.

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