Clonal structure and the specificity of vaccine-induced T cell response to SARS-CoV-2 Spike protein

Adenovirus vaccines, particularly the COVID-19 Ad5-nCoV adenovirus vaccine, have emerged as promising tools in the fight against infectious diseases. In this study, we investigated the structure of the T cell response to the Spike protein of the SARS-CoV-2 virus used in the COVID-19 Ad5-nCoV adenoviral vaccine in a phase 3 clinical trial (NCT04540419). In 69 participants, we collected peripheral blood samples at four time points after vaccination or placebo injection. Sequencing of T cell receptor repertoires from Spike-stimulated T cell cultures at day 14 from 17 vaccinated revealed a more diverse CD4+ T cell repertoire compared to CD8+. Nevertheless, CD8+ clonotypes accounted for more than half of the Spike-specific repertoire. Our longitudinal analysis showed a peak T cell response at day 14, followed by a decline until month 6. Remarkably, multiple T cell clonotypes persisted for at least 6 months after vaccination, as demonstrated by ex vivo stimulation. Examination of CDR3 regions revealed homologous sequences in both CD4+ and CD8+ clonotypes, with major CD8+ clonotypes sharing high similarity with annotated sequences specific for the NYNYLYRLF peptide, suggesting potential immunodominance. In conclusion, our study demonstrates the immunogenicity of the Ad5-nCoV adenoviral vaccine and highlights its ability to induce robust and durable T cell responses. These findings provide valuable insight into the efficacy of the vaccine against COVID-19 and provide critical information for ongoing efforts to control infectious diseases.

Authors
Sheetikov S.A.1, 2 , Khmelevskaya A.A.1 , Zornikova K.V.1, 2 , Zvyagin I.V.3, 4 , Shomuradova A.S.1, 2 , Serdyuk Y.V.1 , Shakirova N.T.1 , Peshkova I.O.1 , Titov Aleksei1 , Romaniuk D.S.1 , Shagina I.A.3, 4 , Chudakov D.M.3, 4, 5 , Kiryukhin D.O. 1 , Shcherbakova O.V.1 , Khamaganova E.G.1 , Dzutseva Vitalina6, 7 , Afanasiev Andrei7 , Bogolyubova A.V.1 , Efimov G.A.1
Publisher
Frontiers Media S.A.
Language
English
Pages
1369436
Status
Published
Volume
15
Year
2024
Organizations
  • 1 National Medical Research Center for Hematology
  • 2 Lomonosov Moscow State University
  • 3 Pirogov Russian National Research Medical University
  • 4 Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry
  • 5 Central European Institute of Technology, Masaryk University
  • 6 Novosibirsk State University, Medical School
  • 7 NPO Petrovax Pharm LLC
Keywords
T cell; vaccination; SARS-CoV-2; adenoviral vaccine; T cell receptor; spike protein; TCR sequencing

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