Cellular Immunity of SARS-CoV-2 in the Borriana COVID-19 Cohort: A Nested Case–Control Study

Author:

Domènech-Montoliu Salvador1,Puig-Barberà Joan2ORCID,Pac-Sa María Rosario3,Orrico-Sanchéz Alejandro245ORCID,Gómez-Lanas Lorna6,Sala-Trull Diego6,Domènech-Leon Carmen7,Del Rio-González Alba8,Sánchez-Urbano Manuel6ORCID,Satorres-Martinez Paloma6,Aparisi-Esteve Laura9,Badenes-Marques Gema6,Blasco-Gari Roser6,Casanova-Suarez Juan10,Gil-Fortuño María11,Hernández-Pérez Noelia11,Jovani-Sales David6ORCID,López-Diago Laura12,Notari-Rodríguez Cristina6,Pérez-Olaso Oscar11,Romeu-Garcia María Angeles3,Ruíz-Puig Raquel6,Arnedo-Pena Alberto3413ORCID

Affiliation:

1. Medical Direction University Hospital de la Plana, 12540 Vila-real, Spain

2. Vaccines Research Unit, Foundation for the Promotion of Health and Biomedical Research in Valencia Region FISABIO-Public Health, 46020 Valencia, Spain

3. Public Health Center, 12003 Castelló de la Plana, Spain

4. Epidemiology and Public Health (CIBERESP), 28029 Madrid, Spain

5. Secretary of Chair of Vaccines Catholic University of Valencia, 46001 Valencia, Spain

6. Emergency Service University Hospital de la Plana, 12540 Vila-real, Spain

7. Department of Medicine, University CEU Cardenal Herrera, 12006 Castelló de la Plana, Spain

8. Health Centers I and II, 12530 Borriana, Spain

9. Carinyena Health Center, 12540 Vila-real, Spain

10. Nursing Service University Hospital de la Plana, 12540 Vila-real, Spain

11. Microbiology Service University Hospital de la Plana, 12540 Vila-real, Spain

12. Clinical Analysis Service University Hospital de la Plana, 12540 Vila-real, Spain

13. Department of Health Science, Public University Navarra, 31006 Pamplona, Spain

Abstract

Our goal was to determine the cellular immune response (CIR) in a sample of the Borriana COVID-19 cohort (Spain) to identify associated factors and their relationship with infection, reinfection and sequelae. We conducted a nested case–control study using a randomly selected sample of 225 individuals aged 18 and older, including 36 individuals naïve to the SARS-CoV-2 infection and 189 infected patients. We employed flow-cytometry–based immunoassays for intracellular cytokine staining, using Wuhan and BA.2 antigens, and chemiluminescence microparticle immunoassay to detect SARS-CoV-2 antibodies. Logistic regression models were applied. A total of 215 (95.6%) participants exhibited T-cell response (TCR) to at least one antigen. Positive responses of CD4+ and CD8+ T cells were 89.8% and 85.3%, respectively. No difference in CIR was found between naïve and infected patients. Patients who experienced sequelae exhibited a higher CIR than those without. A positive correlation was observed between TCR and anti-spike IgG levels. Factors positively associated with the TCR included blood group A, number of SARS-CoV-2 vaccine doses received, and anti-N IgM; factors inversely related were the time elapsed since the last vaccine dose or infection, and blood group B. These findings contribute valuable insights into the nuanced immune landscape shaped by SARS-CoV-2 infection and vaccination.

Funder

Consellería de Sanitat Universal i Salut Pública

EU Operational Program of the European Regional Development Fund

Publisher

MDPI AG

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