Frontiers in Immunology (Oct 2023)

Distinct anti-NP, anti-RBD and anti-Spike antibody profiles discriminate death from survival in COVID-19

  • Carolina do Prado Servian,
  • Mônica Spadafora-Ferreira,
  • Déborah Carolina Carvalho dos Anjos,
  • Adriana Oliveira Guilarde,
  • Adriana Oliveira Guilarde,
  • Antonio Roberto Gomes-Junior,
  • Moara Alves Santa Bárbara Borges,
  • Moara Alves Santa Bárbara Borges,
  • Letícia Carrijo Masson,
  • João Marcos Maia Silva,
  • Matheus Henrique Assis de Lima,
  • Brenda Grazielli Nogueira Moraes,
  • Sueli Meira Souza,
  • Luiz Eterno Xavier,
  • Denise Cristina André de Oliveira,
  • João Victor Batalha-Carvalho,
  • Ana Maria Moro,
  • Ana Maria Moro,
  • Anamélia Lorenzetti Bocca,
  • Irmtraut Araci Hoffmann Pfrimer,
  • Nádia Lago Costa,
  • Valéria Christina de Rezende Feres,
  • Fabiola Souza Fiaccadori,
  • Menira Souza,
  • Luiz Gustavo Gardinassi,
  • Edison Luiz Durigon,
  • Pedro Roosevelt Torres Romão,
  • Soraia Attie Calil Jorge,
  • Verônica Coelho,
  • Verônica Coelho,
  • Verônica Coelho,
  • Viviane Fongaro Botosso,
  • Simone Gonçalves Fonseca,
  • Simone Gonçalves Fonseca

DOI
https://doi.org/10.3389/fimmu.2023.1206979
Journal volume & issue
Vol. 14

Abstract

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IntroductionInfection by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) induces rapid production of IgM, IgA, and IgG antibodies directed to multiple viral antigens that may have impact diverse clinical outcomes.MethodsWe evaluated IgM, IgA, and IgG antibodies directed to the nucleocapsid (NP), IgA and IgG to the Spike protein and to the receptor-binding domain (RBD), and the presence of neutralizing antibodies (nAb), in a cohort of unvaccinated SARS-CoV-2 infected individuals, in the first 30 days of post-symptom onset (PSO) (T1).ResultsThis study included 193 coronavirus disease 2019 (COVID-19) participants classified as mild, moderate, severe, critical, and fatal and 27 uninfected controls. In T1, we identified differential antibody profiles associated with distinct clinical presentation. The mild group presented lower levels of anti-NP IgG, and IgA (vs moderate and severe), anti-NP IgM (vs severe, critical and fatal), anti-Spike IgA (vs severe and fatal), and anti-RBD IgG (vs severe). The moderate group presented higher levels of anti-RBD IgA, comparing with severe group. The severe group presented higher levels of anti-NP IgA (vs mild and fatal) and anti-RBD IgG (vs mild and moderate). The fatal group presented higher levels of anti-NP IgM and anti-Spike IgA (vs mild), but lower levels of anti-NP IgA (vs severe). The levels of nAb was lower just in mild group compared to severe, critical, and fatal groups, moreover, no difference was observed among the more severe groups. In addition, we studied 82 convalescent individuals, between 31 days to 6 months (T2) or more than 6 months (T3), PSO, those: 12 mild, 26 moderate, and 46 severe plus critical. The longitudinal analyzes, for the severe plus critical group showed lower levels of anti-NP IgG, IgA and IgM, anti-Spike IgA in relation T3. The follow-up in the fatal group, reveals that the levels of anti-spike IgG increased, while anti-NP IgM levels was decreased along the time in severe/critical and fatal as well as anti-NP IgG and IgA in several/critical groups.DiscussionIn summary, the anti-NP IgA and IgG lower levels and the higher levels of anti-RBD and anti-Spike IgA in fatal compared to survival group of individuals admitted to the intensive care unit (ICU). Collectively, our data discriminate death from survival, suggesting that anti-RBD IgA and anti-Spike IgA may play some deleterious effect, in contrast with the potentially protective effect of anti-NP IgA and IgG in the survival group.

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