Anti-SARS-CoV-2 antibodies from severe COVID-19 individuals or S2 immunizations do not worsen disease in hamsters
Visualitza/Obre
Autor/a
Data de publicació
2025-11-24ISSN
2399-3642
Resum
Severe COVID-19 associates with humoral immune response dysregulation. While antibodies confer
protection against SARS-CoV-2, evidence also support their putative contribution to disease severity.
Our study demonstrates that higher levels of S2-IgG, and S2-, RBD-, and Nucleocapsid-IgA
differentiate severe and non-severe cases. However, no major antibody functional differences are
found between both COVID-19 manifestations. Enhanced Fc-dependent functions in severe cases are
primarily driven by increased antibody titers. No differences in antibody avidity are found between
severe and non-severe cases, but a gradation in binding strength across specificities suggests that
early anti-RBD, -S2, and -Nucleocapsid antibodies may originate from different pathways. In golden
Syrian hamsters, S2 immunization or transfer of RBD-depleted antibodies isolated from severe and
non-severe cases promote a faster clinical recovery after SARS-CoV-2 challenge, despite a transient
initial weight loss. These findings indicate that antibodies are not major determinants of COVID-19
severity and suggest additional factors influencing disease outcomes.
Tipus de document
Article
Versió del document
Versió publicada
Llengua
Anglès
Matèries (CDU)
619 - Veterinària
Pàgines
17
Publicat per
Nature Research
Publicat a
Communications Biology
Número de l'acord de la subvenció
MICINN/Programa Estatal de promoción del talento y su empleabilidad en I+D+I/FJC2021-047205-I/ES/Development of a prophylactic vaccine targeting HIV Env vulnerability sites/
MICINN/ /RYC2020-028934-I/ES/ /
ESF/ / /EU/ /
Programa
Sanitat Animal
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