SARS-CoV-2 Spike and Nucleocapsid Antibody Response in Vaccinated Croatian Healthcare Workers and Infected Hospitalized Patients: A Single Center Cohort Study

Author:

Brlić Paola KučanORCID,Pavletić Martina,Lerga Mate,Krstanović Fran,Matešić Marina PribanićORCID,Miklić Karmela,Malić Suzana,Mikša Leonarda,Pajcur Maja,Peruč Dolores,Schubert MarenORCID,Bertoglio FedericoORCID,Arapović JuricaORCID,Protić Alen,Šustić AlanORCID,Milošević Marko,Šain Luka ČičinORCID,Jonjić Stipan,Lisnić Vanda JuranićORCID,Brizić IlijaORCID

Abstract

Studies assessing the dynamics and duration of antibody responses following SARS-CoV-2 infection or vaccination are an invaluable tool for vaccination schedule planning, assessment of risk groups and management of pandemics. In this study, we developed and employed ELISA assays to analyze the humoral responses to Nucleocapsid and Spike proteins in vaccinated health-care workers (HCW) and critically ill COVID-19 patients. Sera of more than 1000 HCWs and critically ill patients from the Clinical Hospital Center Rijeka were tested across a one-year period, encompassing the spread of major SARS-CoV-2 variants of concern (VOCs). We observed 97% of seroconversion in HCW cohort as well as sustained anti-Spike antibody response in vaccinees for more than 6 months. In contrast, the infection-induced anti-Nucleocapsid response was waning significantly in a six-month period. Furthermore, a substantial decrease in vaccinees’ anti-Spike antibodies binding to Spike protein of Omicron VOC was also observed. Critically ill COVID-19 patients had higher levels of anti-Spike and anti-Nucleocapsid antibodies compared to HCWs. No significant differences in anti-Spike and anti-Nucleocapsid antibody levels between the critically ill COVID-19 patients that were on non-invasive oxygen supplementation and those on invasive ventilation support were observed. However, stronger anti-Spike, but not anti-Nucleocapsid, antibody response correlated with a better disease outcome in the cohort of patients on invasive ventilation support. Altogether, our results contribute to the growing pool of data on humoral responses to SARS-CoV-2 infection and vaccination.

Funder

European Regional Development Fund

Helmholtz Association

Croatian Science Foundation

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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