Author: Goncalves, David; Mezidi, Mehdi; Bastard, Paul; Perret, Magali; Saker, Kahina; Fabien, Nicole; Pescarmona, Rémi; Lombard, Christine; Walzer, Thierry; Casanova, Jeanâ€Laurent; Belot, Alexandre; Richard, Jeanâ€Christophe; Trouilletâ€Assant, Sophie
Title: Antibodies against type I interferon: detection and association with severe clinical outcome in COVIDâ€19 patients Cord-id: 3iy723hv Document date: 2021_8_17
ID: 3iy723hv
Snippet: OBJECTIVES: Impairment of type I interferon (IFNâ€I) immunity has been reported in critically ill COVIDâ€19 patients. This defect can be explained in a subset of patients by the presence of circulating autoantibodies (autoâ€Abs) against IFNâ€I. We set out to improve the detection and the quantification of IFNâ€I autoâ€Abs in a cohort of critically ill COVIDâ€19 patients, in order to better evaluate the prevalence of these Abs as the pandemic progresses, and how they correlate with the cli
Document: OBJECTIVES: Impairment of type I interferon (IFNâ€I) immunity has been reported in critically ill COVIDâ€19 patients. This defect can be explained in a subset of patients by the presence of circulating autoantibodies (autoâ€Abs) against IFNâ€I. We set out to improve the detection and the quantification of IFNâ€I autoâ€Abs in a cohort of critically ill COVIDâ€19 patients, in order to better evaluate the prevalence of these Abs as the pandemic progresses, and how they correlate with the clinical course of the disease. METHODS: The concentration of antiâ€IFNâ€Î±(2) Abs was determined in the serum of 84 critically ill COVIDâ€19 patients who were admitted to ICU in Hospices Civils de Lyon, France, using a commercially available kit (Thermo Fisher, Catalog #BMS217). RESULTS: A total of 21 of 84 (25%) critically ill COVIDâ€19 patients had circulating antiâ€IFNâ€Î±(2) Abs above cutâ€off (> 34 ng mL(−1)). Among them, 15 of 21 had Abs with neutralising activity against IFNâ€Î±(2), that is 15 of 84 (18%) critically ill patients. In addition, we noticed an impairment of the IFNâ€I response in the majority of patients with neutralising antiâ€IFNâ€Î±(2) Abs. There was no significant difference in the clinical characteristics or outcome of with or without neutralising antiâ€IFNâ€Î±(2) autoâ€Abs. We detected antiâ€IFNâ€Î±(2) autoâ€Abs in COVIDâ€19 patients' sera throughout their ICU stay. Finally, we also found autoâ€Abs against multiple subtypes of IFNâ€I including IFNâ€Ï‰. CONCLUSIONS: We reported that 18% of critically ill COVIDâ€19 patients were positive for IFNâ€I autoâ€Abs, whereas all mild COVIDâ€19 patients were negative, confirming that the presence of these antibodies is associated with a higher risk of developing a critical COVIDâ€19 form.
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