Author: Richter, Alex G.; Shields, Adrian M.; Karim, Abid; Birch, David; Faustini, Sian E.; Steadman, Lora; Ward, Kerensa; Plant, Timothy; Reynolds, Gary; Veenith, Tonny; Cunningham, Adam F.; Drayson, Mark T.; Wraith, David C.
Title: Establishing the prevalence of common tissueâ€specific autoantibodies following severe acute respiratory syndrome coronavirus 2 infection Cord-id: hkutwed9 Document date: 2021_6_13
ID: hkutwed9
Snippet: Coronavirus 19 (COVIDâ€19) has been associated with both transient and persistent systemic symptoms that do not appear to be a direct consequence of viral infection. The generation of autoantibodies has been proposed as a mechanism to explain these symptoms. To understand the prevalence of autoantibodies associated with severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) infection, we investigated the frequency and specificity of clinically relevant autoantibodies in 84 individuals
Document: Coronavirus 19 (COVIDâ€19) has been associated with both transient and persistent systemic symptoms that do not appear to be a direct consequence of viral infection. The generation of autoantibodies has been proposed as a mechanism to explain these symptoms. To understand the prevalence of autoantibodies associated with severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) infection, we investigated the frequency and specificity of clinically relevant autoantibodies in 84 individuals previously infected with SARSâ€CoVâ€2, suffering from COVIDâ€19 of varying severity in both the acute and convalescent setting. These were compared with results from 32 individuals who were on the intensive therapy unit (ITU) for nonâ€COVID reasons. We demonstrate a higher frequency of autoantibodies in the COVIDâ€19 ITU group compared with nonâ€COVIDâ€19 ITU disease control patients and that autoantibodies were also found in the serum 3–5 months postâ€COVIDâ€19 infection. Nonâ€COVID patients displayed a diverse pattern of autoantibodies; in contrast, the COVIDâ€19 groups had a more restricted panel of autoantibodies including skin, skeletal muscle and cardiac antibodies. Our results demonstrate that respiratory viral infection with SARSâ€CoVâ€2 is associated with the detection of a limited profile of tissueâ€specific autoantibodies, detectable using routine clinical immunology assays. Further studies are required to determine whether these autoantibodies are specific to SARSâ€CoVâ€2 or a phenomenon arising from severe viral infections and to determine the clinical significance of these autoantibodies.
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