Restrained memory CD8+T cell responses favors viral persistence and elevated IgG responses in patients with severe Long COVID

Author:

Rodriguez Lucie,Tan Ziyang,Lakshmikanth Tadepally,Wang Jun,Barcenilla Hugo,Swank Zoe,Zuo Fanglei,Abolhassani Hassan,Pavlovitch-Bedzyk Ana Jimena,Wang Chunlin,Gonzalez Laura,Mugabo Constantin Habimana,Johnsson Anette,Chen Yang,James Anna,Mikes Jaromir,Kleberg Linn,Sundling ChristopherORCID,Björnson Mikael,Bonnier Malin Nygren,Ståhlberg Marcus,Runold Michael,Björkander Sophia,Melén Erik,Meyts Isabelle,Weyenbergh Johan Van,Hammarström Qian-Pan,Davis Mark M,Walt David R.ORCID,Landegren Nils, ,Aiuti Alessandro,Casari Giorgio,Casanova Jean-Laurent,Jamoulle Marc,Bruchfeld Judith,Brodin PetterORCID

Abstract

AbstractDuring the COVID-19 pandemic it was widely described that certain individuals infected by SARS-CoV-2 experience persistent disease signs and symptoms, Long COVID, which in some cases is very severe with life changing consequences. To maximize our chances of identifying the underpinnings of this illness, we have focused on 121 of the most severe cases from >1000 patients screened in specialized clinics in Sweden and Belgium. We restricted this study to subjects with objective measures of organ damage or dysfunction, >3 months following a verified, but mild-to-moderate SARS-CoV-2 infection. By performing systems-level immunological testing and comparisons to controls fully convalescent following a similar mild/moderate COVID-19 episode, we identify elevated serological responses to SARS-CoV-2 in severe Long COVID suggestive of chronic antigen stimulation. Persistent viral reservoirs have been proposed in Long COVID and using multiple orthogonal methods for detection of SARS-CoV-2 RNA and protein in plasma we identify a subset of patients with detectable antigens, but with minimal overlap across assays, and no correlation to symptoms or immune measurements. Elevated serologic responses to SARS-CoV-2 on the other hand were inversely correlated with clonally expanded memory CD8+T cells, indicating that restrained clonal expansion enables viral persistence, chronic antigen exposure and elevated IgG responses, even if antigen-detection in blood is not universally possible.

Publisher

Cold Spring Harbor Laboratory

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