Prolonged T-cell activation and long COVID symptoms independently associate with severe COVID-19 at 3 months

T细胞活化持续时间延长和新冠长期症状与3个月后出现重症新冠独立相关。

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作者:Marianna Santopaolo #,Michaela Gregorova #,Fergus Hamilton,David Arnold,Anna Long,Aurora Lacey,Elizabeth Oliver,Alice Halliday,Holly Baum,Kristy Hamilton,Rachel Milligan,Olivia Pearce,Lea Knezevic,Begonia Morales Aza,Alice Milne,Emily Milodowski,Eben Jones,Rajeka Lazarus,Anu Goenka,Adam Finn ,Nicholas Maskell,Andrew D Davidson,Kathleen Gillespie,Linda Wooldridge,Laura Rivino

Abstract

Coronavirus disease-19 (COVID-19) causes immune perturbations which may persist long term, and patients frequently report ongoing symptoms for months after recovery. We assessed immune activation at 3-12 months post hospital admission in 187 samples from 63 patients with mild, moderate, or severe disease and investigated whether it associates with long COVID. At 3 months, patients with severe disease displayed persistent activation of CD4+ and CD8+ T-cells, based on expression of HLA-DR, CD38, Ki67, and granzyme B, and elevated plasma levels of interleukin-4 (IL-4), IL-7, IL-17, and tumor necrosis factor-alpha (TNF-α) compared to mild and/or moderate patients. Plasma from severe patients at 3 months caused T-cells from healthy donors to upregulate IL-15Rα, suggesting that plasma factors in severe patients may increase T-cell responsiveness to IL-15-driven bystander activation. Patients with severe disease reported a higher number of long COVID symptoms which did not however correlate with cellular immune activation/pro-inflammatory cytokines after adjusting for age, sex, and disease severity. Our data suggests that long COVID and persistent immune activation may correlate independently with severe disease.

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