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Delayed bystander CD8 T cell activation, early immune pathology and persistent dysregulation characterise severe COVID-19

Authors
  • Bergamaschi, Laura
  • Mescia, Federica
  • Turner, Lorinda
  • Hanson, Aimee
  • Kotagiri, Prasanti
  • Dunmore, Benjamin J
  • Ruffieux, Hélène
  • De Sa, Aloka
  • Huhn, Oisín
  • Morgan, Michael D
  • Gerber, Pehuen Pereyra
  • Wills, Mark R
  • Baker, Stephen
  • Calero-Nieto, Fernando J
  • Doffinger, Rainer
  • Dougan, Gordon
  • Elmer, Anne
  • Goodfellow, Ian G
  • Gupta, Ravindra K
  • Hosmillo, Myra
  • And 17 more
Publication Date
Sep 27, 2024
Source
Apollo - University of Cambridge Repository
Keywords
Language
English
License
Green
External links

Abstract

<jats:title>Summary</jats:title><jats:p>In a study of 207 SARS-CoV2-infected individuals with a range of severities followed over 12 weeks from symptom onset, we demonstrate that an early robust bystander CD8 T cell immune response, without systemic inflammation, is characteristic of asymptomatic or mild disease. Those presenting to hospital had delayed bystander responses and systemic inflammation already evident at around symptom onset. Such early evidence of inflammation suggests immunopathology may be inevitable in some individuals, or that preventative intervention might be needed before symptom onset. Viral load does not correlate with the development of this pathological response, but does with its subsequent severity. Immune recovery is complex, with profound persistent cellular abnormalities correlating with a change in the nature of the inflammatory response, where signatures characteristic of increased oxidative phosphorylation and reactive-oxygen species-associated inflammation replace those driven by TNF and IL-6. These late immunometabolic inflammatory changes and unresolved immune defects may have clinical implications.</jats:p>

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