The impact of hypoxia on B cells in COVID-19

Author:

Kotagiri Prasanti,Mescia Federica,Hanson Aimee,Turner Lorinda,Bergamaschi Laura,Peñalver Ana,Richoz Nathan,Moore Stephen D,Ortmann Brian M,Dunmore Benjamin J.,Ruffieux HeleneORCID,Morgan Michael D,Tuong Zewen Kelvin,Bashford-Rogers Rachael J M,Hosmillo Myra,Baker Stephen,Elmer Anne,Goodfellow Ian G,Gupta Ravindra K.ORCID,Kingston Nathalie,Lehner Paul J.,Matheson Nicholas J.,Richardson Sylvia,Saunders Caroline,Weekes Michael P.ORCID,Göttgens Berthold,Toshner Mark,Hess Christoph,Maxwell Patrick. H.,Clatworthy Menna. R.,Nathan James A.,Bradley John R.,Lyons Paul A.,Burrows Natalie,Smith Kenneth G.C.,

Abstract

AbstractProminent early features of COVID-19 include severe, often clinically silent, hypoxia and a pronounced reduction in B cells, the latter important in defence against SARS-CoV-2. This brought to mind the phenotype of mice with VHL-deficient B cells, in which Hypoxia-Inducible Factors are constitutively active, suggesting hypoxia might drive B cell abnormalities in COVID-19. We demonstrated the breadth of early and persistent defects in B cell subsets in moderate/severe COVID-19, including reduced marginal zone-like, memory and transitional B cells, changes we also observed in B cell VHL-deficient mice. This was corroborated by hypoxia-related transcriptional changes in COVID-19 patients, and by similar B cell abnormalities in mice kept in hypoxic conditions, including reduced marginal zone and germinal center B cells. Thus hypoxia might contribute to B cell pathology in COVID-19, and in other hypoxic states. Through this mechanism it may impact on COVID-19 outcome, and be remediable through early oxygen therapy.

Publisher

Cold Spring Harbor Laboratory

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