Unbiased single cell spatial analysis localises inflammatory clusters of immature neutrophils-CD8 T cells to alveolar progenitor cells in fatal COVID-19 lungs

Author:

,Weeratunga Praveen,Denney Laura,Bull Joshua A.ORCID,Repapi Emmanouela,Sergeant Martin,Etherington Rachel,Vuppussetty Chaitanya,Turner Gareth D.H.,Clelland Colin,Cross Amy,Issa Fadi,de Andrea Carlos Eduardo,Bermejo Ignacio Melero,Sims David,McGowan Simon,Zurke Yasemin-Xiomara,Ahern David J.,Gamez Eddie C,Whalley Justin,Richards Duncan,Klenerman Paul,Monaco Claudia,Udalova Irina A.,Dong Tao,Ogg Graham,Knight Julian C.,Byrne Helen M.,Taylor Stephen,Ho Ling-Pei

Abstract

AbstractSingle cell spatial interrogation of the immune-structural interactions in COVID -19 lungs is challenging, mainly because of the marked cellular infiltrate and architecturally distorted microstructure. To address this, we developed a suite of mathematical tools to search for statistically significant co-locations amongst immune and structural cells identified using 37-plex imaging mass cytometry. This unbiased method revealed a cellular map interleaved with an inflammatory network of immature neutrophils, cytotoxic CD8 T cells, megakaryocytes and monocytes co-located with regenerating alveolar progenitors and endothelium. Of note, a highly active cluster of immature neutrophils and cytotoxic CD8 T cells, was found spatially linked with alveolar progenitor cells, and temporally with the diffuse alveolar damage stage. These findings provide new insights into how immune cells interact in the lungs of severe COVID-19 disease. We provide our pipeline [Spatial Omics Oxford Pipeline (SpOOx)] and visual-analytical tool, Multi-Dimensional Viewer (MDV) software, as a resource for spatial analysis.Graphical abstract

Publisher

Cold Spring Harbor Laboratory

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