High throughput spatial immune mapping reveals an innate immune scar in post-COVID-19 brains

Marius Schwabenland; Dilara Hasavci; Sibylle Frase; Katharina Wolf; Nikolaus Deigendesch; Joerg M Buescher; Kirsten D Mertz; Benjamin Ondruschka; Hermann Altmeppen; Jakob Matschke; Markus Glatzel; Stephan Frank; Robert Thimme; Juergen Beck; Jonas A Hosp; Thomas Blank; Bertram Bengsch; Marco Prinz

doi:10.1007/s00401-024-02770-6

High throughput spatial immune mapping reveals an innate immune scar in post-COVID-19 brains

Marius Schwabenland
Dilara Hasavci
Sibylle Frase
Katharina Wolf
Nikolaus Deigendesch
Joerg M Buescher
Kirsten D Mertz
Benjamin Ondruschka
Hermann Altmeppen
Jakob Matschke
Markus Glatzel
Stephan Frank
Robert Thimme
Juergen Beck
Jonas A Hosp
Thomas Blank
Bertram Bengsch
Marco Prinz

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Abstract

The underlying pathogenesis of neurological sequelae in post-COVID-19 patients remains unclear. Here, we used multidimensional spatial immune phenotyping and machine learning methods on brains from initial COVID-19 survivors to identify the biological correlate associated with previous SARS-CoV-2 challenge. Compared to healthy controls, individuals with post-COVID-19 revealed a high percentage of TMEM119+P2RY12+CD68+Iba1+HLA-DR+CD11c+SCAMP2+ microglia assembled in prototypical cellular nodules. In contrast to acute SARS-CoV-2 cases, the frequency of CD8+ parenchymal T cells was reduced, suggesting an immune shift toward innate immune activation that may contribute to neurological alterations in post-COVID-19 patients.

Bibliographical data

Original language	English
ISSN	0001-6322
DOIs	https://doi.org/10.1007/s00401-024-02770-6
Publication status	Published - 25.07.2024

Comment Deanary

PubMed	39060438