Local CCL18 and CCL21 expand lung fibrovascular niches and recruit lymphocytes, leading to tertiary lymphoid structure formation in prolonged COVID-19

Ronja Mothes
Anna Pascual-Reguant
Ralf Koehler
Juliane Liebeskind
Alina Liebheit
Sandy Bauherr
Carsten Dittmayer
Michael Laue
Regina von Manitius
Sefer Elezkurtaj
Pawel Durek
Frederik Heinrich
Gitta Anne Heinz
Gabriela Maria Guerra
Benedikt Obermayer
Jenny Meinhardt
Jana Ihlow
Josefine Radke
Frank L. Heppner
Philipp Enghard
Helena Stockmann
Tom Aschman
Julia Schneider
Victor Corman
Leif Erik Sander
Mir-Farzin Mashreghi
Thomas Conrad
Andreas Hocke
Raluca A. Niesner
Helena Radbruch
Anja E. Hauser

1 evaluations Published on Mar 27, 2022

This article on Sciety

Abstract

Post-acute lung sequelae of COVID-19 are challenging many survivors across the world, yet the mechanisms behind are poorly understood. Our results delineate an inflammatory cascade of events occurring along disease progression within fibrovascular niches. It is initiated by endothelial dysfunction, followed by heme scavenging of CD163⁺ macrophages and production of CCL18. This chemokine synergizes with local CCL21 upregulation to influence the stromal composition favoring endothelial to mesenchymal transition. The local immune response is further modulated via recruitment of CCR7⁺ T cells into the expanding fibrovascular niche and imprinting an exhausted, T follicular helper–like phenotype in these cells. Eventually, this culminates in the formation of tertiary lymphoid structures, further perpetuating chronic inflammation. Thus, our work presents misdirected immune-stromal interaction mechanisms promoting a self-sustained and non-resolving local immune response that extends beyond active viral infection and leads to profound tissue repurposing and chronic inflammation.

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