Vascular Damage, Thromboinflammation, Plasmablast Activation, T-Cell Dysregulation and Pathological Histiocytic Response in Pulmonary Draining Lymph Nodes of COVID-19

Jasmin D Haslbauer; Carl Zinner; Anna K Stalder; Jan Schneeberger; Thomas Menter; Stefano Bassetti; Kirsten D Mertz; Philip Went; Matthias S Matter; Alexandar Tzankov

doi:10.3389/fimmu.2021.763098

Vascular Damage, Thromboinflammation, Plasmablast Activation, T-Cell Dysregulation and Pathological Histiocytic Response in Pulmonary Draining Lymph Nodes of COVID-19

Front Immunol. 2021 Dec 13:12:763098. doi: 10.3389/fimmu.2021.763098. eCollection 2021.

Affiliations

¹ Pathology, Institute of Medical Genetics and Pathology, University Hospital Basel, University of Basel, Basel, Switzerland.
² Department of Biomedicine, University of Basel, Basel, Switzerland.
³ Department of Internal Medicine, University Hospital Basel, University of Basel, Basel, Switzerland.
⁴ Pathology, Cantonal Hospital Baselland, Liestal, Switzerland.
⁵ Pathology, Cantonal Hospital Graubünden, Chur, Switzerland.

Abstract

Although initial immunophenotypical studies on peripheral blood and bronchoalveolar lavage samples have provided a glimpse into the immunopathology of COVID-19, analyses of pulmonary draining lymph nodes are currently scarce. 22 lethal COVID-19 cases and 28 controls were enrolled in this study. Pulmonary draining lymph nodes (mediastinal, tracheal, peribronchial) were collected at autopsy. Control lymph nodes were selected from a range of histomorphological sequelae [unremarkable histology, infectious mononucleosis, follicular hyperplasia, non-SARS related HLH, extrafollicular plasmablast activation, non-SARS related diffuse alveolar damage (DAD), pneumonia]. Samples were mounted on a tissue microarray and underwent immunohistochemical staining for a selection of immunological markers and in-situ hybridization for Epstein Barr Virus (EBV) and SARS-CoV-2. Gene expression profiling was performed using the HTG EdgeSeq Immune Response Panel. Characteristic patterns of a dysregulated immune response were detected in COVID-19: 1. An accumulation of extrafollicular plasmablasts with a relative paucity or depletion of germinal centers. 2. Evidence of T-cell dysregulation demonstrated by immunohistochemical paucity of FOXP3+, Tbet+ and LEF1+ positive T-cells and a downregulation of key genes responsible for T-cell crosstalk, maturation and migration as well as a reactivation of herpes viruses in 6 COVID-19 lymph nodes (EBV, HSV). 3. Macrophage activation by a M2-polarized, CD163+ phenotype and increased incidence of hemophagocytic activity. 4. Microvascular dysfunction, evidenced by an upregulation of hemostatic (CD36, PROCR, VWF) and proangiogenic (FLT1, TEK) genes and an increase of fibrin microthrombi and CD105+ microvessels. Taken together, these findings imply widespread dysregulation of both innate and adoptive pathways with concordant microvascular dysfunction in severe COVID-19.

Keywords: COVID-19; T-cell dysregulation; immunopathology; lymph nodes; macrophage activation; plasmablasts; thromboinflammation; thrombosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Aged, 80 and over
COVID-19 / immunology*
COVID-19 / pathology*
Cohort Studies
Female
Humans
Lung
Lymph Nodes / immunology*
Lymph Nodes / pathology*
Macrophage Activation / immunology
Male
Middle Aged
SARS-CoV-2
T-Lymphocytes / immunology
T-Lymphocytes / pathology
Thromboinflammation / immunology
Thromboinflammation / pathology
Thromboinflammation / virology