Comparative single-cell analysis reveals IFN-γ as a driver of respiratory sequelae after acute COVID-19.

Comparative single-cell analysis reveals IFN-γ as a driver of respiratory sequelae after acute COVID-19.

Publication date: Jul 17, 2024

Postacute sequelae of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection (PASC) represent an urgent public health challenge and are estimated to affect more than 60 million individuals globally. Although a growing body of evidence suggests that dysregulated immune reactions may be linked with PASC symptoms, most investigations have primarily centered around blood-based studies, with few focusing on samples derived from affected tissues. Furthermore, clinical studies alone often provide correlative insights rather than causal mechanisms. Thus, it is essential to compare clinical samples with relevant animal models and conduct functional experiments to understand the etiology of PASC. In this study, we comprehensively compared bronchoalveolar lavage fluid single-cell RNA sequencing data derived from clinical PASC samples and a mouse model of PASC. This revealed a pro-fibrotic monocyte-derived macrophage response in respiratory PASC, as well as abnormal interactions between pulmonary macrophages and respiratory resident T cells, in both humans and mice. Interferon-γ (IFN-γ) emerged as a key node mediating the immune anomalies in respiratory PASC. Neutralizing IFN-γ after the resolution of acute SARS-CoV-2 infection reduced lung inflammation and tissue fibrosis in mice. Together, our study underscores the importance of performing comparative analysis to understand the cause of PASC and suggests that the IFN-γ signaling axis might represent a therapeutic target.

Concepts Keywords
Coronavirus Animals
Essential Bronchoalveolar Lavage Fluid
Fibrosis COVID-19
Mice Disease Models, Animal
Proteins Female
Humans
Interferon-gamma
Interferon-gamma
Lung
Macrophages, Alveolar
Male
Mice
SARS-CoV-2
Single-Cell Analysis
T-Lymphocytes

Semantics

Type Source Name
disease IDO cell
disease MESH sequelae
disease MESH COVID-19
disease VO Severe acute respiratory syndrome coronavirus 2
disease MESH infection
disease IDO blood
disease MESH etiology
disease VO macrophage
disease MESH anomalies
pathway REACTOME SARS-CoV-2 Infection
disease MESH lung inflammation
disease MESH fibrosis
disease MESH Disease Models Animal

Original Article

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