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Rappe, Julie C.F. ; Finsterbusch, Katja ; Crotta, Stefania ; Mack, Matthias ; Priestnall, Simon L. ; Wack, Andreas

A TLR7 antagonist restricts interferon-dependent and -independent immunopathology in a mouse model of severe influenza

Rappe, Julie C.F., Finsterbusch, Katja, Crotta, Stefania, Mack, Matthias, Priestnall, Simon L. and Wack, Andreas (2021) A TLR7 antagonist restricts interferon-dependent and -independent immunopathology in a mouse model of severe influenza. Journal of Experimental Medicine 218 (11), e20201631.

Date of publication of this fulltext: 05 Oct 2023 10:51
Article
DOI to cite this document: 10.5283/epub.54789


Abstract

Cytokine-mediated immune-cell recruitment and inflammation contribute to protection in respiratory virus infection. However, uncontrolled inflammation and the "cytokine storm" are hallmarks of immunopathology in severe infection. Cytokine storm is a broad term for a phenomenon with diverse characteristics and drivers, depending on host genetics, age, and other factors. Taking advantage of the ...

Cytokine-mediated immune-cell recruitment and inflammation contribute to protection in respiratory virus infection. However, uncontrolled inflammation and the "cytokine storm" are hallmarks of immunopathology in severe infection. Cytokine storm is a broad term for a phenomenon with diverse characteristics and drivers, depending on host genetics, age, and other factors. Taking advantage of the differential use of virus-sensing systems by different cell types, we test the hypothesis that specifically blocking TLR7-dependent, immune cell-produced cytokines reduces influenza-related immunopathology. In a mouse model of severe influenza characterized by a type I interferon (IFN-I)-driven cytokine storm, TLR7 antagonist treatment leaves epithelial antiviral responses unaltered but acts through pDCs and monocytes to reduce IFN-I and other cytokines in the lung, thus ameliorating inflammation and severity. Moreover, even in the absence of IFN-I signaling, TLR7 antagonism reduces inflammation and mortality driven by monocyte-produced chemoattractants and neutrophil recruitment into the infected lung. Hence, TLR7 antagonism reduces diverse types of cytokine storm in severe influenza.



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Details

Item typeArticle
Journal or Publication TitleJournal of Experimental Medicine
Publisher:ROCKEFELLER UNIV PRESS
Place of Publication:NEW YORK
Volume:218
Number of Issue or Book Chapter:11
Page Range:e20201631
Date2 September 2021
InstitutionsMedicine > Abteilung für Nephrologie
Identification Number
ValueType
10.1084/jem.20201631DOI
KeywordsPLASMACYTOID DENDRITIC CELLS; DEMONSTRATES CLINICAL ACTIVITY; SINGLE-STRANDED RNA; I INTERFERON; LUNG INJURY; RECEPTOR 7; AIRWAY INFLAMMATION; MURINE MODEL; PHASE 2A; RECOGNITION;
Dewey Decimal Classification600 Technology > 610 Medical sciences Medicine
StatusPublished
RefereedYes, this version has been refereed
Created at the University of RegensburgYes
URN of the UB Regensburgurn:nbn:de:bvb:355-epub-547892
Item ID54789

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