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BCL-XL antagonism selectively reduces neutrophil life span within inflamed tissues without causing neutropenia

Authors :
Jai Rautela
Peter E. Czabotar
Tobias Kratina
Christine R. Keenan
Yifan Zhan
Huon L. Wong
Nicholas D. Huntington
Manuela S Hancock
Christine A White
Emma M. Carrington
Ahmad Wardak
Vanessa L. Bryant
Wesley Wong
Rhys S. Allan
Guillaume Lessene
Yuyan Yang
Damian B D'Silva
Robyn L Schenk
Andrew M. Lew
Jacinta Hansen
Nadia Iannarella
Marco J Herold
Cynthia Louis
Robyn M. Sutherland
Ian P. Wicks
Duong Nhu
Source :
Blood Adv
Publication Year :
2021
Publisher :
American Society of Hematology, 2021.

Abstract

Neutrophils help to clear pathogens and cellular debris, but can also cause collateral damage within inflamed tissues. Prolonged neutrophil residency within an inflammatory niche can exacerbate tissue pathology. Using both genetic and pharmacological approaches, we show that BCL-XL is required for the persistence of neutrophils within inflammatory sites in mice. We demonstrate that a selective BCL-XL inhibitor (A-1331852) has therapeutic potential by causing apoptosis in inflammatory human neutrophils ex vivo. Moreover, in murine models of acute and chronic inflammatory disease, it reduced inflammatory neutrophil numbers and ameliorated tissue pathology. In contrast, there was minimal effect on circulating neutrophils. Thus, we show a differential survival requirement in activated neutrophils for BCL-XL and reveal a new therapeutic approach to neutrophil-mediated diseases.

Details

Language :
English
Database :
OpenAIRE
Journal :
Blood Adv
Accession number :
edsair.doi.dedup.....ebdaa032d6d3dbd2b6325707daeeec77