| Literature DB >> 33741905 |
Utsa Karmakar1, Julia Y Chu1, Kruthika Sundaram1, Anne L Astier1,2, Hannah Garside1, Carsten G Hansen1, Ian Dransfield1, Sonja Vermeren3.
Abstract
Persistent neutrophilic inflammation drives host damage in autoimmune diseases that are characterized by abundant immune complexes. Insoluble immune complexes (iICs) potently activate pro-inflammatory neutrophil effector functions. We and others have shown that iICs also promote resolution of inflammation via stimulation of neutrophil apoptosis. We demonstrate here that iICs trigger FcγRIIa-dependent neutrophil macropinocytosis, leading to the rapid uptake, and subsequent degradation of iICs. We provide evidence that concurrent iIC-induced neutrophil apoptosis is distinct from phagocytosis-induced cell death. First, uptake of iICs occurs by FcγRII-stimulated macropinocytosis, rather than phagocytosis. Second, production of reactive oxygen species, but not iIC-internalization is a pre-requisite for iIC-induced neutrophil apoptosis. Our findings identify a previously unknown mechanism by which neutrophils can remove pro-inflammatory iICs from the circulation. Together iIC clearance and iIC-induced neutrophil apoptosis may act to prevent the potential escalation of neutrophilic inflammation in response to iICs.Entities:
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Year: 2021 PMID: 33741905 PMCID: PMC7979711 DOI: 10.1038/s41419-021-03528-8
Source DB: PubMed Journal: Cell Death Dis Impact factor: 8.469