Abstract
AbstractPolymorphonuclear neutrophils (PMNs) can differentiate into distinct states, which can either exacerbate or resolve inflammation. Our study shows that mice challenged with TLR agonists exhibited PMN differentiation along two major paths characterized by the expression of CCR5 or PD-L1. Similar differentiation was observed in the blood of severe COVID-19 patients and the synovial fluid of osteoarthritis patients. Prolongedin vitropriming of human PMNs modeled the differentiation paths. Actin disassembly favored CCR5 upregulation, while NF-kB activation stabilized the actin cytoskeleton and suppressed the development of CCR5+PMNs. Additionally, PD-L1 upregulation was triggered by STAT3 signaling and NF-kB activation. Functionally, CCR5 expressing PMNs were pro-NETotic, while PD-L1+PMNs showed immunosuppressive functions by inhibiting T cell proliferation via PD1. Together, PMN differentiation depended on the priming conditions, and the balance between actin disassembly and NF-kB/STAT3 activation translated the present micro-milieu into phenotypic and functional diversification of PMNs.SynopsisNeutrophils underwent phenotypical and functional diversification bothin vivoandin vitro. Actin disassembly led to the generation of CCR5highneutrophils with increased spontaneous NETosis, whereas NF-kB and STAT3 induced PD-L1 expression with T-cell suppressive properties as a deviation from the default pathway.PMN of mice challenged with TLR agonists develop two distinct phenotypes, CCR5highand PD-L1high.CCR5 and PD-L1-defined neutrophil phenotypes were found in blood of patients with severe COVID-19 and in the synovial fluid of osteoarthritis patients.In vitropriming induced a similar bifurcation of PMN phenotypes marked by either CCR5 or PD-L1.Actin disassembly preceded canonical development of CCR5+PMN.NF-kB halted actin disassembly by LPL regulation.During neutrophil priming, STAT3 aided NF-kB in the expression of PD-L1.Graphical abstract
Publisher
Cold Spring Harbor Laboratory