Traffic-emitted ultrafine particles disrupt macrophage efferocytosis and resolution of allergic lung inflammation
Ontology highlight
ABSTRACT: Background: Particulate matter (PM) in air pollution is a major
health concern. PM includes ultrafine particles (UFPs; PM0.1
and particles of <
_0.1 𝛍m), which can evoke lung inflammation.
However, the impact of UFPs on the resolution of lung
inflammation, a potentially important link to chronic
inflammatory diseases, remains to be determined.
Objective: We sought to investigate the impact of UFPs on the
resolution of allergic lung inflammation and to identify potential
therapeutic interventions to mitigate these effects.
Methods: UFPs were collected from urban Boston. Using a
mouse model, transient allergic lung inflammation was induced
by exposure to house dust mite. Mice were then exposed to
UFPs, and their inflammatory responses were assessed. The
therapeutic potential of a resolution agonist, resolvin D2 (RvD2;
7S,16R,17S-trihydroxy-4Z,8E,10Z,12E,14E,19Z-
docosahexaenoic acid), was also determined.
Results: UFP exposure impaired lung eosinophil clearance and
reduced macrophage efferocytosis, key processes in resolving
lung inflammation. This disruption was mediated by altered
expression of ecto-5Ī„-nucleotidase (Nt5e, gene encoding for
CD73). Administration of RvD2, a potent proresolving
mediator, increased macrophage efferocytosis of apoptotic
eosinophils and neutrophils and partially corrected the
UFP-disrupted resolution mechanisms.
Conclusions: Environmental exposure to traffic-emitted UFPs
can fundamentally undermine endogenous resolution processes
—pathologic mechanisms that can be partially rescued by
signaling pathways activated by RvD2. (J Allergy Clin Immunol
2026;157:238-52.)
ORGANISM(S): Mus musculus (mouse)
SUBMITTER: Robert Nshimiyimana
PROVIDER: S-BSST2110 | biostudies-other |
REPOSITORIES: biostudies-other
ACCESS DATA