Dual neutrophil subsets exacerbate or suppress inflammation in tuberculosis via IL-1β or PD-L1.
Emilie Doz-DeblauweBadreddine BounabFlorence CarrerasJulia S FahelSergio C OliveiraMohamed LamkanfiYves Le VernPierre GermonJulien PichonFlorent KempfChristophe PagetAude RemotNathalie WinterPublished in: Life science alliance (2024)
Neutrophils can be beneficial or deleterious during tuberculosis (TB). Based on the expression of MHC-II and programmed death ligand 1 (PD-L1), we distinguished two functionally and transcriptionally distinct neutrophil subsets in the lungs of mice infected with mycobacteria. Inflammatory [MHC-II - , PD-L1 lo ] neutrophils produced inflammasome-dependent IL-1β in the lungs in response to virulent mycobacteria and "accelerated" deleterious inflammation, which was highly exacerbated in IFN-γR -/- mice. Regulatory [MHC-II + , PD-L1 hi ] neutrophils "brake" inflammation by suppressing T-cell proliferation and IFN-γ production. Such beneficial regulation, which depends on PD-L1, is controlled by IFN-γR signaling in neutrophils. The hypervirulent HN878 strain from the Beijing genotype curbed PD-L1 expression by regulatory neutrophils, abolishing the braking function and driving deleterious hyperinflammation in the lungs. These findings add a layer of complexity to the roles played by neutrophils in TB and may explain the reactivation of this disease observed in cancer patients treated with anti-PD-L1.
Keyphrases
- oxidative stress
- mycobacterium tuberculosis
- cell proliferation
- immune response
- poor prognosis
- squamous cell carcinoma
- high fat diet induced
- air pollution
- emergency department
- type diabetes
- binding protein
- metabolic syndrome
- long non coding rna
- papillary thyroid
- hiv aids
- hiv infected
- young adults
- adverse drug
- human immunodeficiency virus
- klebsiella pneumoniae
- wild type