Aged polymorphonuclear leukocytes cause fibrotic interstitial lung disease in the absence of regulation by B cells.
Jung Hwan KimJohn PodstawkaYuefei LouLu LiEsther K S LeeMaziar DivangahiBjörn PetriFrank R JirikMargaret M KellyBryan G YippPublished in: Nature immunology (2018)
Pulmonary immunity requires tight regulation, as interstitial inflammation can compromise gas exchange and lead to respiratory failure. Here we found a greater number of aged CD11bhiL-selectinloCXCR4+ polymorphonuclear leukocytes (PMNs) in lung vasculature than in the peripheral circulation. Using pulmonary intravital microscopy, we observed lung PMNs physically interacting with B cells via β2 integrins; this initiated neutrophil apoptosis, which led to macrophage-mediated clearance. Genetic deletion of B cells led to the accumulation of aged PMNs in the lungs without systemic inflammation, which caused pathological fibrotic interstitial lung disease that was attenuated by the adoptive transfer of B cells or depletion of PMNs. Thus, the lungs are an intermediary niche in the PMN lifecycle wherein aged PMNs are regulated by B cells, which restrains their potential to cause pulmonary pathology.
Keyphrases
- interstitial lung disease
- systemic sclerosis
- idiopathic pulmonary fibrosis
- pulmonary hypertension
- respiratory failure
- rheumatoid arthritis
- oxidative stress
- extracorporeal membrane oxygenation
- peripheral blood
- adipose tissue
- endoplasmic reticulum stress
- mechanical ventilation
- high resolution
- intensive care unit
- blood brain barrier
- stem cells
- copy number
- single molecule
- mesenchymal stem cells
- optical coherence tomography
- protein kinase
- dna methylation
- acute respiratory distress syndrome
- chemotherapy induced
- pi k akt