Impaired upper respiratory tract barrier function during postnatal development predisposes to invasive pneumococcal disease.
Kristen L Lokken-ToyliSurya D AggarwalGavyn Chern Wei BeeWouter A A de Steenhuijsen PitersCindy WuKenny Zhi Ming ChenCynthia LoomisDebby BogaertJeffrey N WeiserPublished in: PLoS pathogens (2024)
Infants are highly susceptible to invasive respiratory and gastrointestinal infections. To elucidate the age-dependent mechanism(s) that drive bacterial spread from the mucosa, we developed an infant mouse model using the prevalent pediatric respiratory pathogen, Streptococcus pneumoniae (Spn). Despite similar upper respiratory tract (URT) colonization levels, the survival rate of Spn-infected infant mice was significantly decreased compared to adults and corresponded with Spn dissemination to the bloodstream. An increased rate of pneumococcal bacteremia in early life beyond the newborn period was attributed to increased bacterial translocation across the URT barrier. Bacterial dissemination in infant mice was independent of URT monocyte or neutrophil infiltration, phagocyte-derived ROS or RNS, inflammation mediated by toll-like receptor 2 or interleukin 1 receptor signaling, or the pore-forming toxin pneumolysin. Using molecular barcoding of Spn, we found that only a minority of bacterial clones in the nasopharynx disseminated to the blood in infant mice, indicating the absence of robust URT barrier breakdown. Rather, transcriptional profiling of the URT epithelium revealed a failure of infant mice to upregulate genes involved in the tight junction pathway. Expression of many such genes was also decreased in early life in humans. Infant mice also showed increased URT barrier permeability and delayed mucociliary clearance during the first two weeks of life, which corresponded with tighter attachment of bacteria to the respiratory epithelium. Together, these results demonstrate a window of vulnerability during postnatal development when altered mucosal barrier function facilitates bacterial dissemination.
Keyphrases
- respiratory tract
- early life
- toll like receptor
- high fat diet induced
- mouse model
- immune response
- escherichia coli
- inflammatory response
- preterm infants
- oxidative stress
- poor prognosis
- cell death
- insulin resistance
- endothelial cells
- metabolic syndrome
- dna damage
- single cell
- dendritic cells
- skeletal muscle
- reactive oxygen species
- ulcerative colitis