Abstract
Background
The developmental immaturity of the innate immune system helps explains the increased risk of infection in the neonatal period. Importantly, innate immune signaling pathways such as p65/NFκB and c-Jun/AP1 are responsible for the prevention of hepatocyte apoptosis in adult animals, yet whether developmental immaturity of these pathways increases the risk of hepatic injury in the neonatal period is unknown.Methods
Using a murine model of endotoxemia (LPS 5 mg/kg IP x 1) in neonatal (P3) and adult mice, we evaluated histologic evidence of hepatic injury and apoptosis, presence of p65/NFκB and c-Jun/AP1 activation and associated transcriptional regulation of apoptotic genes.Results
We demonstrate that in contrast to adults, endotoxemic neonatal (P3) mice exhibit a significant increase in hepatic apoptosis. This is associated with absent hepatic p65/NFκB signaling and impaired expression of anti-apoptotic target genes. Hepatic c-Jun/AP1 activity was attenuated in endotoxemic P3 mice, with resulting upregulation of pro-apoptotic factors.Conclusions
These results demonstrate that developmental absence of innate immune p65/NFκB and c-Jun/AP1 signaling, and target gene expression is associated with apoptotic injury in neonatal mice. More work is needed to determine if this contributes to long-term hepatic dysfunction, and whether immunomodulatory approaches can prevent this injury.Impact
Various aspects of developmental immaturity of the innate immune system may help explain the increased risk of infection in the neonatal period. In adult models of inflammation and infection, innate immune signaling pathways such as p65/NFκB and c-Jun/AP1 are responsible for a protective, pro-inflammatory transcriptome and regulation of apoptosis. We demonstrate that in contrast to adults, endotoxemic neonatal (P3) mice exhibit a significant increase in hepatic apoptosis associated with absent hepatic p65/NFκB signaling and c-Jun/AP1 activity. We believe that these results may explain in part hepatic dysfunction with neonatal sepsis, and that there may be unrecognized developmental and long-term hepatic implications of early life exposure to systemic inflammatory stress.References
Articles referenced by this article (98)
The global burden of paediatric and neonatal sepsis: a systematic review.
Lancet Respir Med, (3):223-230 2018
MED: 29508706
Impact of sepsis on neurodevelopmental outcome in a Swiss National Cohort of extremely premature infants.
Pediatrics, (2):e348-57 2011
MED: 21768312
Protecting the Newborn and Young Infant from Infectious Diseases: Lessons from Immune Ontogeny.
Immunity, (3):350-363 2017
MED: 28329702
Immaturity of infection control in preterm and term newborns is associated with impaired toll-like receptor signaling.
J Infect Dis, (2):296-302 2006
MED: 17191175
High expression levels of macrophage migration inhibitory factor sustain the innate immune responses of neonates.
Proc Natl Acad Sci U S A, (8):E997-1005 2016
MED: 26858459
A prime time for trained immunity: innate immune memory in newborns and infants.
Neonatology, (2):136-141 2013
MED: 24356292
Innate immunity of the newborn: basic mechanisms and clinical correlates.
Nat Rev Immunol, (5):379-390 2007
MED: 17457344
Innate immunity in human newborn infants: prematurity means more than immaturity.
J Matern Fetal Neonatal Med, (1):25-31 2010
MED: 20569168
Show 10 more references (10 of 98)
Citations & impact
Impact metrics
Article citations
Sex Differences in Hepatic Inflammation, Lipid Metabolism, and Mitochondrial Function Following Early Lipopolysaccharide Exposure in Epileptic WAG/Rij Rats.
Antioxidants (Basel), 13(8):957, 07 Aug 2024
Cited by: 0 articles | PMID: 39199203 | PMCID: PMC11351225
Similar Articles
To arrive at the top five similar articles we use a word-weighted algorithm to compare words from the Title and Abstract of each citation.
Immunotolerant p50/NFκB Signaling and Attenuated Hepatic IFNβ Expression Increases Neonatal Sensitivity to Endotoxemia.
Front Immunol, 9:2210, 26 Sep 2018
Cited by: 6 articles | PMID: 30319651 | PMCID: PMC6168645
Maturation of the Acute Hepatic TLR4/NF-κB Mediated Innate Immune Response Is p65 Dependent in Mice.
Front Immunol, 11:1892, 21 Aug 2020
Cited by: 7 articles | PMID: 32973783 | PMCID: PMC7472845
Perinatal Endotoxemia Induces Sustained Hepatic COX-2 Expression through an NFκB-Dependent Mechanism.
J Innate Immun, 8(4):386-399, 29 Apr 2016
Cited by: 9 articles | PMID: 27160391 | PMCID: PMC5761660
Developmentally Regulated Innate Immune NFκB Signaling Mediates IL-1α Expression in the Perinatal Murine Lung.
Front Immunol, 10:1555, 10 Jul 2019
Cited by: 6 articles | PMID: 31354715 | PMCID: PMC6637303
