| Literature DB >> 27114524 |
James Lawrence Wynn1, Chris S Wilson2, Jacek Hawiger3, Philip O Scumpia4, Andrew F Marshall5, Jin-Hua Liu5, Irina Zharkikh6, Hector R Wong7, Patrick Lahni7, John T Benjamin5, Erin J Plosa5, Jörn-Hendrik Weitkamp5, Edward R Sherwood8, Lyle L Moldawer9, Ricardo Ungaro9, Henry V Baker10, M Cecilia Lopez10, Steven J McElroy11, Natacha Colliou12, Mansour Mohamadzadeh12, Daniel Jensen Moore13.
Abstract
Interleukin (IL)-18 is an important effector of innate and adaptive immunity, but its expression must also be tightly regulated because it can potentiate lethal systemic inflammation and death. Healthy and septic human neonates demonstrate elevated serum concentrations of IL-18 compared with adults. Thus, we determined the contribution of IL-18 to lethality and its mechanism in a murine model of neonatal sepsis. We find that IL-18-null neonatal mice are highly protected from polymicrobial sepsis, whereas replenishing IL-18 increased lethality to sepsis or endotoxemia. Increased lethality depended on IL-1 receptor 1 (IL-1R1) signaling but not adaptive immunity. In genome-wide analyses of blood mRNA from septic human neonates, expression of the IL-17 receptor emerged as a critical regulatory node. Indeed, IL-18 administration in sepsis increased IL-17A production by murine intestinal γδT cells as well as Ly6G(+) myeloid cells, and blocking IL-17A reduced IL-18-potentiated mortality to both neonatal sepsis and endotoxemia. We conclude that IL-17A is a previously unrecognized effector of IL-18-mediated injury in neonatal sepsis and that disruption of the deleterious and tissue-destructive IL-18/IL-1/IL-17A axis represents a novel therapeutic approach to improve outcomes for human neonates with sepsis.Entities:
Keywords: IL-17; IL-18; neonate; pathogenesis; sepsis
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Year: 2016 PMID: 27114524 PMCID: PMC4868456 DOI: 10.1073/pnas.1515793113
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205