High expression levels of macrophage migration inhibitory factor sustain the innate immune responses of neonates

Thierry Roger; Anina Schneider; Manuela Weier; Fred C. G. J. Sweep; Didier Le Roy; Jürgen Bernhagen; Thierry Calandra; Eric Giannoni

doi:10.1073/pnas.1514018113

Edited by Richard Bucala, Yale University School of Medicine, New Haven, CT, and accepted by the Editorial Board January 11, 2016 (received for review July 17, 2015)

Significance

During pregnancy, high circulating levels of adenosine and prostaglandins reduce the ability of fetal immune cells to mount powerful proinflammatory responses. In contrast, newborns express 10-fold higher levels of the proinflammatory immune regulator migration inhibitory factor (MIF) compared with adults. MIF sustains cell activation and cytokine production and counterregulates adenosine and prostaglandin E2-mediated immunosuppression in newborn monocytes. Yet excessive MIF expression during an established infection worsens the outcome of newborn mice. Thus, we identify a unique role for MIF in regulating neonatal innate immune responses and propose that MIF has a protective role to reduce susceptibility to infection during the neonatal period but may favor uncontrolled inflammation during sepsis, leading to adverse outcomes.

Abstract

The vulnerability to infection of newborns is associated with a limited ability to mount efficient immune responses. High concentrations of adenosine and prostaglandins in the fetal and neonatal circulation hamper the antimicrobial responses of newborn immune cells. However, the existence of mechanisms counterbalancing neonatal immunosuppression has not been investigated. Remarkably, circulating levels of macrophage migration inhibitory factor (MIF), a proinflammatory immunoregulatory cytokine expressed constitutively, were 10-fold higher in newborns than in children and adults. Newborn monocytes expressed high levels of MIF and released MIF upon stimulation with Escherichia coli and group B Streptococcus, the leading pathogens of early-onset neonatal sepsis. Inhibition of MIF activity or MIF expression reduced microbial product-induced phosphorylation of p38 and ERK1/2 mitogen-activated protein kinases and secretion of cytokines. Recombinant MIF used at newborn, but not adult, concentrations counterregulated adenosine and prostaglandin E2-mediated inhibition of ERK1/2 activation and TNF production in newborn monocytes exposed to E. coli. In agreement with the concept that once infection is established high levels of MIF are detrimental to the host, treatment with a small molecule inhibitor of MIF reduced systemic inflammatory response, bacterial proliferation, and mortality of septic newborn mice. Altogether, these data provide a mechanistic explanation for how newborns may cope with an immunosuppressive environment to maintain a certain threshold of innate defenses. However, the same defense mechanisms may be at the expense of the host in conditions of severe infection, suggesting that MIF could represent a potential attractive target for immune-modulating adjunctive therapies for neonatal sepsis.

Footnotes

↵¹To whom correspondence should be addressed. Email: Eric.Giannoni{at}chuv.ch.

Author contributions: T.R., D.L.R., T.C., and E.G. designed research; T.R., A.S., M.W., D.L.R., and E.G. performed research; F.C.G.J.S. and J.B. contributed new reagents/analytic tools; T.R., A.S., M.W., T.C., and E.G. analyzed data; and T.R. and E.G. wrote the paper.
The authors declare no conflict of interest.
This article is a PNAS Direct Submission. R.B. is a guest editor invited by the Editorial Board.
This article contains supporting information online at www.pnas.org/lookup/suppl/doi:10.1073/pnas.1514018113/-/DCSupplemental.

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