In this issue of Blood, Aksoy and colleagues contribute to the understanding of remarkable immunoregulatory controls at the time of birth by showing that impaired synthesis of interferon-β (IFNβ) and IFN-inducible factors elicited by lipopolysaccharide (LPS) depends on the transcriptional activity of interferon regulatory factor 3 (IRF-3) downstream of Toll-like receptor-4 (TLR4).
The human newborn is profoundly susceptible to intracellular bacterial pathogens that require Th1-dependent host defense pathways for eradication. The molecular basis for the newborn's attenuated response to such infections remains a mystery but is likely a consequence of the immunosuppression required for survival in utero.
In this article, Aksoy and colleagues show that an impaired response of monocyte-derived dendritic cells (moDCs) from newborns to LPS (at concentrations that occur during bacterial sepsis) depends on transcriptional activity downstream of Toll-like receptor 4 (TLR4) that is independent of myeloid differentiation factor 88 (MyD88). In addition, LPS fails to induce synthesis of IFNβ in cord blood at levels that are clearly detected in adult blood. In line with this seminal observation, the induction of CXCL10—a prototypic IFN-dependent gene—was diminished in cord blood. In contrast, induction of IL-1β and IL-6 mRNA by LPS is comparable in cord and adult blood. Specificity of this deficiency was shown by demonstrating that genes that depend on MyD88 (NF-κB activation) were similar after LPS stimulation for adult and newborn moDCs.
The authors also demonstrate that LPS-induced translocation of interferon regulatory factor 3 (IRF-3) to the nucleus occurred in both adult and neonatal moDCs. However, IRF-3 DNA binding to the coactivator CREB-binding protein (CBP) was decreased in neonatal compared with adult moDCs. The authors concluded that deficient IRF-3/CBP interaction in LPS-stimulated neonatal moDCs may reduce their ability to elicit Th1 responses. The findings are relevant to our understanding of immunosuppression in utero and in early life but have not been tested in an in vivo experimental model. The timing and the processes involved in the transition to mature form of immunity remain areas for further discovery.
The author declares no competing financial interests. ▪
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