Abstract

Intrauterine growth restriction (IUGR) is a relevant predictor for higher rates of neonatal sepsis worldwide and is associated with an impaired neonatal immunity and lower immune cell counts. During the perinatal period, the liver is a key immunological organ responsible for the nuclear factor kappa B (NF-κB)-mediated innate immune response to inflammatory stimuli, but whether this role is affected by IUGR is unknown. Herein, we hypothesized that the newborn liver adapts to calorie-restriction IUGR by inducing changes in the NF-κB signaling transcriptome, leading to an attenuated acute proinflammatory response to intraperitoneal lipopolysaccharide (LPS). We first assessed the hepatic gene expression of key NF-κB factors in the IUGR and normally grown (NG) newborn mice. Real-time quantitative PCR (RT-qPCR) analysis revealed an upregulation of both IκB proteins genes (Nfkbia and Nfkbib) and the NF-κB subunit Nfkb1 in IUGR vs. NG. We next measured the LPS-induced hepatic expression of acute proinflammatory genes (Ccl3, Cxcl1, Il1b, Il6, and Tnf) and observed that the IUGR liver produced an attenuated acute proinflammatory cytokine gene response (Il1b and Tnf) to LPS in IUGR vs. unexposed (CTR). Consistent with these results, LPS-exposed hepatic tumor necrosis factor alpha (TNF-α) protein concentrations were lower in IUGR vs. LPS-exposed NG and did not differ from IUGR CTR. Sex differences at the transcriptome level were observed in the IUGR male vs. female. Our results demonstrate that IUGR induces key modifications in the NF-κB transcriptomic machinery in the newborn that compromised the acute proinflammatory cytokine gene and protein response to LPS. Our results bring novel insights in understanding how the IUGR newborn is immunocompromised due to fundamental changes in NF-κB key factors.

Highlights

  • Worldwide, intrauterine growth restriction (IUGR) affects approximately 10% of all newborns [1]

  • Average litter weight at E18.5 was significantly reduced in both IUGR male and female fetuses compared to normally grown (NG) (p < 0.001)

  • Similar differences continued in both IUGR male and female P0 neonatal mice compared to NG (p < 0.001)

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Summary

Introduction

Intrauterine growth restriction (IUGR) affects approximately 10% of all newborns [1]. Nuclear factor kappa B (NF-kB) signaling has a protective key role as a regulator of the acute phase innate immune response and immune organ development [15]. Recent studies have linked the NF-kB innate immune transcriptome to multiple factors that control nutrient metabolism, cell survival, and organ development [19,20,21]. These same pathways are severely affected in target organs in the growth-restricted fetus and neonate, including the liver [22,23,24,25]

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