Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age

Neonatal pain-related stress is associated with elevated salivary cortisol levels to age 18 months in children born very preterm, compared to full-term, suggesting early programming effects. Importantly, interactions between immune/inflammatory and neuroendocrine systems may underlie programming eff...

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Autores principales: Grunau, Ruth E., Cepeda, Ivan L., Chau, Cecil M. Y., Brummelte, Susanne, Weinberg, Joanne, Lavoie, Pascal M., Ladd, Mihoko, Hirschfeld, Aaron F., Russell, Evan, Koren, Gideon, Van Uum, Stan, Brant, Rollin, Turvey, Stuart E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3774765/
https://www.ncbi.nlm.nih.gov/pubmed/24066085
http://dx.doi.org/10.1371/journal.pone.0073926
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author Grunau, Ruth E.
Cepeda, Ivan L.
Chau, Cecil M. Y.
Brummelte, Susanne
Weinberg, Joanne
Lavoie, Pascal M.
Ladd, Mihoko
Hirschfeld, Aaron F.
Russell, Evan
Koren, Gideon
Van Uum, Stan
Brant, Rollin
Turvey, Stuart E.
author_facet Grunau, Ruth E.
Cepeda, Ivan L.
Chau, Cecil M. Y.
Brummelte, Susanne
Weinberg, Joanne
Lavoie, Pascal M.
Ladd, Mihoko
Hirschfeld, Aaron F.
Russell, Evan
Koren, Gideon
Van Uum, Stan
Brant, Rollin
Turvey, Stuart E.
author_sort Grunau, Ruth E.
collection PubMed
description Neonatal pain-related stress is associated with elevated salivary cortisol levels to age 18 months in children born very preterm, compared to full-term, suggesting early programming effects. Importantly, interactions between immune/inflammatory and neuroendocrine systems may underlie programming effects. We examined whether cortisol changes persist to school age, and if common genetic variants in the promoter region of the NFKBIA gene involved in regulation of immune and inflammatory responses, modify the association between early experience and later life stress as indexed by hair cortisol levels, which provide an integrated index of endogenous HPA axis activity. Cortisol was assayed in hair samples from 128 children (83 born preterm ≤32 weeks gestation and 45 born full-term) without major sensory, motor or cognitive impairments at age 7 years. We found that hair cortisol levels were lower in preterm compared to term-born children. Downregulation of the HPA axis in preterm children without major impairment, seen years after neonatal stress terminated, suggests persistent alteration of stress system programming. Importantly, the etiology was gender-specific such that in preterm boys but not girls, specifically those with the minor allele for NFKBIA rs2233409, lower hair cortisol was associated with greater neonatal pain (number of skin-breaking procedures from birth to term), independent of medical confounders. Moreover, the minor allele (CT or TT) of NFKBIA rs2233409 was associated with higher secretion of inflammatory cytokines, supporting the hypothesis that neonatal pain-related stress may act as a proinflammatory stimulus that induces long-term immune cell activation. These findings are the first evidence that a long-term association between early pain-related stress and cortisol may be mediated by a genetic variants that regulate the activity of NF-κB, suggesting possible involvement of stress/inflammatory mechanisms in HPA programming in boys born very preterm.
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spelling pubmed-37747652013-09-24 Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age Grunau, Ruth E. Cepeda, Ivan L. Chau, Cecil M. Y. Brummelte, Susanne Weinberg, Joanne Lavoie, Pascal M. Ladd, Mihoko Hirschfeld, Aaron F. Russell, Evan Koren, Gideon Van Uum, Stan Brant, Rollin Turvey, Stuart E. PLoS One Research Article Neonatal pain-related stress is associated with elevated salivary cortisol levels to age 18 months in children born very preterm, compared to full-term, suggesting early programming effects. Importantly, interactions between immune/inflammatory and neuroendocrine systems may underlie programming effects. We examined whether cortisol changes persist to school age, and if common genetic variants in the promoter region of the NFKBIA gene involved in regulation of immune and inflammatory responses, modify the association between early experience and later life stress as indexed by hair cortisol levels, which provide an integrated index of endogenous HPA axis activity. Cortisol was assayed in hair samples from 128 children (83 born preterm ≤32 weeks gestation and 45 born full-term) without major sensory, motor or cognitive impairments at age 7 years. We found that hair cortisol levels were lower in preterm compared to term-born children. Downregulation of the HPA axis in preterm children without major impairment, seen years after neonatal stress terminated, suggests persistent alteration of stress system programming. Importantly, the etiology was gender-specific such that in preterm boys but not girls, specifically those with the minor allele for NFKBIA rs2233409, lower hair cortisol was associated with greater neonatal pain (number of skin-breaking procedures from birth to term), independent of medical confounders. Moreover, the minor allele (CT or TT) of NFKBIA rs2233409 was associated with higher secretion of inflammatory cytokines, supporting the hypothesis that neonatal pain-related stress may act as a proinflammatory stimulus that induces long-term immune cell activation. These findings are the first evidence that a long-term association between early pain-related stress and cortisol may be mediated by a genetic variants that regulate the activity of NF-κB, suggesting possible involvement of stress/inflammatory mechanisms in HPA programming in boys born very preterm. Public Library of Science 2013-09-16 /pmc/articles/PMC3774765/ /pubmed/24066085 http://dx.doi.org/10.1371/journal.pone.0073926 Text en © 2013 Grunau et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Grunau, Ruth E.
Cepeda, Ivan L.
Chau, Cecil M. Y.
Brummelte, Susanne
Weinberg, Joanne
Lavoie, Pascal M.
Ladd, Mihoko
Hirschfeld, Aaron F.
Russell, Evan
Koren, Gideon
Van Uum, Stan
Brant, Rollin
Turvey, Stuart E.
Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title_full Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title_fullStr Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title_full_unstemmed Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title_short Neonatal Pain-Related Stress and NFKBIA Genotype Are Associated with Altered Cortisol Levels in Preterm Boys at School Age
title_sort neonatal pain-related stress and nfkbia genotype are associated with altered cortisol levels in preterm boys at school age
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3774765/
https://www.ncbi.nlm.nih.gov/pubmed/24066085
http://dx.doi.org/10.1371/journal.pone.0073926
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