Literature DB >> 30171870

Immune and metabolic shifts during neonatal development reprogram liver identity and function.

Brenda Naemi Nakagaki1, Kassiana Mafra1, Érika de Carvalho1, Mateus Eustáquio Lopes1, Raquel Carvalho-Gontijo1, Hortência Maciel de Castro-Oliveira1, Gabriel Henrique Campolina-Silva2, Camila Dutra Moreira de Miranda1, Maísa Mota Antunes1, Ana Carolina Carvalho Silva1, Ariane Barros Diniz1, Débora Moreira Alvarenga1, Maria Alice Freitas Lopes1, Viviane Aparecida de Souza Lacerda1, Matheus Silvério Mattos1, Alan Moreira Araújo1, Paula Vieira Teixeira Vidigal3, Cristiano Xavier Lima4, Germán A B Mahecha2, Mila Fernandes Moreira Madeira5, Gabriel Rocha Fernandes6, Raquel Ferraz Nogueira7, Thais Garcias Moreira8, Bruna Araújo David9, Rafael Machado Rezende8, Gustavo Batista Menezes10.   

Abstract

BACKGROUND & AIMS: The liver is the main hematopoietic site in embryos, becoming a crucial organ in both immunity and metabolism in adults. However, how the liver adapts both the immune system and enzymatic profile to challenges in the postnatal period remains elusive. We aimed to identify the mechanisms underlying this adaptation.
METHODS: We analyzed liver samples from mice on day 0 after birth until adulthood. Human biopsies from newborns and adults were also examined. Liver immune cells were phenotyped using mass cytometry (CyTOF) and expression of several genes belonging to immune and metabolic pathways were measured. Mortality rate, bacteremia and hepatic bacterial retention after E. coli challenge were analyzed using intravital and in vitro approaches. In a set of experiments, mice were prematurely weaned and the impact on gene expression of metabolic pathways was evaluated.
RESULTS: Human and mouse newborns have a sharply different hepatic cellular composition and arrangement compared to adults. We also found that myeloid cells and immature B cells primarily compose the neonatal hepatic immune system. Although neonatal mice were more susceptible to infections, a rapid evolution to an efficient immune response was observed. Concomitantly, newborns displayed a reduction of several macronutrient metabolic functions and the normal expression level of enzymes belonging to lipid and carbohydrate metabolism was reached around the weaning period. Interestingly, early weaning profoundly disturbed the expression of several hepatic metabolic pathways, providing novel insights into how dietary schemes affect the metabolic maturation of the liver.
CONCLUSION: In newborns, the immune and metabolic profiles of the liver are dramatically different to those of the adult liver, which can be explained by the differences in the liver cell repertoire and phenotype. Also, dietary and antigen cues may be crucial to guide liver development during the postnatal phase. LAY
SUMMARY: Newborns face major challenges in the extra-uterine life. In fact, organs need to modify their cellular composition and gene expression profile in order to adapt to changes in both microbiota and diet throughout life. The liver is interposed between the gastrointestinal system and the systemic circulation, being the destination of all macronutrients and microbial products from the gut. Therefore, it is expected that delicately balanced mechanisms govern the transformation of a neonatal liver to a key organ in adults.
Copyright © 2018 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Diet; Early weaning; Immune system; Immunity; In vivo imaging; Metabolism; Newborn

Year:  2018        PMID: 30171870     DOI: 10.1016/j.jhep.2018.08.018

Source DB:  PubMed          Journal:  J Hepatol        ISSN: 0168-8278            Impact factor:   25.083


  11 in total

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