Immune Dysregulation in Children With Down Syndrome

Dean Huggard; Dean Huggard; Dean Huggard; Dean Huggard; Derek G. Doherty; Derek G. Doherty; Eleanor J. Molloy; Eleanor J. Molloy; Eleanor J. Molloy; Eleanor J. Molloy; Eleanor J. Molloy

doi:10.3389/fped.2020.00073

Frontiers in Pediatrics (Feb 2020)

Immune Dysregulation in Children With Down Syndrome

Dean Huggard,
Dean Huggard,
Dean Huggard,
Dean Huggard,
Derek G. Doherty,
Derek G. Doherty,
Eleanor J. Molloy,
Eleanor J. Molloy,
Eleanor J. Molloy,
Eleanor J. Molloy,
Eleanor J. Molloy

Affiliations

Dean Huggard: Paediatrics, Trinity College, The University of Dublin, Dublin, Ireland
Dean Huggard: Trinity Translational Medicine Institute (TTMI), Trinity College Dublin, Dublin, Ireland
Dean Huggard: Paediatrics, Children's Hospital Ireland at Crumlin and Tallaght, Dublin, Ireland
Dean Huggard: National Children's Research Centre Dublin, Dublin, Ireland
Derek G. Doherty: Paediatrics, Trinity College, The University of Dublin, Dublin, Ireland
Derek G. Doherty: Trinity Translational Medicine Institute (TTMI), Trinity College Dublin, Dublin, Ireland
Eleanor J. Molloy: Paediatrics, Trinity College, The University of Dublin, Dublin, Ireland
Eleanor J. Molloy: Trinity Translational Medicine Institute (TTMI), Trinity College Dublin, Dublin, Ireland
Eleanor J. Molloy: Paediatrics, Children's Hospital Ireland at Crumlin and Tallaght, Dublin, Ireland
Eleanor J. Molloy: National Children's Research Centre Dublin, Dublin, Ireland
Eleanor J. Molloy: Coombe Women and Infants University Hospital, Dublin, Ireland

DOI: https://doi.org/10.3389/fped.2020.00073
Journal volume & issue: Vol. 8

Abstract

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Down syndrome (DS) is the most common genetic syndrome associated with immune defects. The extent of immune dysregulation in DS is substantial, spanning the innate and adaptive systems and including anomalies in: T and B cells, monocytes, neutrophil chemotaxis, circulating cytokines, and suboptimal antibody responses which all contribute to an increased risk of infections, poorer clinical outcomes and chronic inflammation in this vulnerable cohort. Other aspects of innate immunity may also be abnormal and contribute to the increased morbidity and warrant further interrogation such as: gamma delta T cell function, the inflammasome, Toll-like receptors and their pathways. Pharmacotherapies such as pavilizumab, pneumococcal and influenza immunizations, as well as potential immunoprophylactic agents such as pidotimod, azithromycin and Broncho-Vaxom may help alleviate the infectious consequences. Children with DS need to be managed with a heightened sense of awareness and urgency in the setting of sepsis and signs of chronic inflammation need regular screening and appropriate follow up.

Published in Frontiers in Pediatrics

ISSN: 2296-2360 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Pediatrics
Website: http://journal.frontiersin.org/journal/pediatrics

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Abstract

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