Becky Adkins scite author profile

Immunity in the newborn is characterized by minimal Th1 function but an excess of Th2 activity. Since Th1 lymphocytes are important to counter microbes and Th2 cells favor allergies, the newborn faces susceptibility to microbial infections and allergic reactions. Delayed maturation of certain dendritic cells leads to limited IL-12 production during the neonatal period. The Th2 cytokine locus of neonatal CD4+ T cells is epigenetically poised for rapid and robust production of IL-4 and IL-13. Together, these circumstances lead to efficient differentiation of Th2 cells and the expression of an IL-4Rα/IL-13Rα1 heteroreceptor on Th1 cells. Upon rechallenge, Th2 cells rapidly produce IL-4 which utilizes the heteroreceptor to drive apoptosis of Th1 cells yielding the Th2 bias of neonatal immunity.

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Essential role of TNF receptor superfamily 25 (TNFRSF25) in the development of allergic lung inflammation

Fang

et al. 2008

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T-cell function in newborn mice and humans

1999

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Becky Adkins

Neonatal adaptive immunity comes of age

Challenges in infant immunity: implications for responses to infection and vaccines

Neonatal immunity: faulty T-helpers and the shortcomings of dendritic cells

Essential role of TNF receptor superfamily 25 (TNFRSF25) in the development of allergic lung inflammation

T-cell function in newborn mice and humans

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