Intestinal Microbial Diversity during Early-Life Colonization Shapes Long-Term IgE Levels

Microbial exposure following birth profoundly impacts mammalian immune system development. Microbiota alterations are associated with increased incidence of allergic and autoimmune disorders with elevated serum IgE as a hallmark. The previously reported abnormally high serum IgE levels in germ-free...

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Veröffentlicht in:Cell host & microbe 2013-11, Vol.14 (5), p.559-570
Hauptverfasser: Cahenzli, Julia, Köller, Yasmin, Wyss, Madeleine, Geuking, Markus B., McCoy, Kathy D.
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Sprache:eng
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Zusammenfassung:Microbial exposure following birth profoundly impacts mammalian immune system development. Microbiota alterations are associated with increased incidence of allergic and autoimmune disorders with elevated serum IgE as a hallmark. The previously reported abnormally high serum IgE levels in germ-free mice suggests that immunoregulatory signals from microbiota are required to control basal IgE levels. We report that germ-free mice and those with low-diversity microbiota develop elevated serum IgE levels in early life. B cells in neonatal germ-free mice undergo isotype switching to IgE at mucosal sites in a CD4 T-cell- and IL-4-dependent manner. A critical level of microbial diversity following birth is required in order to inhibit IgE induction. Elevated IgE levels in germ-free mice lead to increased mast-cell-surface-bound IgE and exaggerated oral-induced systemic anaphylaxis. Thus, appropriate intestinal microbial stimuli during early life are critical for inducing an immunoregulatory network that protects from induction of IgE at mucosal sites. [Display omitted] •Germ-free and mice with low-diversity microbiota develop high serum IgE levels•B cells in germ-free mice undergo IgE class switch recombination at mucosal sites•A diverse microbiota early in life is required to inhibit IgE induction•Hyper IgE in germ-free mice leads to exaggerated oral-induced systemic anaphylaxis
ISSN:1931-3128
1934-6069
DOI:10.1016/j.chom.2013.10.004