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

Artigo Acesso aberto Revisado por pares

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

2013; Cell Press; Volume: 14; Issue: 5 Linguagem: Inglês

10.1016/j.chom.2013.10.004

ISSN

1934-6069

Autores

Julia Cahenzli, Yasmin Köller, Madeleine Wyss, Markus B. Geuking, Kathy D. McCoy,

Tópico(s)

Immune Cell Function and Interaction

Resumo

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.

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