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  3. Using Precisely Defined in vivo Microbiotas to Understand Microbial Regulation of IgE.
 

Using Precisely Defined in vivo Microbiotas to Understand Microbial Regulation of IgE.

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BORIS DOI
10.7892/boris.149731
Publisher DOI
10.3389/fimmu.2019.03107
PubMed ID
32010146
Description
Early life exposure to microbes plays an important role in immune system development. Germ-free mice, or mice colonized with a low-diversity microbiota, exhibit high serum IgE levels. An increase in microbial richness, providing it occurs in a critical developmental window early in life, leads to inhibition of this hygiene-induced IgE. However, whether this inhibition is dependent solely on certain microbial species, or is an additive effect of microbial richness, remains to be determined. Here we report that mice colonized with a combination of bacterial species with specific characteristics is required to inhibit IgE levels. These defined characteristics include the presence in early life, acetate production and immunogenicity reflected by induction of IgA. Suppression of IgE did not correlate with production of the short chain fatty acids propionate and butyrate, or induction of peripherally induced Tregs in mucosal tissues. Thus, inhibition of IgE induction can be mediated by specific microbes and their associated metabolic pathways and immunogenic properties.
Date of Publication
2020
Publication Type
Article
Subject(s)
600 Technology > 610 Medicine & health
Keyword(s)
IgE SCFA Tregs gnotobiotic microbiota
Language(s)
en
Contributor(s)
Wyss, Madeleine
Brown, Kirsty
Thomson, Carolyn A
Koegler, Mia
Terra, Fernanda
Fan, Vina
Ronchi, Francesca
Department for BioMedical Research, Forschungsgruppe Gastroenterologie / Mukosale Immunologie
Bihan, Dominique
Lewis, Ian
Geuking, Markus B
McCoy, Kathy D
Additional Credits
Department for BioMedical Research, Forschungsgruppe Gastroenterologie / Mukosale Immunologie
Series
Frontiers in immunology
Publisher
Frontiers Research Foundation
ISSN
1664-3224
Access(Rights)
open.access
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