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Age, microbiota, and T cells shape diverse individual IgA repertoires in the intestine

Authors :
Oliver Pabst
Sebastian Suerbaum
Andrew J. Macpherson
Lisa Föhse
Immo Prinz
Benjamin Wahl
Cornelia Lindner
Source :
The Journal of experimental medicine, The Journal of Experimental Medicine, Journal of experimental medicine : JEM 209(2), 365-377 (2012). doi:10.1084/jem.20111980
Publication Year :
2012

Abstract

High-throughput sequencing reveals stability of the intestinal IgA repertoire after plasma cell depletion and changes in repertoire diversity with age and microbial colonization.<br />Intestinal immunoglobulin A (IgA) ensures host defense and symbiosis with our commensal microbiota. Yet previous studies hint at a surprisingly low diversity of intestinal IgA, and it is unknown to what extent the diverse Ig arsenal generated by somatic recombination and diversification is actually used. In this study, we analyze more than one million mouse IgA sequences to describe the shaping of the intestinal IgA repertoire, its determinants, and stability over time. We show that expanded and infrequent clones combine to form highly diverse polyclonal IgA repertoires with very little overlap between individual mice. Selective homing allows expanded clones to evenly seed the small but not large intestine. Repertoire diversity increases during aging in a dual process. On the one hand, microbiota-, T cell–, and transcription factor RORγt–dependent but Peyer’s patch–independent somatic mutations drive the diversification of expanded clones, and on the other hand, new clones are introduced into the repertoire of aged mice. An individual’s IgA repertoire is stable and recalled after plasma cell depletion, which is indicative of functional memory. These data provide a conceptual framework to understand the dynamic changes in the IgA repertoires to match environmental and intrinsic stimuli.

Details

Volume :
209
Issue :
2
Database :
OpenAIRE
Journal :
The Journal of experimental medicine
Accession number :
edsair.doi.dedup.....ef5aef18bd15ad568cc0ea09099a6390
Full Text :
https://doi.org/10.1084/jem.20111980