Maternal Immunoglobulin A regulates the development of the neonatal microbiota and intestinal microbiota-specific CD4+ T cell responses

Author:

Abbott Darryl A.ORCID,Rai Ali T.,Yang Aaron,Cai Yixuan,Fabre Shelcie,Frazer Austin J.,Deschepper Jacob D.,Poholek Amanda C.,Hand Timothy W.

Abstract

AbstractBreast milk is a complex mixture of nutrients and bioactives that promote infant development and decrease the incidence of chronic inflammatory disease. We investigated the role of one milk-derived bioactive, Immunoglobulin A (IgA) on the developing small intestinal microbiota and immune system. We demonstrate that early in life, milk-derived IgA suppressed colonization of the small intestine byEnterobacteriaceaeand regulated the maturation of the small intestinal epithelium and the development of intestinal IL-17-producing CD4+T cells.Enterobacteriaceae- specific CD4+T cells, induced in the first weeks of life in the absence of milk-derived IgA, persisted in the intestine as memory T cells that can contribute to inflammatory disease later in life. Our study suggests that milk-derived IgA shapes mucosal immunity by regulating the neonatal microbiota thus preventing the development of long-lived intestinal microbiota-specific T cells.

Publisher

Cold Spring Harbor Laboratory

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