Early-life Programming of Mesenteric Lymph Node Stromal Cell Identity by the Lymphotoxin Pathway Regulates Adult Mucosal Immunity

Overview

Journal Sci Immunol

Specialty Allergy & Immunology

Date 2019 Dec 22

PMID 31862865

Citations 16

Authors

Conglei Li

Evelyn Lam

Christian Perez-Shibayama

Lesley A Ward

Jianbo Zhang

Dennis Lee

Albert Nguyen

Musaddeque Ahmed

Emma Brownlie

Kirill V Korneev

Olga Rojas

Tian Sun

William Navarre

Housheng Hansen He

Shan Liao

Alberto Martin

Burkhard Ludewig

Jennifer L Gommerman

Affiliations

Soon will be listed here.

Abstract

Redundant mechanisms support immunoglobulin A (IgA) responses to intestinal antigens. These include multiple priming sites [mesenteric lymph nodes (MLNs), Peyer's patches, and isolated lymphoid follicles] and various cytokines that promote class switch to IgA, even in the absence of T cells. Despite these backup mechanisms, vaccination against enteric pathogens such as rotavirus has limited success in some populations. Genetic and environmental signals experienced during early life are known to influence mucosal immunity, yet the mechanisms for how these exposures operate remain unclear. Here, we used rotavirus infection to follow antigen-specific IgA responses through time and in different gut compartments. Using genetic and pharmacological approaches, we tested the role of the lymphotoxin (LT) pathway-known to support IgA responses-at different developmental stages. We found that LT-β receptor (LTβR) signaling in early life programs intestinal IgA responses in adulthood by affecting antibody class switch recombination to IgA and subsequent generation of IgA antibody-secreting cells within an intact MLN. In addition, early-life LTβR signaling dictates the phenotype and function of MLN stromal cells to support IgA responses in the adult. Collectively, our studies uncover new mechanistic insights into how early-life LTβR signaling affects mucosal immune responses during adulthood.

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