Compartmentalized gut lymph node drainage dictates adaptive immune responses

免疫系统 淋巴结 淋巴系统 免疫耐受 获得性免疫系统 FOXP3型 T细胞 生物 免疫 抗原 炎症 淋巴 免疫学 医学 病理
作者
Daria Esterházy,Maria Cecília Campos Canesso,Luka Mesin,Paul Müller,Tiago B. R. Castro,Ainsley Lockhart,Mahmoud Eljalby,Ana Maria Caetano Faria,Daniel Mucida
出处
期刊:Nature [Nature Portfolio]
卷期号:569 (7754): 126-130 被引量:322
标识
DOI:10.1038/s41586-019-1125-3
摘要

The intestinal immune system has the challenging task of tolerating foreign nutrients and the commensal microbiome, while excluding or eliminating ingested pathogens. Failure of this balance leads to conditions such as inflammatory bowel diseases, food allergies and invasive gastrointestinal infections1. Multiple immune mechanisms are therefore in place to maintain tissue integrity, including balanced generation of effector T (TH) cells and FOXP3+ regulatory T (pTreg) cells, which mediate resistance to pathogens and regulate excessive immune activation, respectively1–4. The gut-draining lymph nodes (gLNs) are key sites for orchestrating adaptive immunity to luminal perturbations5–7. However, it is unclear how they simultaneously support tolerogenic and inflammatory reactions. Here we show that gLNs are immunologically specific to the functional gut segment that they drain. Stromal and dendritic cell gene signatures and polarization of T cells against the same luminal antigen differ between gLNs, with the proximal small intestine-draining gLNs preferentially giving rise to tolerogenic responses and the distal gLNs to pro-inflammatory T cell responses. This segregation permitted the targeting of distal gLNs for vaccination and the maintenance of duodenal pTreg cell induction during colonic infection. Conversely, the compartmentalized dichotomy was perturbed by surgical removal of select distal gLNs and duodenal infection, with effects on both lymphoid organ and tissue immune responses. Our findings reveal that the conflict between tolerogenic and inflammatory intestinal responses is in part resolved by discrete gLN drainage, and encourage antigen targeting to specific gut segments for therapeutic immune modulation. Immune responses in the gut and associated draining lymph nodes differ between tolerogenic and inflammatory depending on their anatomical location.
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