Innate immune system signaling and CD11b+CD11c+CD103+cell migration to the brain underlie changes in mouse behavior after microbial colonization-Reference-Cited by-同舟云学术

Innate immune system signaling and CD11b⁺CD11c⁺CD103⁺cell migration to the brain underlie changes in mouse behavior after microbial colonization

Published:2024-07-03 Issue: Volume: Page:
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Author:

Philip Vivek,Kraimi Narjis,Zhang Hailong,Lu Jun,De Palma Giada,Shimbori Chiko,McCoy Kathy D.,Hapfelmeier Siegfried,Schären Olivier P.,Macpherson Andrew J,Chirdo Fernando,Surette Michael G.,Verdu Elena F.,Liu Fang,Collins Stephen M,Bercik Premysl

Abstract

AbstractBackground and AimsAccumulating evidence suggests the microbiota is a key factor in disorders of gut-brain interaction (DGBI), by affecting host immune and neural systems. However, the underlying mechanisms remain elusive due to their complexity and clinical heterogeneity of patients with DGBIs. We aimed to identify neuroimmune pathways that are critical in microbiota-gut-brain communication during de novo gut colonization.MethodsWe employed a combination of gnotobiotic and state-of-the-art microbial tools, behavioral analysis, immune and pharmacological approaches. Germ-free wild type, MyD88−/−Ticam1−/−and SCID mice were studied before and after colonization with specific pathogen-free microbiota, Altered Schaedler Flora, E. coli or S. typhimurium (permanent or transient colonizers). TLR agonists and antagonists, CCR7 antagonist or immunomodulators were used to study immune pathways. We assessed brain c-Fos, brain-derived neurotrophic factor, and dendritic and glial cells by immunofluorescence, expression of neuroimmune genes by NanoString and performed brain proteomics.ResultsBacterial monocolonization, conventionalization or administration of microbial products to germ-free mice altered mouse behavior similarly, acting through Toll-like receptor or nucleotide-binding oligomerization domain signaling. The process required CD11b+CD11c+CD103+cell activation and migration into the brain. The change in behavior did not require the continued presence of bacteria and was associated with activation of multiple neuro-immune networks in the gut and the brain.ConclusionsChanges in neural plasticity occur rapidly upon initial gut microbial colonization and involve innate immune signaling to the brain, mediated by CD11b+CD11c+CD103+cell migration. The results identify a new target with therapeutic potential for DGBIs developing in context of increased gut and blood-brain barrier permeability.Highlights

Microbiota impairment is a key factor in disorders of gut-brain interaction (DGBI)

Microbial colonization induces changes in brain and behavior via innate immunity

Microbial colonization activates multiple neuro-immune networks in gut and brain

Behavioral change is mediated by CD11b+CD11c+CD103+cells migration to the brain

Publisher

Cold Spring Harbor Laboratory

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