Gut symbiotic microbes imprint intestinal immune cells with the innate receptor SLAMF4 which contributes to gut immune protection against enteric pathogens
Gut symbiotic microbes imprint intestinal immune cells with the innate receptor SLAMF4 which contributes to gut immune protection against enteric pathogens
BackgroundInteractions between host immune cells and gut microbiota are crucial for the integrity and function of the intestine. How these interactions regulate immune cell responses in the intestine remains a major gap in the field.AimWe have identified the signalling lymphocyte activation molecule family member 4 (SLAMF4) as an immunomodulator of the intestinal immunity. The aim is to determine how SLAMF4 is acquired in the gut and what its contribution to intestinal immunity is.MethodsExpression of SLAMF4 was assessed in mice and humans. The mechanism of induction was studied using GFPtgbone marrow chimaera mice, lymphotoxin α and TNLG8A-deficient mice, as well as gnotobiotic mice. Role in immune protection was revealed using oral infection withListeria monocytogenesandCytobacter rodentium.ResultsSLAMF4 is a selective marker of intestinal immune cells of mice and humans. SLAMF4 induction occurs directly in the intestinal mucosa without the involvement of the gut-associated lymphoid tissue. Gut bacterial products, particularly those of gut anaerobes, and gut-resident antigen-presenting cell (APC)TNLG8Aare key contributors of SLAMF4 induction in the intestine. Importantly, lack of SLAMF4 expression leads the increased susceptibility of mice to infection by oral pathogens culminating in their premature death.ConclusionsSLAMF4 is a marker of intestinal immune cells which contributes to the protection against enteric pathogens and whose expression is dependent on the presence of the gut microbiota. This discovery provides a possible mechanism for answering the long-standing question of how the intertwining of the host and gut microbial biology regulates immune cell responses in the gut.
- Rutgers, The State University of New Jersey United States
- Eastern Michigan University United States
- UNIVERSITY OF MICHIGAN
- University of Michigan–Ann Arbor United States
Flow Cytometry, Real-Time Polymerase Chain Reaction, Gastrointestinal Microbiome, Mice, Inbred C57BL, Mice, Signaling Lymphocytic Activation Molecule Family, Animals, Germ-Free Life, Humans, Gut Microbiota, Intestinal Mucosa, Symbiosis, Immunity, Mucosal, Signal Transduction
Flow Cytometry, Real-Time Polymerase Chain Reaction, Gastrointestinal Microbiome, Mice, Inbred C57BL, Mice, Signaling Lymphocytic Activation Molecule Family, Animals, Germ-Free Life, Humans, Gut Microbiota, Intestinal Mucosa, Symbiosis, Immunity, Mucosal, Signal Transduction
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