Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation

Cláudia S. Rodrigues; Joana Gaifem; Márcia S. Pereira; Maria Francisca Alves; Mariana Silva; Nuno Padrão; Bruno Cavadas; Catarina Moreira-Barbosa; Inês Alves; Ricardo Marcos-Pinto; Joana Torres; Aonghus Lavelle; Jean Frederic Colombel; Harry Sokol; Salomé S. Pinho

doi:10.1080/19490976.2025.2461210

Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation

Cláudia S. Rodrigues
, Joana Gaifem
, Márcia S. Pereira
, Maria Francisca Alves
, Mariana Silva
, Nuno Padrão
, Bruno Cavadas
, Catarina Moreira-Barbosa
, Inês Alves
, Ricardo Marcos-Pinto
, Joana Torres
, Aonghus Lavelle
, Jean Frederic Colombel
, Harry Sokol
, Salomé S. Pinho

Research output: Contribution to journal › Article › peer-review

Abstract

The perturbation of the symbiotic relationship between microbes and intestinal immune system contributes to gut inflammation and Inflammatory Bowel Disease (IBD) development. The host mucosa glycans (glycocalyx) creates a major biological interface between gut microorganisms and host immunity that remains ill-defined. Glycans are essential players in IBD immunopathogenesis, even years before disease onset. However, how changes in mucosa glycosylation shape microbiome and how this impact gut immune response and inflammation remains to be clarified. Here, we revealed that alterations in the expression of complex branched N-glycans at gut mucosa surface, modeled in glycoengineered mice, resulted in dysbiosis, with a deficiency in Firmicutes bacteria. Concomitantly, this mucosa N-glycan switch was associated with a downregulation of type 3 innate lymphoid cells (ILC3)-mediated immune response, leading to the transition of ILC3 toward an ILC1 proinflammatory phenotype and increased TNFα production. In addition, we demonstrated that the mucosa glycosylation remodeling through prophylactic supplementation with glycans at steady state was able to restore microbial-derived short-chain fatty acids and microbial sensing (by NOD2 expression) alongside the rescue of the expression of ILC3 module, suppressing intestinal inflammation and controlling disease onset. In a complementary approach, we further showed that IBD patients, often displaying dysbiosis, exhibited a tendency of decreased MGAT5 expression at epithelial cells that was accompanied by reduced ILC3 expression in gut mucosa. Altogether, these results unlock the effects of alterations in mucosa glycome composition in the regulation of the bidirectional crosstalk between microbiota and gut immune response, revealing host branched N-glycans/microbiota/ILC3 axis as an essential pathway in gut homeostasis and in preventing health to intestinal inflammation transition.

Original language	English
Article number	2461210
Journal	Gut Microbes
Volume	17
Issue number	1
DOIs	https://doi.org/10.1080/19490976.2025.2461210
Publication status	Published - 2025
Externally published	Yes

Keywords

ILC3
intestinal inflammation
microbiome
N-glycans
prophylaxis

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10.1080/19490976.2025.2461210

Cite this

Rodrigues, C. S., Gaifem, J., Pereira, M. S., Alves, M. F., Silva, M., Padrão, N., Cavadas, B., Moreira-Barbosa, C., Alves, I., Marcos-Pinto, R., Torres, J., Lavelle, A., Colombel, J. F., Sokol, H., & Pinho, S. S. (2025). Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation. Gut Microbes, 17(1), Article 2461210. https://doi.org/10.1080/19490976.2025.2461210

@article{9d55a2c0c334463f951ce6cdcaa18319,

title = "Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation",

abstract = "The perturbation of the symbiotic relationship between microbes and intestinal immune system contributes to gut inflammation and Inflammatory Bowel Disease (IBD) development. The host mucosa glycans (glycocalyx) creates a major biological interface between gut microorganisms and host immunity that remains ill-defined. Glycans are essential players in IBD immunopathogenesis, even years before disease onset. However, how changes in mucosa glycosylation shape microbiome and how this impact gut immune response and inflammation remains to be clarified. Here, we revealed that alterations in the expression of complex branched N-glycans at gut mucosa surface, modeled in glycoengineered mice, resulted in dysbiosis, with a deficiency in Firmicutes bacteria. Concomitantly, this mucosa N-glycan switch was associated with a downregulation of type 3 innate lymphoid cells (ILC3)-mediated immune response, leading to the transition of ILC3 toward an ILC1 proinflammatory phenotype and increased TNFα production. In addition, we demonstrated that the mucosa glycosylation remodeling through prophylactic supplementation with glycans at steady state was able to restore microbial-derived short-chain fatty acids and microbial sensing (by NOD2 expression) alongside the rescue of the expression of ILC3 module, suppressing intestinal inflammation and controlling disease onset. In a complementary approach, we further showed that IBD patients, often displaying dysbiosis, exhibited a tendency of decreased MGAT5 expression at epithelial cells that was accompanied by reduced ILC3 expression in gut mucosa. Altogether, these results unlock the effects of alterations in mucosa glycome composition in the regulation of the bidirectional crosstalk between microbiota and gut immune response, revealing host branched N-glycans/microbiota/ILC3 axis as an essential pathway in gut homeostasis and in preventing health to intestinal inflammation transition.",

keywords = "ILC3, intestinal inflammation, microbiome, N-glycans, prophylaxis",

author = "Rodrigues, \{Cl{\'a}udia S.\} and Joana Gaifem and Pereira, \{M{\'a}rcia S.\} and Alves, \{Maria Francisca\} and Mariana Silva and Nuno Padr{\~a}o and Bruno Cavadas and Catarina Moreira-Barbosa and In{\^e}s Alves and Ricardo Marcos-Pinto and Joana Torres and Aonghus Lavelle and Colombel, \{Jean Frederic\} and Harry Sokol and Pinho, \{Salom{\'e} S.\}",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s). Published with license by Taylor \& Francis Group, LLC.",

year = "2025",

doi = "10.1080/19490976.2025.2461210",

language = "English",

volume = "17",

journal = "Gut Microbes",

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Rodrigues, CS, Gaifem, J, Pereira, MS, Alves, MF, Silva, M, Padrão, N, Cavadas, B, Moreira-Barbosa, C, Alves, I, Marcos-Pinto, R, Torres, J, Lavelle, A, Colombel, JF, Sokol, H & Pinho, SS 2025, 'Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation', Gut Microbes, vol. 17, no. 1, 2461210. https://doi.org/10.1080/19490976.2025.2461210

TY - JOUR

T1 - Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3

T2 - a key driver of intestinal inflammation

AU - Rodrigues, Cláudia S.

AU - Gaifem, Joana

AU - Pereira, Márcia S.

AU - Alves, Maria Francisca

AU - Silva, Mariana

AU - Padrão, Nuno

AU - Cavadas, Bruno

AU - Moreira-Barbosa, Catarina

AU - Alves, Inês

AU - Marcos-Pinto, Ricardo

AU - Torres, Joana

AU - Lavelle, Aonghus

AU - Colombel, Jean Frederic

AU - Sokol, Harry

AU - Pinho, Salomé S.

PY - 2025

Y1 - 2025

N2 - The perturbation of the symbiotic relationship between microbes and intestinal immune system contributes to gut inflammation and Inflammatory Bowel Disease (IBD) development. The host mucosa glycans (glycocalyx) creates a major biological interface between gut microorganisms and host immunity that remains ill-defined. Glycans are essential players in IBD immunopathogenesis, even years before disease onset. However, how changes in mucosa glycosylation shape microbiome and how this impact gut immune response and inflammation remains to be clarified. Here, we revealed that alterations in the expression of complex branched N-glycans at gut mucosa surface, modeled in glycoengineered mice, resulted in dysbiosis, with a deficiency in Firmicutes bacteria. Concomitantly, this mucosa N-glycan switch was associated with a downregulation of type 3 innate lymphoid cells (ILC3)-mediated immune response, leading to the transition of ILC3 toward an ILC1 proinflammatory phenotype and increased TNFα production. In addition, we demonstrated that the mucosa glycosylation remodeling through prophylactic supplementation with glycans at steady state was able to restore microbial-derived short-chain fatty acids and microbial sensing (by NOD2 expression) alongside the rescue of the expression of ILC3 module, suppressing intestinal inflammation and controlling disease onset. In a complementary approach, we further showed that IBD patients, often displaying dysbiosis, exhibited a tendency of decreased MGAT5 expression at epithelial cells that was accompanied by reduced ILC3 expression in gut mucosa. Altogether, these results unlock the effects of alterations in mucosa glycome composition in the regulation of the bidirectional crosstalk between microbiota and gut immune response, revealing host branched N-glycans/microbiota/ILC3 axis as an essential pathway in gut homeostasis and in preventing health to intestinal inflammation transition.

AB - The perturbation of the symbiotic relationship between microbes and intestinal immune system contributes to gut inflammation and Inflammatory Bowel Disease (IBD) development. The host mucosa glycans (glycocalyx) creates a major biological interface between gut microorganisms and host immunity that remains ill-defined. Glycans are essential players in IBD immunopathogenesis, even years before disease onset. However, how changes in mucosa glycosylation shape microbiome and how this impact gut immune response and inflammation remains to be clarified. Here, we revealed that alterations in the expression of complex branched N-glycans at gut mucosa surface, modeled in glycoengineered mice, resulted in dysbiosis, with a deficiency in Firmicutes bacteria. Concomitantly, this mucosa N-glycan switch was associated with a downregulation of type 3 innate lymphoid cells (ILC3)-mediated immune response, leading to the transition of ILC3 toward an ILC1 proinflammatory phenotype and increased TNFα production. In addition, we demonstrated that the mucosa glycosylation remodeling through prophylactic supplementation with glycans at steady state was able to restore microbial-derived short-chain fatty acids and microbial sensing (by NOD2 expression) alongside the rescue of the expression of ILC3 module, suppressing intestinal inflammation and controlling disease onset. In a complementary approach, we further showed that IBD patients, often displaying dysbiosis, exhibited a tendency of decreased MGAT5 expression at epithelial cells that was accompanied by reduced ILC3 expression in gut mucosa. Altogether, these results unlock the effects of alterations in mucosa glycome composition in the regulation of the bidirectional crosstalk between microbiota and gut immune response, revealing host branched N-glycans/microbiota/ILC3 axis as an essential pathway in gut homeostasis and in preventing health to intestinal inflammation transition.

KW - ILC3

KW - intestinal inflammation

KW - microbiome

KW - N-glycans

KW - prophylaxis

UR - https://www.scopus.com/pages/publications/85217372366

U2 - 10.1080/19490976.2025.2461210

DO - 10.1080/19490976.2025.2461210

M3 - Article

C2 - 39918275

AN - SCOPUS:85217372366

SN - 1949-0976

VL - 17

JO - Gut Microbes

JF - Gut Microbes

IS - 1

M1 - 2461210

ER -

Alterations in mucosa branched N-glycans lead to dysbiosis and downregulation of ILC3: a key driver of intestinal inflammation

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Keywords

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