Metabolic control of T cell immune response through glycans in inflammatory bowel disease.

Dias, Ana M; Correia, Alexandra; Pereira, Márcia S; Almeida, Catarina R; Alves, Inês; Pinto, Vanda; Catarino, Telmo A; Mendes, Nuno; Leander, Magdalena; Oliva-Teles, M Teresa; Maia, Luís; Delerue-Matos, Cristina; Taniguchi, Naoyuki; Lima, Margarida; Pedroto, Isabel; Marcos-Pinto, Ricardo; Lago, Paula; Reis, Celso A; Vilanova, Manuel; Pinho, Salomé S

Dias, Ana M; Correia, Alexandra; Pereira, Márcia S; Almeida, Catarina R; Alves, Inês; Pinto, Vanda; Catarino, Telmo A; Mendes, Nuno; Leander, Magdalena; Oliva-Teles, M Teresa; Maia, Luís; Delerue-Matos, Cristina; Taniguchi, Naoyuki; Lima, Margarida; Pedroto, Isabel; Marcos-Pinto, Ricardo; Lago, Paula; Reis, Celso A; Vilanova, Manuel; Pinho, Salomé S.

Afiliação

Dias AM; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Correia A; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Pereira MS; Institute of Biomedical Sciences of Abel Salazar (ICBAS), University of Porto, 4050-313 Porto, Portugal.
Almeida CR; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Alves I; Institute for Molecular and Cell Biology (IBMC), Immunobiology Group, University of Porto, 4200-135 Porto, Portugal.
Pinto V; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Catarino TA; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Mendes N; Institute of Biomedical Sciences of Abel Salazar (ICBAS), University of Porto, 4050-313 Porto, Portugal.
Leander M; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Oliva-Teles MT; Institute of Biomedical Engineering (INEB), 4200-135 Porto, Portugal.
Maia L; Institute for Biomedicine, Department of Medical Sciences, University of Aveiro, 3810-193 Aveiro, Portugal.
Delerue-Matos C; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Taniguchi N; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Lima M; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Pedroto I; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Marcos-Pinto R; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Lago P; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Reis CA; Institute for Research and Innovation in Health (i3S), University of Porto, 4200-135 Porto, Portugal.
Vilanova M; Institute of Molecular Pathology and Immunology of University of Porto (IPATIMUP), 4200-135 Porto, Portugal.
Pinho SS; Hematology Department, Centro Hospitalar do Porto, 4099-001 Porto, Portugal.

Proc Natl Acad Sci U S A ; 115(20): E4651-E4660, 2018 05 15.

Article em En | MEDLINE | ID: mdl-29720442

ABSTRACT

ABSTRACT

Mucosal T lymphocytes from patients with ulcerative colitis (UC) were previously shown to display a deficiency in branched N-glycosylation associated with disease severity. However, whether this glycosylation pathway shapes the course of the T cell response constituting a targeted-specific mechanism in UC remains largely unknown. In this study, we demonstrated that metabolic supplementation of ex vivo mucosal T cells from patients with active UC with N-acetylglucosamine (GlcNAc) resulted in enhancement of branched N-glycosylation in the T cell receptor (TCR), leading to suppression of T cell growth, inhibition of the T helper 1 (Th1)/Th17 immune response, and controlled T cell activity. We further demonstrated that mouse models displaying a deficiency in the branched N-glycosylation pathway (MGAT5-/-, MGAT5+/-) exhibited increased susceptibility to severe forms of colitis and early-onset disease. Importantly, the treatment of these mice with GlcNAc reduced disease severity and suppressed disease progression due to a controlled T cell-mediated immune response at the intestinal mucosa. In conclusion, our human ex vivo and preclinical results demonstrate the targeted-specific immunomodulatory properties of this simple glycan, proposing a therapeutic approach for patients with UC.

Assuntos

Acetilglucosamina/farmacologia; Linfócitos T CD4-Positivos/imunologia; Colite Ulcerativa/imunologia; N-Acetilglucosaminiltransferases/fisiologia; Polissacarídeos/metabolismo; Imunidade Adaptativa; Animais; Linfócitos T CD4-Positivos/efeitos dos fármacos; Linfócitos T CD4-Positivos/metabolismo; Estudos de Casos e Controles; Colite Ulcerativa/induzido quimicamente; Colite Ulcerativa/tratamento farmacológico; Colite Ulcerativa/metabolismo; Citocinas/metabolismo; Glicosilação; Humanos; Ativação Linfocitária; Camundongos; Camundongos Endogâmicos C57BL; Camundongos Knockout; Receptores de Antígenos de Linfócitos T/metabolismo

Palavras-chave

T cell receptor; T lymphocytes; adaptive immune response; branched N-glycosylation; intestinal inflammation

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Polissacarídeos / Acetilglucosamina / Linfócitos T CD4-Positivos / Colite Ulcerativa / N-Acetilglucosaminiltransferases Tipo de estudo: Observational_studies / Risk_factors_studies Limite: Animals / Humans Idioma: En Ano de publicação: 2018 Tipo de documento: Article

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