Literature DB >> 32060138

GCNT1-Mediated O-Glycosylation of the Sialomucin CD43 Is a Sensitive Indicator of Notch Signaling in Activated T Cells.

Eric Perkey1,2, Dave Maurice De Sousa3,4, Léolène Carrington5, Jooho Chung2, Alexander Dils2, David Granadier2, Ute Koch6, Freddy Radtke6, Burkhard Ludewig7, Bruce R Blazar8, Christian W Siebel9, Todd V Brennan10, Jeffrey Nolz11, Nathalie Labrecque12,4,13, Ivan Maillard14.   

Abstract

Notch signaling is emerging as a critical regulator of T cell activation and function. However, there is no reliable cell surface indicator of Notch signaling across activated T cell subsets. In this study, we show that Notch signals induce upregulated expression of the Gcnt1 glycosyltransferase gene in T cells mediating graft-versus-host disease after allogeneic bone marrow transplantation in mice. To determine if Gcnt1-mediated O-glycosylation could be used as a Notch signaling reporter, we quantified the core-2 O-glycoform of CD43 in multiple T cell subsets during graft-versus-host disease. Pharmacological blockade of Delta-like Notch ligands abrogated core-2 O-glycosylation in a dose-dependent manner after allogeneic bone marrow transplantation, both in donor-derived CD4+ and CD8+ effector T cells and in Foxp3+ regulatory T cells. CD43 core-2 O-glycosylation depended on cell-intrinsic canonical Notch signals and identified CD4+ and CD8+ T cells with high cytokine-producing ability. Gcnt1-deficient T cells still drove lethal alloreactivity, showing that core-2 O-glycosylation predicted, but did not cause, Notch-dependent T cell pathogenicity. Using core-2 O-glycosylation as a marker of Notch signaling, we identified Ccl19-Cre+ fibroblastic stromal cells as critical sources of Delta-like ligands in graft-versus-host responses irrespective of conditioning intensity. Core-2 O-glycosylation also reported Notch signaling in CD8+ T cell responses to dendritic cell immunization, Listeria infection, and viral infection. Thus, we uncovered a role for Notch in controlling core-2 O-glycosylation and identified a cell surface marker to quantify Notch signals in multiple immunological contexts. Our findings will help refine our understanding of the regulation, cellular source, and timing of Notch signals in T cell immunity.
Copyright © 2020 by The American Association of Immunologists, Inc.

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Year:  2020        PMID: 32060138      PMCID: PMC7306398          DOI: 10.4049/jimmunol.1901194

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  59 in total

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Journal:  J Clin Invest       Date:  2017-03-20       Impact factor: 14.808

3.  Absence of P-selectin in recipients of allogeneic bone marrow transplantation ameliorates experimental graft-versus-host disease.

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5.  Blockade of individual Notch ligands and receptors controls graft-versus-host disease.

Authors:  Ivy T Tran; Ashley R Sandy; Alexis J Carulli; Christen Ebens; Jooho Chung; Gloria T Shan; Vedran Radojcic; Ann Friedman; Thomas Gridley; Amy Shelton; Pavan Reddy; Linda C Samuelson; Minhong Yan; Christian W Siebel; Ivan Maillard
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9.  Specific fibroblastic niches in secondary lymphoid organs orchestrate distinct Notch-regulated immune responses.

Authors:  Nicolas Fasnacht; Hsin-Ying Huang; Ute Koch; Stéphanie Favre; Floriane Auderset; Qian Chai; Lucas Onder; Sandra Kallert; Daniel D Pinschewer; H Robson MacDonald; Fabienne Tacchini-Cottier; Burkhard Ludewig; Sanjiv A Luther; Freddy Radtke
Journal:  J Exp Med       Date:  2014-10-13       Impact factor: 14.307

10.  Maturation of lymph node fibroblastic reticular cells from myofibroblastic precursors is critical for antiviral immunity.

Authors:  Qian Chai; Lucas Onder; Elke Scandella; Cristina Gil-Cruz; Christian Perez-Shibayama; Jovana Cupovic; Renzo Danuser; Tim Sparwasser; Sanjiv A Luther; Volker Thiel; Thomas Rülicke; Jens V Stein; Thomas Hehlgans; Burkhard Ludewig
Journal:  Immunity       Date:  2013-04-25       Impact factor: 31.745

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