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Circulating CD103+ γδ and CD8+ T cells are clonally shared with tissue-resident intraepithelial lymphocytes in celiac disease

Louise F. Risnes, Linn M. Eggesbø, Stephanie Zühlke, Shiva Dahal‐Koirala, Ralf S. Neumann, Knut E. A. Lundin, Asbjørn Christophersen, Ludvig M. Sollid

2021Mucosal Immunology33 citationsDOIOpen Access PDF

Abstract

Gut intraepithelial γδ and CD8+ αβ T lymphocytes have been connected to celiac disease (CeD) pathogenesis. Based on the previous observation that activated (CD38+), gut-homing (CD103+) γδ and CD8+ αβ T cells increase in blood upon oral gluten challenge, we wanted to shed light on the pathogenic involvement of these T cells by examining the clonal relationship between cells of blood and gut during gluten exposure. Of 20 gluten-challenged CeD patients, 8 and 10 had increase in (CD38+CD103+) γδ and CD8+ αβ T cells, respectively, while 16 had increase in gluten-specific CD4+ T cells. We obtained γδ and αβ TCR sequences of >2500 single cells from blood and gut of 5 patients, before and during challenge. We observed extensive sharing between blood and gut γδ and CD8+ αβ T-cell clonotypes even prior to gluten challenge. In subjects with challenge-induced surge of γδ and/or CD8+ αβ T cells, as larger populations of cells analyzed, we observed more expanded clonotypes and clonal sharing, yet no discernible TCR similarities between expanded and/or shared clonotypes. Thus, CD4+ T cells appear to drive expansion of clonally diverse γδ or CD8+ αβ T-cell clonotypes that may not be specific for the gluten antigen.

Topics & Concepts

Intraepithelial lymphocyteCD8BiologyImmunologyCD38Cytotoxic T cellGlutenHoming (biology)T cellPathogenesisAntigenImmune systemCell biologyGeneticsStem cellIn vitroCD34EcologyFood scienceCeliac Disease Research and ManagementMicroscopic ColitisT-cell and B-cell Immunology