Litcius/Paper detail

Structural bases of T cell antigen receptor recognition in celiac disease

Laura Ciacchi, Hugh H. Reid, Jamie Rossjohn

2022Current Opinion in Structural Biology12 citationsDOIOpen Access PDF

Abstract

Celiac disease (CeD) is a human leukocyte antigen (HLA)-linked autoimmune-like disorder that is triggered by the ingestion of gluten or related storage proteins. The majority of CeD patients are HLA-DQ2.5+, with the remainder being either HLA-DQ8+ or HLA-DQ2.2+. Structural studies have shown how deamidation of gluten epitopes engenders binding to HLA-DQ2.5/8, which then triggers an aberrant CD4+ T cell response. HLA tetramer studies, combined with structural investigations, have demonstrated that repeated patterns of TCR usage underpins the immune response to some HLADQ2.5/8 restricted gluten epitopes, with distinct TCR motifs representing common landing pads atop the HLA–gluten complexes. Structural studies have provided insight into TCR specificity and cross-reactivity towards gluten epitopes, as well as cross-reactivity to bacterial homologues of gluten epitopes, suggesting that environmental factors may directly play a role in CeD pathogenesis. Collectively, structural immunology-based studies in the CeD axis may lead to new therapeutics/diagnostics to treat CeD, and also serve as an exemplar for other T cell mediated autoimmune diseases.

Topics & Concepts

EpitopeDeamidationT-cell receptorHuman leukocyte antigenImmunologyGlutenT cellAntigenBiologyImmune systemBiochemistryEnzymeCeliac Disease Research and ManagementMicroscopic ColitisMonoclonal and Polyclonal Antibodies Research