High abundance of plasma cells secreting transglutaminase 2–specific IgA autoantibodies with limited somatic hypermutation in celiac disease intestinal lesions

174

143

Celiac disease is an intestinal autoimmune disease driven by dietary gluten and gluten-specific CD4 + T-cell responses. In celiac patients on a gluten-free diet, exposure to gluten induces the appearance of gluten-specific CD4 + T cells with gut-homing potential in the peripheral blood. Here we show that gluten exposure also induces the appearance of activated, gut-homing CD8 + αβ and γδ T cells in the peripheral blood. Single-cell T-cell receptor sequence analysis indicates that both of these cell populations have highly focused Tcell receptor repertoires, indicating that their induction is antigendriven. These results reveal a previously unappreciated role of antigen in the induction of CD8 + αβ and γδ T cells in celiac disease and demonstrate a coordinated response by all three of the major types of T cells. More broadly, these responses may parallel adaptive immune responses to viral pathogens and other systemic autoimmune diseases.autoimmunity | mucosal immunity

Section: Resultssupporting

confidence: 92%

Dietary gluten triggers concomitant activation of CD4 ⁺ and CD8 ⁺ αβ T cells and γδ T cells in celiac disease

Han

Newell

Glanville

et al. 2013

174

143

“…That all 19 mAbs generated were genetically unrelated and used multiple V genes in each patient shows that there was not preferred V-gene use like those seen in autoantibodies against TG2 (7). The fact that the autoantibodies were polyclonal excludes a single forbidden clonotype of pathogenic autoantibodies in each patient.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, one notion for the origin of pathogenic autoantibodies is the propensity of certain V genes or alleles or preferred combinations of H and L chains to give rise to high-affinity autoantibodies against self-antigens (6). An elegant study showed that authentic human monoclonal autoantibodies (mAbs) against transglutinaminase 2 (TG2) in celiac disease used preferred V genes (7). There were few somatic mutations in the mAbs so that germ-line V genes could produce high-affinity autoantibodies against TG2, but whether the autoantibodies against TG2 are pathogenic for celiac disease is unclear (7).…”

mentioning

confidence: 99%

“…An elegant study showed that authentic human monoclonal autoantibodies (mAbs) against transglutinaminase 2 (TG2) in celiac disease used preferred V genes (7). There were few somatic mutations in the mAbs so that germ-line V genes could produce high-affinity autoantibodies against TG2, but whether the autoantibodies against TG2 are pathogenic for celiac disease is unclear (7). Conversely, an alternative origin of pathogenic autoantibodies is that the autoantibodies arise in response to a pathogen antigen that mimics a selfantigen (8).…”

mentioning

confidence: 99%

See 1 more Smart Citation

Characterization of pathogenic human monoclonal autoantibodies against GM-CSF

Wang

Thomson

Allan

et al. 2013

The origin of pathogenic autoantibodies remains unknown. Idiopathic pulmonary alveolar proteinosis is caused by autoantibodies against granulocyte–macrophage colony-stimulating factor (GM-CSF). We generated 19 monoclonal autoantibodies against GM-CSF from six patients with idiopathic pulmonary alveolar proteinosis. The autoantibodies used multiple V genes, excluding preferred V-gene use as an etiology, and targeted at least four nonoverlapping epitopes on GM-CSF, suggesting that GM-CSF is driving the autoantibodies and not a B-cell epitope on a pathogen cross-reacting with GM-CSF. The number of somatic mutations in the autoantibodies suggests that the memory B cells have been helped by T cells and re-entered germinal centers. All autoantibodies neutralized GM-CSF bioactivity, with general correlations to affinity and off-rate. The binding of certain autoantibodies was changed by point mutations in GM-CSF that reduced binding to the GM-CSF receptor. Those monoclonal autoantibodies that potently neutralize GM-CSF may be useful in treating inflammatory disease, such as rheumatoid arthritis and multiple sclerosis, cancer, and pain.

“…The panel of TG2-specific mAbs described above was generated from small intestinal biopsies of celiac disease patients (23). Based on competitive ELISA experiments, we recently showed that 49 of 57 mAbs could be placed into one of four distinct epitope groups (epitope 1-4, targeted by 30, 6, 11, and 2 mAbs, respectively), which correlated with mAb VH-segment use.…”

Section: Disulfide Bond Formation In Itg2 Prevents the Stabilizing Efmentioning

confidence: 99%

Activity-regulating structural changes and autoantibody epitopes in transglutaminase 2 assessed by hydrogen/deuterium exchange

Iversen

Mysling

Hnida

et al. 2014

Self Cite

The multifunctional enzyme transglutaminase 2 (TG2) is the target of autoantibodies in the gluten-sensitive enteropathy celiac disease. In addition, the enzyme is responsible for deamidation of gluten peptides, which are subsequently targeted by T cells. To understand the regulation of TG2 activity and the enzyme's role as an autoantigen in celiac disease, we have addressed structural properties of TG2 in solution by using hydrogen/deuterium exchange monitored by mass spectrometry. We demonstrate that Ca 2+ binding, which is necessary for TG2 activity, induces structural changes in the catalytic core domain of the enzyme. Cysteine oxidation was found to abolish these changes, suggesting a mechanism whereby disulfide bond formation inactivates the enzyme. Further, by using TG2-specific human monoclonal antibodies generated from intestinal plasma cells of celiac disease patients, we observed that binding of TG2 by autoantibodies can induce structural changes that could be relevant for the pathogenesis. Detailed mapping of two of the main epitopes targeted by celiac disease autoantibodies revealed that they are located adjacent to each other in the N-terminal part of the TG2 molecule.