Your search keyword '"Sollid, Ludvig M."' showing total 50 results

1. Dissecting autoimmune encephalitis through the lens of intrathecal B cells.

Author

Iversen, Rasmus and Sollid, Ludvig M.

Subjects

*B cells, *T cells, *B cell receptors, *T cell receptors, *ENCEPHALITIS, *PLASMA cells, *REGULATORY T cells

Abstract

The article explores autoimmune encephalitis, a condition where the immune system attacks the brain. It emphasizes the role of B cells in the development of autoantibodies, which are responsible for the disease. The authors studied immune cells from patients with anti-LGI1 and anti-CASPR2 encephalitis and found an abundance of plasma cells that produce the autoantibodies. They also discuss the interaction between T cells and B cells in the activation and expansion of B cells. The article suggests that B cells may be activated outside of the central nervous system and cross the blood-brain barrier to produce autoantibodies. It mentions the potential for B cell-targeted therapies in treating autoimmune diseases, but the specific antigens recognized by T cells in autoimmune encephalitis remain unknown. [Extracted from the article]

Published

2024

2. Single-cell approaches to dissect adaptive immune responses involved in autoimmunity: the case of celiac disease.

Author

Lindeman, Ida and Sollid, Ludvig M.

Published

2022

3. C‐type lectin‐like CD161 is not a co‐signalling receptor in gluten‐reactive CD4 + T cells.

Author

Wyrożemski, Łukasz, Sollid, Ludvig M., and Qiao, Shuo‐Wang

Subjects

*T cells, *CD4 antigen, *KILLER cells, *CELIAC disease, *MEMBRANE proteins

Abstract

C‐type lectin‐like CD161, a class II transmembrane protein, is a surface receptor expressed by NK cells and T cells. In coeliac disease, CD161 was expressed more frequently on gluten‐reactive CD4 + T cells compared to other memory CD4 + T cells isolated from the same tissue compartment. CD161 is a putative co‐signalling molecule that was proposed to act as co‐stimulatory receptor in the context of signalling through TCR, but contradicting results were published. In order to understand the role of CD161 in gluten‐reactive CD4 + T cells, we combined T cell stimulation assays or T cell proliferation assays with ligation of CD161 and intracellular cytokine staining. We found that CD161 ligation provided neither co‐stimulatory nor co‐inhibitory signals to modulate proliferation and IFN‐γ or IL‐21 production by gluten‐reactive CD4 + T cell clones. Thus, we suggest that CD161 does not function as a co‐signalling receptor in the context of gluten‐reactive CD4 + T cells. [ABSTRACT FROM AUTHOR]

Published

2021

4. Update 2020: nomenclature and listing of celiac disease–relevant gluten epitopes recognized by CD4+ T cells.

Author

Sollid, Ludvig M., Tye-Din, Jason A., Qiao, Shuo-Wang, Anderson, Robert P., Gianfrani, Carmen, and Koning, Frits

Subjects

*HLA histocompatibility antigens, *EPITOPES, *GLUTEN, *GLUTELINS, *CELIAC disease, *T cells, *T cell receptors

Abstract

Celiac disease is caused by an abnormal intestinal T cell response to cereal gluten proteins. The disease has a strong human leukocyte antigen (HLA) association, and CD4+ T cells recognizing gluten epitopes presented by disease-associated HLA-DQ allotypes are considered to be drivers of the disease. This paper provides an update of the currently known HLA-DQ restricted gluten T cell epitopes with their names and sequences. [ABSTRACT FROM AUTHOR]

Published

2020

5. In memoriam: Erik Thorsby (1938‐2021).

Author

Sollid, Ludvig M., Lundin, Knut E. A., Leivestad, Torbjørn, Spurkland, Anne, and Vartdal, Frode

Subjects

*TRANSPLANTATION of organs, tissues, etc., *FIRE chiefs, *HISTOCOMPATIBILITY antigens, *TRANSPLANTATION immunology, *TYPE 1 diabetes, *DRAFT (Military service), *FIRE stations, *T cell receptors

Abstract

Erik failed to raise HLA-specific rabbit antibodies, which could help to identify donor-recipient pairs bearing compatible HLA molecules. Erik became a world expert in this field producing key papers on the HLA association of type 1 diabetes,12 multiple sclerosis13 and coeliac disease.14,15 We were all fortunate to collaborate with Erik on different aspects of HLA biology, ranging from organ transplantation to the molecular underpinnings of HLA association in coeliac disease. From one of the volunteers, Erik collected serum which identified the antigen MH,3 later baptized HLA-B5. GLO:2CR/01jul21:sji13055-fig-0001.jpg PHOTO (COLOR): . gl Erik Thorsby, one of the true pioneers in the fields of HLA, immunogenetics and transplantation immunology, passed away on March 23rd. [Extracted from the article]

Published

2021

6. Erik Thorsby (1938–2021).

Author

Sollid, Ludvig M., Lundin, Knut E. A., Leivestad, Torbjørn, Spurkland, Anne, and Vartdal, Frode

Subjects

*TRANSPLANTATION immunology, *TYPE 1 diabetes, *DRAFT (Military service), *VASCULAR endothelial cells, *ANTIGEN presentation

Abstract

From one of the volunteers Erik collected serum which identified the antigen MH (Thorsby and Kissmeyer-Nielsen [14]), later baptised HLA-B5. We were all fortunate to collaborate with Erik on different aspects of HLA biology, ranging from organ transplantation to the molecular underpinnings of HLA-association in coeliac disease. Graph Erik Thorsby, one of the true pioneers in the fields of HLA, immunogenetics and transplantation immunology passed away on March 23rd. Erik failed to raise HLA specific rabbit antibodies, which could help to identify donor-recipient pairs bearing compatible HLA-molecules. [Extracted from the article]

Published

2021

7. Two novel HLA-DQ2.5-restricted gluten T cell epitopes in the DQ2.5-glia-γ4 epitope family.

Author

Qiao, Shuo-Wang and Sollid, Ludvig M.

Subjects

*T cells, *GLUTEN, *EPITOPES, *GLUTELINS, *CELIAC disease, *CYTOTOXIC T cells, *T cell receptors

Abstract

Celiac disease is a chronic inflammatory condition of the small intestine caused by aberrant adaptive immune response to gluten protein from wheat and related cereal plants. Over 90% of celiac disease patients carry the HLA-DQ2.5 allotype and HLA-DQ2.5 presents gluten peptides to gluten-reactive CD4+ T cells in celiac disease patients. A large number of HLA-DQ2.5-restricted gluten T cell epitopes have been identified over the years. These epitopes are in general proline-rich and contain at least one glutamic acid residue that is generated from glutamine in the native gluten protein by deamidation. The deamidation is mediated by the enzyme transglutaminase 2 (TG2). It has been shown that the same T cell could recognize several different HLA-DQ2.5-restricted gluten T cell epitopes due to sequence similarities. In this paper, we demonstrate that three T cell clones derived from duodenal biopsies of different celiac disease patients are able to respond to at least five different gluten T cell epitopes within the DQ2.5-glia-γ4 epitope family, including two novel epitopes. [ABSTRACT FROM AUTHOR]

Published

2019

8. T Cells in Celiac Disease.

Author

Jabri, Bana and Sollid, Ludvig M.

Subjects

*CELIAC disease, *T cells, *GLUTEN, *AUTOIMMUNE diseases, *LYMPHOCYTES, *EPITHELIAL cells

Abstract

Celiac disease is a human T cell-mediated autoimmunelike disorder caused by exposure to dietary gluten in genetically predisposed individuals. This review will discuss how CD4 T cell responses directed against an exogenous Ag can cause an autoreactive B cell response and participate in the licensing of intraepithelial lymphocytes to kill intestinal epithelial cells. Furthermore, this review will examine the mechanisms by which intraepithelial cytotoxic T cells mediate tissue destruction in celiac disease. [ABSTRACT FROM AUTHOR]

Published

2017

9. Molecular mechanisms for contribution of MHC molecules to autoimmune diseases.

Author

Sollid, Ludvig M, Pos, Wouter, and Wucherpfennig, Kai W

Subjects

*MOLECULAR biology, *MAJOR histocompatibility complex, *DISEASE susceptibility, *AUTOIMMUNE diseases, *MEDICAL research

Abstract

It will soon be 50 years since the first MHC associations with human disease were described. These seminal studies opened a flourishing area of research, yet much remains to be discovered. Genome-wide association studies of autoimmune diseases have demonstrated that the MHC region has effect sizes that supersede those for any non-MHC locus for most diseases. Thus, an understanding of how particular MHC alleles confer susceptibility will be essential for a comprehensive understanding of autoimmune disease pathogenesis. Here we review recent exciting findings in this important field. [ABSTRACT FROM AUTHOR]

Published

2014

10. Autoimmunity provoked by foreign antigens.

Author

Iversen, Rasmus and Sollid, Ludvig M.

Subjects

*AUTOIMMUNITY, *T cells, *B cells, *CELIAC disease, *MAJOR histocompatibility complex

Abstract

The article focuses on a study which reveals that exogenous gluten drives T cell–B cell interactions that cause autoimmunity in celiac disease. It mentions that the gluten epitopes that are recognized by the CD4+ T cells uniformly contain negatively charged glutamate residues that are important for binding to the CeD-associated major histocompatibility complex (MHC) class II molecules.

Published

2020

11. Separate Gut Plasma Cell Populations Produce Auto‐Antibodies against Transglutaminase 2 and Transglutaminase 3 in Dermatitis Herpetiformis.

Author

Das, Saykat, Stamnaes, Jorunn, Kemppainen, Esko, Hervonen, Kaisa, Lundin, Knut E. A., Parmar, Naveen, Jahnsen, Frode L., Jahnsen, Jørgen, Lindfors, Katri, Salmi, Teea, Iversen, Rasmus, and Sollid, Ludvig M.

Subjects

*PLASMA cells, *CELL populations, *AUTOANTIBODIES, *IMMUNOGLOBULINS, *MONOCLONAL antibodies, *SKIN inflammation, *CELIAC disease

Abstract

Dermatitis herpetiformis (DH) is an inflammatory skin disorder often considered as an extra intestinal manifestation of celiac disease (CeD). Hallmarks of CeD and DH are auto‐antibodies to transglutaminase 2 (TG2) and transglutaminase 3 (TG3), respectively. DH patients have auto‐antibodies reactive with both transglutaminase enzymes. Here it is reported that in DH both gut plasma cells and serum auto‐antibodies are specific for either TG2 or TG3 with no TG2–TG3 cross reactivity. By generating monoclonal antibodies from TG3‐specific duodenal plasma cells of DH patients, three conformational epitope groups are defined. Both TG2‐specific and TG3‐specific gut plasma cells have few immunoglobulin (Ig) mutations, and the two transglutaminase‐reactive populations show distinct selection of certain heavy and light chain V‐genes. Mass spectrometry analysis of TG3‐specific serum IgA corroborates preferential usage of IGHV2‐5 in combination with IGKV4‐1. Collectively, these results demonstrate parallel induction of anti‐TG2 and anti‐TG3 auto‐antibody responses involving separate B‐cell populations in DH patients. [ABSTRACT FROM AUTHOR]

Published

2023

12. Expression of transglutaminase 2 in human gut epithelial cells: Implications for coeliac disease.

Author

Amundsen, Sunniva F., Stamnaes, Jorunn, Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*CELIAC disease, *EPITHELIAL cells, *GLUTEN, *TRANSGLUTAMINASES, *WESTERN immunoblotting, *DUODENAL diseases, *MASS spectrometry

Abstract

Background: Formation of complexes between transglutaminase 2 (TG2) and gluten can mechanistically explain why TG2 serves both as B-cell autoantigen and as an enzyme that creates deamidated gluten epitopes in coeliac disease (CeD). A model has been proposed where TG2 released from shed epithelial cells encounters high concentrations of dietary gluten peptides to form these TG2:gluten complexes. In this work we have characterised TG2 protein expression in gut epithelial cells in humans. Methods: Western blot analysis, immunofluorescence staining and mass spectrometry in combination with laser capture microdissection to gain spatial resolution were used to characterise TG2 expression in the epithelial cell layer of healthy and coeliac disease affected duodenum. Findings: TG2 is expressed in human duodenal epithelial cells, including cells in the apical region that are shed into the gut lumen. In untreated CeD the apical expression of TG2 is doubled. Enzymatically active TG2 is readily released from isolated human intestinal epithelial cells. Conclusion: Shed epithelial cells are a plausible source of pathogenic TG2 enzyme in CeD. Increased epithelial TG2 expression and increased epithelial shedding in active CeD may reinforce action of luminal TG2 in this condition. [ABSTRACT FROM AUTHOR]

Published

2023

13. Identification of gluten T cell epitopes driving celiac disease.

Author

Chlubnová, Markéta, Christophersen, Asbjørn O., Sandve, Geir Kjetil F., Lundin, Knut E. A., Jahnsen, Jørgen, Dahal-Koirala, Shiva, and Sollid, Ludvig M.

Subjects

*CELIAC disease, *EPITOPES, *GLUTEN, *GLUTELINS, *PEPTIDOMIMETICS, *T cells

Abstract

The article discusses a research study conducted to combine the knowledge of a distinct phenotype of gluten-reactive T cells and key features of known gluten epitopes for the discovery of unknown epitopes. It is noted that the research tested 42 wheat gluten–reactive T cell clones, isolated on the basis of distinct phenotype and with no reactivity to known epitopes, against synthetic peptides bioinformatically identified from a wheat gluten protein database.

Published

2023

14. The development and validation of a high-capacity serological assay for celiac disease.

Author

Klaasen, Rolf A., Warren, David J., Iversen, Rasmus, Bolstad, Nils, Andersen, Ina L., Mjønes, Patricia, Rønne, Elin, Lundin, Knut E.A., Sollid, Ludvig M., and Ness–Jensen, Eivind

Subjects

*CELIAC disease, *MEDICAL screening, *DIAGNOSIS, *IMMUNOGLOBULIN A, *IMMUNOGLOBULINS

Abstract

• A high capacity anti-transglutaminase 2 IgA and IgG assay is possible. • Anti-transglutaminase 2 IgA and IgG could be used in population screening. • Anti-transglutaminase 2 IgA levels correlates with disease severity. The aim of the present study was to develop and clinically validate a high-throughput assay for serum IgA and IgG antibodies against transglutaminase-2 (TG2) and to determine appropriate assay cut-offs for large-scale population screening for celiac disease. An automated method was developed using dual label time-resolved fluorometry on the AutoDELFIA platform. Individuals (n = 1920) from the general population were screened. Subjects with serum anti-TG2 concentrations above a preliminary cut-off (>0.3 mg*/L anti-TG2 IgA or >0.5 mg*/L anti-TG2 IgG) were offered endoscopic examination and biopsy. A diagnosis of celiac disease was given if villous atrophy (Marsh grade 3) was found. The assay had a limit of quantification of 0.25 mg*/L (anti-TG2 IgA) and 0.60 mg*/L (anti-TG2 IgG) with imprecision (CV) < 16% and <18% respectively. A total of 66 individuals were above the preliminary cut-off, and 56 underwent endoscopy. Of these, 26 were diagnosed with celiac disease. Sixty-eight percent of subjects with anti-TG2 IgA ≥ 0.7 mg*/L or anti-TG2 IgG ≥ 1.0 mg*/L had biopsy-proven celiac disease, and utilization of these higher cut-offs identified 96% of biopsy-positive patients. At the time of endoscopy, all individuals with anti-TG2 IgA > 2.0 mg*/L had celiac disease, and this cut-off identified 88% of newly diagnosed celiac patients. Eight percent (2/26) of the newly diagnosed patients had primarily anti-TG2 IgG. In this study we developed and clinically validated a robust and automated assay suitable for celiac disease screening in the general population. [ABSTRACT FROM AUTHOR]

Published

2022

15. Selective activation of naïve B cells with unique epitope specificity shapes autoantibody formation in celiac disease.

Author

Das, Saykat, Stamnaes, Jorunn, Høydahl, Lene S., Skagen, Christine, Lundin, Knut E.A., Jahnsen, Jørgen, Sollid, Ludvig M., and Iversen, Rasmus

Subjects

*B cells, *CELIAC disease, *IMMUNOLOGIC memory, *AUTOANTIBODIES, *PLASMA cells

Abstract

Many antibody responses induced by infection, vaccination or autoimmunity show signs of convergence across individuals with epitope-dependent selection of particular variable region gene segments and complementarity determining region 3 properties. However, not much is known about the relationship between antigen-specific effector cells and antigen-specific precursors present in the naïve B-cell repertoire. Here, we sought to address this relationship in the context of celiac disease, where there is a stereotyped autoantibody response against the enzyme transglutaminase 2 (TG2). By generating TG2-specific monoclonal antibodies from both duodenal plasma cells and circulating naïve B cells, we demonstrate a discord between the naïve TG2-specific repertoire and the cells that are selected for autoantibody production. Hence, the naïve repertoire does not fully reflect the epitope preference and gene usage observed for memory B cells and plasma cells. Instead, distinct naïve B cells that target particular TG2 epitopes appear to be selectively activated at the expense of TG2-binding B cells targeting other epitopes. [Display omitted] • Celiac disease autoantibodies show V gene- and CDR3-dependent targeting of epitopes. • Bias toward N-terminal epitopes is not explained by masking of C-terminal epitopes. • Autoreactive naïve B cells are present in healthy individuals and in celiac patients. • The naïve autoreactive repertoire does not mirror the disease effector repertoire. • Autoreactive B cells targeting particular epitopes are selectively activated. [ABSTRACT FROM AUTHOR]

Published

2024

16. Injection of prototypic celiac anti-transglutaminase 2 antibodies in mice does not cause enteropathy.

Author

Lindstad, Christian B., du Pré, M. Fleur, Stamnaes, Jorunn, and Sollid, Ludvig M.

Subjects

*INTESTINAL diseases, *GLUTELINS, *SOLAR plexus, *IMMUNOGLOBULINS, *CELIAC disease, *SYMPTOMS, *GLUTEN, *GLIADINS

Abstract

Background: Celiac disease is an autoimmune enteropathy driven by dietary intake of gluten proteins. Typical histopathologic features are villous flattening, crypt hyperplasia and infiltration of inflammatory cells in the intestinal epithelium and lamina propria. The disease is hallmarked by the gluten-dependent production of autoantibodies targeting the enzyme transglutaminase 2 (TG2). While these antibodies are specific and sensitive diagnostic markers of the disease, a role in the development of the enteropathy has never been established. Methods: We addressed this question by injecting murine antibodies harboring the variable domains of a prototypic celiac anti-TG2 immunoglobulin into TG2-sufficient and TG2-deficient mice evaluating for celiac enteropathy. Results: We found no histopathologic abnormalities nor clinical signs of disease related to the injection of anti-TG2 IgG or IgA. Conclusions: Our findings do not support a direct role for secreted anti-TG2 antibodies in the development of the celiac enteropathy. [ABSTRACT FROM AUTHOR]

Published

2022

17. Phenotype‐Based Isolation of Antigen‐Specific CD4+ T Cells in Autoimmunity: A Study of Celiac Disease.

Author

Christophersen, Asbjørn, Dahal‐Koirala, Shiva, Chlubnová, Markéta, Jahnsen, Jørgen, Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*CELIAC disease, *T cells, *AUTOIMMUNITY, *PEPTIDES, *CYTOTOXIC T cells, *CD4 antigen, *EPITOPES

Abstract

The pathogenic immune response in celiac disease (CeD) is orchestrated by phenotypically distinct CD4+ T cells that recognize gluten epitopes in the context of disease‐associated HLA‐DQ allotypes. Cells with the same distinct phenotype, but with elusive specificities, are increased across multiple autoimmune conditions. Here, whether sorting of T cells based on their distinct phenotype (Tphe cells) yields gluten‐reactive cells in CeD is tested. The method′s efficiency is benchmarked by parallel isolation of gluten‐reactive T cells (Ttet cells), using HLA‐DQ:gluten peptide tetramers. From gut biopsies of 12 untreated HLA‐DQ2.5+ CeD patients, Ttet+/Tphe+, Ttet−/Tphe+, and Ttet−/Tphe− cells are sorted for single‐cell T‐cell receptor (TCR)‐sequencing (n = 8) and T‐cell clone (TCC)‐generation (n = 5). The generated TCCs are TCR sequenced and tested for their reactivity against deamidated gluten. Gluten‐reactivity is observed in 91.2% of Ttet+/Tphe+ TCCs, 65.3% of Ttet−/Tphe+ TCCs and 0% of Ttet−/Tphe− TCCs. TCR sequencing reveals clonal expansion and sequence sharing across patients, features reflecting antigen‐driven responses. The feasibility to isolate antigen‐specific CD4+ T cells by the sole use of phenotypic markers in CeD outlines a potential avenue for characterizing disease‐driving CD4+ T cells in autoimmune conditions. [ABSTRACT FROM AUTHOR]

Published

2022

18. Structural basis of T cell receptor specificity and cross-reactivity of two HLA-DQ2.5-restricted gluten epitopes in celiac disease.

Author

Ciacchi, Laura, Farenc, Carine, Dahal-Koirala, Shiva, Petersen, Jan, Sollid, Ludvig M., Reid, Hugh H., and Rossjohn, Jamie

Subjects

*CELIAC disease, *EPITOPES, *CROSS reactions (Immunology), *HLA histocompatibility antigens, *SURFACE plasmon resonance, *T cell receptors, *T cells

Abstract

Celiac disease is a T cell-mediated chronic inflammatory condition often characterized by human leukocyte antigen (HLA)-DQ2.5 molecules presenting gluten epitopes derived from wheat, barley, and rye. Although some T cells exhibit cross-reactivity toward distinct gluten epitopes, the structural basis underpinning such cross-reactivity is unclear. Here, we investigated the T-cell receptor specificity and cross-reactivity of two immunodominant wheat gluten epitopes, DQ2.5-glia-α1a (PFPQPELPY) and DQ2.5-glia-ω1 (PFPQPEQPF). We show by surface plasmon resonance that a T-cell receptor alpha variable (TRAV) 4+-T-cell receptor beta variable (TRBV) 29-1+ TCR bound to HLA-DQ2.5-glia-α1a and HLA-DQ2.5-glia-ω1 with similar affinity, whereas a TRAV4- (TRAV9-2+) TCR recognized HLA-DQ2.5-glia-ω1 only. We further determined the crystal structures of the TRAV4+-TRBV29-1+ TCR bound to HLA-DQ2.5-glia-α1a and HLA-DQ2.5-glia-ω1, as well as the structure of an epitope-specific TRAV9-2+-TRBV7-3+ TCRHLA- DQ2.5-glia-ω1 complex. We found that position 7 (p7) of the DQ2.5-glia-α1a and DQ2.5-glia-ω1 epitopes made very limited contacts with the TRAV4+ TCR, thereby explaining the TCR cross-reactivity across these two epitopes. In contrast, within the TRAV9-2+ TCR-HLA-DQ2.5-glia-ω1 ternary complex, the p7-Gln was situated in an electrostatic pocket formed by the hypervariable CDR3β loop of the TCR and Arg70β from HLA-DQ2.5, a polar network which would not be supported by the p7-Leu residue of DQ2.5-glia-α1a. In conclusion, we provide additional insights into the molecular determinants of TCR specificity and cross-reactivity to two closely-related epitopes in celiac disease. [ABSTRACT FROM AUTHOR]

Published

2022

19. Affinity maturation of TCR-like antibodies using phage display guided by structural modeling.

Author

Frick, Rahel, Høydahl, Lene S, Hodnebrug, Ina, Vik, Erik S, Dalhus, Bjørn, Sollid, Ludvig M, Gray, Jeffrey J, Sandlie, Inger, and Løset, Geir Åge

Subjects

*STRUCTURAL models, *MONOCLONAL antibodies, *IMMUNOGLOBULINS, *CELLULAR recognition, *T cells, *CELIAC disease, *GLUTEN

Abstract

TCR-like antibodies represent a unique type of engineered antibodies with specificity toward pHLA, a ligand normally restricted to the sensitive recognition by T cells. Here, we report a phage display-based sequential development path of such antibodies. The strategy goes from initial lead identification through in silico informed CDR engineering in combination with framework engineering for affinity and thermostability optimization, respectively. The strategy allowed the identification of HLA-DQ2.5 gluten peptide-specific TCR-like antibodies with low picomolar affinity. Our method outlines an efficient and general method for development of this promising class of antibodies, which should facilitate their utility including translation to human therapy. [ABSTRACT FROM AUTHOR]

Published

2022

20. Pathogenic T Cells in Celiac Disease Change Phenotype on Gluten Challenge: Implications for T‐Cell‐Directed Therapies.

Author

Christophersen, Asbjørn, Zühlke, Stephanie, Lund, Eivind G., Snir, Omri, Dahal‐Koirala, Shiva, Risnes, Louise Fremgaard, Jahnsen, Jørgen, Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*T cells, *PHENOTYPIC plasticity, *CELIAC disease, *CHEMOKINE receptors, *GLUTEN, *CELL death

Abstract

Gluten‐specific CD4+ T cells being drivers of celiac disease (CeD) are obvious targets for immunotherapy. Little is known about how cell markers harnessed for T‐cell‐directed therapy can change with time and upon activation in CeD and other autoimmune conditions. In‐depth characterization of gluten‐specific CD4+ T cells and CeD‐associated (CD38+ and CD103+) CD8+ and γδ+ T cells in blood of treated CeD patients undergoing a 3 day gluten challenge is reported. The phenotypic profile of gluten‐specific cells changes profoundly with gluten exposure and the cells adopt the profile of gluten‐specific cells in untreated disease (CD147+, CD70+, programmed cell death protein 1 (PD‐1)+, inducible T‐cell costimulator (ICOS)+, CD28+, CD95+, CD38+, and CD161+), yet with some markers being unique for day 6 cells (C‐X‐C chemokine receptor type 6 (CXCR6), CD132, and CD147) and with integrin α4β7, C‐C motif chemokine receptor 9 (CCR9), and CXCR3 being expressed stably at baseline and day 6. Among gluten‐specific CD4+ T cells, 52% are CXCR5+ at baseline, perhaps indicative of germinal‐center reactions, while on day 6 all are CXCR5−. Strikingly, the phenotypic profile of gluten‐specific CD4+ T cells on day 6 largely overlaps with that of CeD‐associated (CD38+ and CD103+) CD8+ and γδ+ T cells. The antigen‐induced shift in phenotype of CD4+ T cells being shared with other disease‐associated T cells is relevant for development of T‐cell‐directed therapies. [ABSTRACT FROM AUTHOR]

Published

2021

21. TG2-gluten complexes as antigens for gluten-specific and transglutaminase-2 specific B cells in celiac disease.

Author

Lindstad, Christian B., Dewan, Alisa E., Stamnaes, Jorunn, Sollid, Ludvig M., and du Pré, M. Fleur

Subjects

*CELIAC disease, *IMMUNOGLOBULIN producing cells, *T cells, *PLASMA cells, *ANTIGENS, *ANTIBODY formation

Abstract

A hallmark of celiac disease is the gluten-dependent production of antibodies specific for deamidated gluten peptides (DGP) and the enzyme transglutaminase 2 (TG2). Both types of antibodies are believed to result from B cells receiving help from gluten-specific CD4+ T cells and differentiating into antibody-producing plasma cells. We have here studied the collaboration between DGP- and TG2-specific B cells with gluten-specific CD4+ T cells using transgenic mice expressing celiac patient-derived T-cell and B-cell receptors, as well as between B-cell transfectants and patient-derived gluten-specific T-cell clones. We show that multivalent TG2-gluten complexes are efficient antigens for both TG2-specific and DGP-specific B cells and allow both types of B cells to receive help from gluten-specific T cells of many different specificities. [ABSTRACT FROM AUTHOR]

Published

2021

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

Author

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

Published

2021

23. Potential impact of celiac disease genetic risk factors on T cell receptor signaling in gluten-specific CD4+ T cells.

Author

Bakker, Olivier B., Ramírez-Sánchez, Aarón D., Borek, Zuzanna A., de Klein, Niek, Li, Yang, Modderman, Rutger, Kooy-Winkelaar, Yvonne, Johannesen, Marie K., Matarese, Filomena, Martens, Joost H. A., Kumar, Vinod, van Bergen, Jeroen, Qiao, Shuo-Wang, Lundin, Knut E. A., Sollid, Ludvig M., Koning, Frits, Wijmenga, Cisca, Withoff, Sebo, and Jonkers, Iris H.

Subjects

*CELIAC disease, *T cell receptors, *CELLULAR signal transduction, *IMMUNE response, *INFLAMMATION

Abstract

Celiac disease is an auto-immune disease in which an immune response to dietary gluten leads to inflammation and subsequent atrophy of small intestinal villi, causing severe bowel discomfort and malabsorption of nutrients. The major instigating factor for the immune response in celiac disease is the activation of gluten-specific CD4+ T cells expressing T cell receptors that recognize gluten peptides presented in the context of HLA-DQ2 and DQ8. Here we provide an in-depth characterization of 28 gluten-specific T cell clones. We assess their transcriptional and epigenetic response to T cell receptor stimulation and link this to genetic factors associated with celiac disease. Gluten-specific T cells have a distinct transcriptional profile that mostly resembles that of Th1 cells but also express cytokines characteristic of other types of T-helper cells. This transcriptional response appears not to be regulated by changes in chromatin state, but rather by early upregulation of transcription factors and non-coding RNAs that likely orchestrate the subsequent activation of genes that play a role in immune pathways. Finally, integration of chromatin and transcription factor binding profiles suggest that genes activated by T cell receptor stimulation of gluten‑specific T cells may be impacted by genetic variation at several genetic loci associated with celiac disease. [ABSTRACT FROM AUTHOR]

Published

2021

24. In Well‐Treated Celiac Patients Low‐Level Mucosal Inflammation Predicts Response to 14‐day Gluten Challenge.

Author

Stamnaes, Jorunn, Stray, Daniel, Stensland, Maria, Sarna, Vikas K., Nyman, Tuula A., Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*INTESTINAL mucosa, *GLUTEN, *PROTEOMICS, *CLINICAL drug trials, *GLUTEN-free diet, *CELIAC disease

Abstract

In celiac disease (CeD), gluten activates adaptive immune cells that cause damage to the small intestinal mucosa. Histological evaluation of intestinal biopsies allows for grading of disease severity. CeD can effectively be treated with a life‐long gluten‐free diet. Gluten challenge of treated CeD patients is used to confirm diagnosis and to test drug efficacy in clinical trials, but patients respond with different magnitudes to the same gluten challenge. In this study of 19 well‐treated CeD patients, proteome analysis of total tissue or isolated epithelial cell compartment from formalin‐fixed paraffin embedded biopsies collected before and after 14‐day gluten challenge demonstrates that patients with strong mucosal response to challenge have signs of ongoing tissue inflammation already before challenge. This low‐level tissue inflammation at baseline is paralleled by increased gluten specific CD4+ T‐cell frequencies in the gut and presence of a low‐level blood inflammatory profile. Thus, apparently well‐treated CeD is frequently not entirely quiescent, with presence of low‐grade inflammation and antigluten immunity in the gut mucosa. Histology assessment alone appears insufficient to judge full recovery and gut mucosal healing of CeD patients. The findings raise a concern whether a seemingly proper gluten‐free diet is able to curb gut inflammation in all CeD patients. [ABSTRACT FROM AUTHOR]

Published

2021

25. Single-cell TCR sequencing of gut intraepithelial γδ T cells reveals a vast and diverse repertoire in celiac disease.

Author

Eggesbø, Linn M., Risnes, Louise F., Neumann, Ralf S., Lundin, Knut E. A., Christophersen, Asbjørn, and Sollid, Ludvig M.

Published

2020

26. A molecular basis for the T cell response in HLA-DQ2.2 mediated celiac disease.

Author

Yi Tian Ting, Dahal-Koirala, Shiva, Hui Shi Keshia Kim, Shuo-Wang Qiao, Neumann, Ralf S., Lundin, Knut E. A., Petersen, Jan, Reid, Hugh H., Sollid, Ludvig M., and Rossjohn, Jamie

Subjects

*CELIAC disease, *T cells, *T cell receptors, *HLA histocompatibility antigens, *PATHOLOGY

Abstract

The highly homologous human leukocyte antigen (HLA)-DQ2 molecules, HLA-DQ2.5 and HLA-DQ2.2, are implicated in the pathogenesis of celiac disease (CeD) by presenting gluten peptides to CD4+ T cells. However, while HLA-DQ2.5 is strongly associated with disease, HLA-DQ2.2 is not, and the molecular basis underpinning this differential disease association is unresolved. We here provide structural evidence for how the single polymorphic residue (HLA-DQ2.5-Tyr22a and HLA-DQ2.2-Phe22a) accounts for HLADQ2.2 additionally requiring gluten epitopes possessing a serine at the P3 position of the peptide. In marked contrast to the biased T cell receptor (TCR) usage associated with HLA-DQ2.5-mediated CeD, we demonstrate with extensive single-cell sequencing that a diverse TCR repertoire enables recognition of the immunodominant HLA-DQ2.2-glut-L1 epitope. The crystal structure of two CeD patient-derived TCR in complex with HLA-DQ2.2 and DQ2.2- glut-L1 (PFSEQEQPV) revealed a docking strategy, and associated interatomic contacts, which was notably distinct from the structures of the TCR:HLA-DQ2.5:gliadin epitope complexes. Accordingly, while the molecular surfaces of the antigen-binding clefts of HLA-DQ2.5 and HLA-DQ2.2 are very similar, differences in the nature of the peptides presented translates to differences in responding T cell repertoires and the nature of engagement of the respective antigen-presenting molecules, which ultimately is associated with differing disease penetrance. [ABSTRACT FROM AUTHOR]

Published

2020

27. Therapeutic and Diagnostic Implications of T Cell Scarring in Celiac Disease and Beyond.

Author

Christophersen, Asbjørn, Risnes, Louise F., Dahal-Koirala, Shiva, and Sollid, Ludvig M.

Subjects

*CELIAC disease, *GLUTELINS, *T cell receptors, *CELL death, *AUTOIMMUNE diseases

Abstract

Few therapeutic and diagnostic tools specifically aim at T cells in autoimmune disorders, but are T cells a narrow target in these diseases? Lessons may be learned from celiac disease (CeD), one of the few autoimmune disorders where the T cell driving antigens are known, i.e. dietary gluten proteins. T cell clonotypes specific to gluten are expanded, persist for decades and express a distinct phenotype in CeD patients. Cells with this phenotype are increased also in other autoimmune conditions. Accordingly, disease-specific CD4+ T cells form an immunological scar in CeD and probably other autoimmune disorders. We discuss approaches how such T cells may be targeted for better treatment and diagnosis via their antigen specificity or via their expression of characteristic phenotypic markers. CD4+ T cells specific for gluten antigen in patients with celiac disease have a narrow phenotype and they persist for decades. Gluten-specific CD4+ T cells appear to drive the development of celiac disease, and CD4+ T cells with overlapping phenotypical and functional properties may drive the pathogenic immune responses of other autoimmune diseases. Antigen-specific T cells could be efficient targets for therapy. Several approaches are conceivable. Disease-driving CD4+ T cells can be silenced by mechanisms of immune deviation or elimination, by reactivation induced cell death or by use of antibodies targeting characteristic phenotypic markers, including activation markers. Further, disease-driving CD4+ T cells can be controlled by agonists of checkpoint inhibition or antagonists of checkpoint stimulation as well as by interfering with homing to specific or inflamed tissue. [ABSTRACT FROM AUTHOR]

Published

2019

28. Cytokine release and gastrointestinal symptoms after gluten challenge in celiac disease.

Author

Goel, Gautam, A-Din, Jason Tye., Shuo-Wang Qiao, Russell, Amy K., Mayassi, Toufic, Ciszewski, Cezary, Sarna, Vikas K., Suyue Wang, Goldstein, Kaela E., Dzuris, John L., Williams, Leslie J., Xavier, Ramnik J., Lundin, Knut E. A., Jabri, Bana, Sollid, Ludvig M., and Anderson, Robert P.

Published

2019

29. Efficient T cell-B cell collaboration guides autoantibody epitope bias and onset of celiac disease.

Author

Iversen, Rasmus, Roy, Bishnudeo, Stamnaes, Jorunn, Høydahl, Lene S., Hnida, Kathrin, Neumann, Ralf S., Korponay-Szabó, Ilma R., Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*CELIAC disease, *T cells, *RECOMBINANT antibodies, *ANTIGEN presentation, *B cells

Abstract

B cells play important roles in autoimmune diseases through autoantibody production, cytokine secretion, or antigen presentation to T cells. In most cases, the contribution of B cells as antigen-presenting cells is not well understood. We have studied the autoantibody response against the enzyme transglutaminase 2 (TG2) in celiac disease patients by generating recombinant antibodies from single gut plasma cells reactive with discrete antigen domains and by undertaking proteomic analysis of anti-TG2 serum antibodies. The majority of the cells recognized epitopes in the N-terminal domain of TG2. Antibodies recognizing C-terminal epitopes interfered with TG2 cross-linking activity, and B cells specific for C-terminal epitopes were inefficient at taking up TG2-gluten complexes for presentation to gluten-specific T cells. The bias toward N-terminal epitopes hence reflects efficient T-B collaboration. Production of antibodies against N-terminal epitopes coincided with clinical onset of disease, suggesting that TG2-reactive B cells with certain epitope specificities could be the main antigen-presenting cells for pathogenic, gluten-specific T cells. The link between B cell epitopes, antigen presentation, and disease onset provides insight into the pathogenic mechanisms of a T cell-mediated autoimmune condition. [ABSTRACT FROM AUTHOR]

Published

2019

30. Epitope Selection for HLA-DQ2 Presentation: Implications for Celiac Disease and Viral Defense.

Author

Shu-Chen Hung, Tieying Hou, Wei Jiang, Nan Wang, Shuo-Wang Qiao, I-Ting Chow, Xiaodan Liu, van der Burg, Sjoerd H., Koelle, David M., Kwok, William W., Sollid, Ludvig M., and Mellins, Elizabeth D.

Subjects

*CELIAC disease, *VIRUS diseases, *HUMAN T cells, *T cells, *CLONE cells

Abstract

We have reported that the major histocompatibility molecule HLA-DQ2 (DQA1*05:01/DQB1*02:01) (DQ2) is relatively resistant to HLA-DM (DM), a peptide exchange catalyst for MHC class II. In this study, we analyzed the role of DQ2/DM interaction in the generation of DQ2-restricted gliadin epitopes, relevant to celiac disease, or DQ2-restricted viral epitopes, relevant to host defense. We used paired human APC, differing in DM expression (DMnull versus DMhigh) or differing by expression of wild-type DQ2, versus a DM-susceptible, DQ2 point mutant DQ2α+53G. The APC pairs were compared for their ability to stimulate human CD4+ T cell clones. Despite higher DQ2 levels, DMhigh APC attenuated T cell responses compared with DMnull APC after intracellular generation of four tested gliadin epitopes. DMhighAPC expressing the DQ2α+53G mutant further suppressed these gliadin-mediated responses. The gliadin epitopes were found to have moderate affinity for DQ2, and even lower affinity for the DQ2 mutant, consistent with DM suppression of their presentation. In contrast, DMhigh APC significantly promoted the presentation of DQ2-restricted epitopes derived intracellularly from inactivated HSV type 2, influenza hemagglutinin, and human papillomavirus E7 protein. When extracellular peptide epitopes were used as Ag, the DQ2 surface levels and peptide affinity were the major regulators of T cell responses. The differential effect of DM on stimulation of the two groups of T cell clones implies differences in DQ2 presentation pathways associated with nonpathogen- and pathogen-derived Ags in vivo. [ABSTRACT FROM AUTHOR]

Published

2019

31. Discriminative T-cell receptor recognition of highly homologous HLA-DQ2-bound gluten epitopes.

Author

Dahal-Koirala, Shiva, Ciacchi, Laura, Petersen, Jan, Risnes, Louise Fremgaard, Neumann, Ralf Stefan, Christophersen, Asbjørn, Lundin, Knut E. A., Reid, Hugh H., Shuo-Wang Qiao, Rossjohn, Jamie, and Sollid, Ludvig M.

Subjects

*T-cell receptor genes, *EPITOPES, *CELIAC disease, *TETRAMERS (Oligomers), *CRYSTAL structure

Abstract

Celiac disease (CeD) provides an opportunity to study the specificity underlying human T-cell responses to an array of similar epitopes presented by the same human leukocyte antigen II (HLA-II) molecule. Here, we investigated T-cell responses to the two immunodominant and highly homologous HLA-DQ2.5–restricted gluten epitopes, DQ2.5-glia-α1a (PFPQPELPY) and DQ2.5-glia-ω1 (PFPQPEQPF). Using HLA-DQ2.5–DQ2.5-glia-α1a and HLA-DQ2.5–DQ2.5-glia-ω1 tetramers and single-cell αβ T-cell receptor (TCR) sequencing, we observed that despite similarity in biased variable-gene usage in the TCR repertoire responding to these nearly identical peptide–HLA-II complexes, most of the T cells are specific for either of the two epitopes. To understand the molecular basis of this exquisite fine specificity, we undertook Ala substitution assays revealing that the p7 residue (Leu/Gln) is critical for specific epitope recognition by both DQ2.5-glia-α1a– and DQ2.5-glia-ω1–reactive T-cell clones. We determined high-resolution binary crystal structures of HLA-DQ2.5 bound to DQ2.5-glia-α1a (2.0 Å) and DQ2.5-glia-ω1 (2.6 Å). These structures disclosed that differences around the p7 residue subtly alter the neighboring substructure and electrostatic properties of the HLA-DQ2.5–peptide complex, providing the fine specificity underlying the responses against these two highly homologous gluten epitopes. This study underscores the ability of TCRs to recognize subtle differences in the peptide–HLA-II landscape in a human disease setting. [ABSTRACT FROM AUTHOR]

Published

2019

32. Disease-driving CD4+ T cell clonotypes persist for decades in celiac disease.

Author

Risnes, Louise F., Christophersen, Asbjørn, Dahal-Koirala, Shiva, Neumann, Ralf S., Sandve, Geir K., Sarna, Vikas K., Lundin, Knut E. A., Shuo-Wang Qiao, Sollid, Ludvig M., Lundin, Knut Ea, and Qiao, Shuo-Wang

Subjects

*CELIAC disease, *CD4 antigen, *T cells, *HLA histocompatibility antigens, *GLUTEN, *PHYSIOLOGY, *CELL receptors, *COMPARATIVE studies, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *HLA-B27 antigen, *EVALUATION research

Abstract

Little is known about the repertoire dynamics and persistence of pathogenic T cells in HLA-associated disorders. In celiac disease, a disorder with a strong association with certain HLA-DQ allotypes, presumed pathogenic T cells can be visualized and isolated with HLA-DQ:gluten tetramers, thereby enabling further characterization. Single and bulk populations of HLA-DQ:gluten tetramer-sorted CD4+ T cells were analyzed by high-throughput DNA sequencing of rearranged TCR-α and -β genes. Blood and gut biopsy samples from 21 celiac disease patients, taken at various stages of disease and in intervals of weeks to decades apart, were examined. Persistence of the same clonotypes was seen in both compartments over decades, with up to 53% overlap between samples obtained 16 to 28 years apart. Further, we observed that the recall response following oral gluten challenge was dominated by preexisting CD4+ T cell clonotypes. Public features were frequent among gluten-specific T cells, as 10% of TCR-α, TCR-β, or paired TCR-αβ amino acid sequences of total 1813 TCRs generated from 17 patients were observed in 2 or more patients. In established celiac disease, the T cell clonotypes that recognize gluten are persistent for decades, making up fixed repertoires that prevalently exhibit public features. These T cells represent an attractive therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2018

33. High-Throughput Single-Cell Analysis of B Cell Receptor Usage among Autoantigen-Specific Plasma Cells in Celiac Disease.

Author

Roy, Bishnudeo, Snir, Omri, Iversen, Rasmus, Sollid, Ludvig M., Neumann, Ralf S., Sandve, Geir Kjetil, and Lundin, Knut E. A.

Subjects

*B cell receptors, *HUMORAL immunity, *PLASMA cells, *CELIAC disease, *AUTOANTIGENS, *AUTOIMMUNE diseases

Abstract

Characterization of Ag-specific BCR repertoires is essential for understanding disease mechanisms involving humoral immunity. This is optimally done by interrogation of paired H chain V region (VH) and L chain V region (VL) sequences of individual and Ag-specific B cells. By applying single-cell high-throughput sequencing on gut lesion plasma cells (PCs), we have analyzed the transglutaminase 2 (TG2)-specific VH:VL autoantibody repertoire of celiac disease (CD) patients. Autoantibodies against TG2 are a hallmark of CD, and anti-TG2 IgA-producing gut PCs accumulate in patients upon gluten ingestion. Altogether, we analyzed paired VH and VL sequences of 1482 TG2-specific and 1421 non-TG2-specific gut PCs from 10 CD patients. Among TG2-specific PCs, we observed a striking bias in IGHV and IGKV/IGLV gene usage, as well as pairing preferences with a particular presence of the IGHV5-51:IGKV1-5 pair. Selective and biased VH:VL pairing was particularly evident among expanded clones. In general, TG2-specific PCs had lower numbers of mutations both in VH and VL genes than in non-TG2-specific PCs. TG2-specific PCs using IGHV5-51 had particularly few mutations. Importantly, VL segments paired with IGHV5-51 displayed proportionally low mutation numbers, suggesting that the low mutation rate among IGHV5-51 PCs is dictated by the BCR specificity. Finally, we observed selective amino acid changes in VH and VL and striking CDR3 length and J segment selection among TG2-specific IGHV5-51: IGKV1-5 pairs. Hence this study reveals features of a disease- and Ag-specific autoantibody repertoire with preferred VH:VL usage and pairings, limited mutations, clonal dominance, and selection of particular CDR3 sequences. [ABSTRACT FROM AUTHOR]

Published

2017

34. Unraveling the structural basis for the unusually rich association of human leukocyte antigen DQ2.5 with class-II-associated invariant chain peptides.

Author

Nguyen, Thanh-Binh, Jayaraman, Priya, Bergseng, Elin, Madhusudhan, M. S., Chu-Young Kim, and Sollid, Ludvig M.

Subjects

*HLA histocompatibility antigens, *HISTOCOMPATIBILITY, *TYPE 1 diabetes, *SENSITIVITY & specificity (Statistics), *PHENOTYPES

Abstract

Human leukocyte antigen (HLA)-DQ2.5 (DQA1*05/DQB1*02) is a class-II major histocompatibility complex protein associated with both type 1 diabetes and celiac disease. One unusual feature of DQ2.5 is its high class-II-associated invariant chain peptide (CLIP) content. Moreover, HLA-DQ2.5 preferentially binds the non-canonical CLIP2 over the canonical CLIP1. To better understand the structural basis of HLA-DQ2.5's unusual CLIP association characteristics, better insight into the HLADQ2.5 ∙CLIP complex structures is required. To this end, we determined the X-ray crystal structure of the HLA-DQ2.5∙ CLIP1 and HLA-DQ2.5∙CLIP2 complexes at 2.73 and 2.20 Å, respectively. We found that HLA-DQ2.5 has an unusually large P4 pocket and a positively charged peptide-binding groove that together promote preferential binding of CLIP2 over CLIP1. An α9-α22-α24-α31-β86-β90 hydrogen bond network located at the bottom of the peptide-binding groove, spanning from the P1 to P4 pockets, renders the residues in this region relatively immobile. This hydrogen bond network, along with a deletion mutation at α53, may lead to HLA-DM insensitivity in HLA-DQ2.5. A molecular dynamics simulation experiment reported here and recent biochemical studies by others support this hypothesis. The diminished HLA-DM sensitivity is the likely reason for the CLIP-rich phenotype of HLA-DQ2.5. [ABSTRACT FROM AUTHOR]

Published

2017

35. Epitope-dependent Functional Effects of Celiac Disease Autoantibodies on Transglutaminase 2.

Author

Hnida, Kathrin, Stamnaes, Jorunn, du Pré, M. Fleur, Mysling, Simon, Jørgensen, Thomas J. D., Sollid, Ludvig M., and Iversen, Rasmus

Subjects

*CELIAC disease, *EPITOPES, *AUTOANTIBODIES, *TRANSGLUTAMINASES, *PROTEIN crosslinking, *CLINICAL immunology

Abstract

Transglutaminase 2 (TG2) is a Ca2+-dependent cross-linking enzyme involved in the pathogenesis of CD. We have previously characterized a panel of anti-TG2 mAbs generated from gut plasma cells of celiac patients and identified four epitopes (epitopes 1-4) located in the N-terminal part of TG2. Binding of the mAbs induced allosteric changes in TG2. Thus, we aimed to determine whether these mAbs could influence enzymatic activity through modulation of TG2 susceptibility to oxidative inactivation and Ca2+ affinity. All tested epitope 1 mAbs, as well as 679-14-D04, which recognizes a previously uncharacterized epitope, prevented oxidative inactivation and increased Ca2 sensitivity of TG2. We have identified crucial residues for binding of 679-14-D04 located within a Ca2+ binding site. Epitope 1 mAbs and 679-14-D04, although recognizing separate epitopes, behaved similarly when assessing their effect on TG2 conformation, suggesting that the shared effects on TG2 function can be explained by induction of the same conformational changes. None of the mAbs targeting other epitopes showed these effects, but epitope 2 mAbs reduced the rate of TG2-catalyzed reactions. Collectively, these effects could be relevant to the pathogenesis of CD. In A20 B cells transduced with TG2-specific B-cell receptor, epitope 2-expressing cells had poorer uptake of TG2-gluten complexes and were less efficient in gluten epitope presentation to T cells than cells expressing an epitope 1 receptor. Thus, the ability of epitope 1-targeting B cells to keep TG2 active and protected from oxidation might explain why generation of epitope 1-targeting plasma cells seems to be favored in celiac patients. [ABSTRACT FROM AUTHOR]

Published

2016

36. Transglutaminase 2 strongly binds to an extracellular matrix component other than fibronectin via its second C-terminal beta-barrel domain.

Author

Stamnaes, Jorunn, Cardoso, Inês, Iversen, Rasmus, and Sollid, Ludvig M.

Subjects

*TRANSGLUTAMINASES, *EXTRACELLULAR matrix, *FIBRONECTIN-binding proteins, *CELIAC disease, *AUTOANTIBODIES, *N-terminal residues

Abstract

Transglutaminase 2 (TG2) is a ubiquitous crosslinking enzyme present in both intra- and extracellular in many cell types and tissues. TG2 is upregulated upon cellular stress or injury, and extracellular TG2 is implicated in several human diseases, including celiac disease. However, incomplete knowledge about extracellular TG2 biology limits our understanding of how TG2 is involved in disease. Here, we demonstrate that binding of TG2 to the ECM of small intestinal tissue sections is the sum of binding to fibronectin (FN) via its N-terminal domain and binding to an abundant, novel extracellular matrix (ECM) interaction partner via its second C-terminal beta-barrel domain. The latter interaction dominates and gives rise to the characteristic reticular staining pattern of extracellular TG2. Of relevance for celiac disease, we show that self-multimerized TG2 does not efficiently deposit in the intestinal ECM, and TG2 complexes may thus become free-floating antigens in tissues in contrast to monomeric TG2 that would readily become sequestered by the ECM. Upon injection of monoclonal antibody targeting the FN-binding site, we observe antibody deposition on extracellular TG2 in cryosections, suggesting that the FN-binding site of TG2 is exposed in vivo. This would explain how and why celiac autoantibodies recognizing the FN-binding site of TG2 can bind TG2 in vitro, in situ as well as in vivo. [ABSTRACT FROM AUTHOR]

Published

2016

37. Pathogenic T Cells in Celiac Disease Change Phenotype on Gluten Challenge: Implications for T‐Cell‐Directed Therapies.

Author

Christophersen, Asbjørn, Zühlke, Stephanie, Lund, Eivind G., Snir, Omri, Dahal‐Koirala, Shiva, Risnes, Louise Fremgaard, Jahnsen, Jørgen, Lundin, Knut E. A., and Sollid, Ludvig M.

Subjects

*CELIAC disease, *PHENOTYPIC plasticity, *GLUTEN, *DEFECATION, *T cells

Abstract

Pathogenic T Cells in Celiac Disease Change Phenotype on Gluten Challenge: Implications for T-Cell-Directed Therapies Grey background indicates time period of gluten ingestion. gl The authors apologize for any inconvenience caused. Median of symptoms expressed in a VAS score (maximal value 100 mm) for the categories Pain, Bloating, Flatulence, Nausea, Satisfaction with defecation and Total complaints and GSRS questionnaire for the categories Pain, Bloating, Constipation, Diarrhea and Satiety in total n = 17 celiac disease patients undergoing a 3-day gluten challenge. [Extracted from the article]

Published

2022

38. Healthy HLA-DQ2.5+ Subjects Lack Regulatory and Memory T Cells Specific for Immunodominant Gluten Epitopes of Celiac Disease.

Author

Christophersen, Asbjørn, Risnes, Louise F., Bergseng, Elin, Lundin, Knut E. A., Sollid, Ludvig M., and Shuo-Wang Qiao

Subjects

*CELIAC disease, *T cells, *GLUTEN, *TETRAMERS (Oligomers), *EPITOPES

Abstract

Celiac disease (CD) is an HLA-associated disorder characterized by a harmful T cell response to dietary gluten. It is not understood why most individuals who carry CD-associated HLA molecules, such as HLA-DQ2.5, do not develop CD despite continuous gluten exposure. In this study, we have used tetramers of HLA-DQ2.5 bound with immunodominant gluten epitopes to explore whether HLA-DQ2.5+ healthy individuals mount a specific CD4+ T cell response to gluten. We found that gluten tetramer-binding memory cells were rare in blood of healthy individuals. These cells showed lower tetramer-binding intensity and no signs of biased TCR usage compared with gluten tetramer-binding memory T cells from patients. After sorting and in vitro expansion, only 18% of the tetramer-binding memory cells from healthy subjects versus 79% in CD patients were gluten-reactive upon tetramer restaining. Further, T cell clones of tetramer-sorted memory cells of healthy individuals showed lower gluten-specific proliferative responses compared with those of CD patients, indicating that tetramer-binding memory cells in healthy control subjects may be cross-reactive T cells. In duodenal biopsy specimens of healthy control subjects, CD4+ T cells were determined not to be gluten reactive. Finally, gluten tetramer-binding cells of healthy individuals did not coexpress regulatory T cell markers (Foxp3+ CD25+) and cultured T cell clones did not express a cytokine profile that indicated immune-dampening properties. The results demonstrate that healthy HLA-DQ2.5+ individuals do not mount a T cell response to immunodominant gluten epitopes of CD. [ABSTRACT FROM AUTHOR]

Published

2016

39. Igs as Substrates for Transglutaminase 2: Implications for Autoantibody Production in Celiac Disease.

Author

Iversen, Rasmus, du Pré, M. Fleur, Di Niro, Roberto, and Sollid, Ludvig M.

Subjects

*TRANSGLUTAMINASES, *IMMUNOGLOBULINS, *CELIAC disease treatment, *T cell receptors, *DEAMINATION

Abstract

Autoantibodies specific for the enzyme transglutaminase 2 (TG2) are a hallmark of the gluten-sensitive enteropathy celiac disease. Production of the Abs is strictly dependent on exposure to dietary gluten proteins, thus raising the question how a foreign Ag (gluten) can induce an autoimmune response. It has been suggested that TG2-reactive B cells are activated by gluten-reactive T cells following receptor-mediated uptake of TG2-gluten complexes. In this study, we propose a revised model that is based on the ability of the BCR to serve as a substrate to TG2 and become cross-linked to gluten-derived peptides. We show that TG2-speciflc IgD molecules are preferred in the reaction and that binding of TG2 via a common epitope targeted by cells using the IgH variable gene segment (IGHV)5-51 results in more efficient cross-linking. Based on these findings we hypothesize that IgD-expressing B cells using IGHV5-51 are preferentially activated, and we suggest that this property can explain the previously reported low number of somatic mutations as well as the overrepresentation of IGHV5-51 among TG2-specific plasma cells in the celiac lesion. The model also couples gluten peptide uptake by TG2-reactive B cells directly to peptide deamidation, which is necessary for the activation of gluten-reactive T cells. It thereby provides a link between gluten deamidation, T cell activation, and the production of TG2-specific Abs. These are all key events in the development of celiac disease, and by connecting them the model may explain why the same enzyme that catalyzes gluten deamidation is also an autoantigen, something that is hardly coincidental. [ABSTRACT FROM AUTHOR]

Published

2015

40. Structural basis for antigen recognition by transglutaminase 2-specific autoantibodies in celiac disease.

Author

Xi Chen, Hnida, Kathrin, Graewert, Melissa Ann, Andersen, Jan Terje, Iversen, Rasmus, Tuukkanen, Anne, Svergun, Dmitri, and Sollid, Ludvig M.

Subjects

*TRANSGLUTAMINASES, *AUTOANTIBODIES, *CELIAC disease, *ANTIGENS, *X-ray scattering

Abstract

Antibodies to the autoantigen transglutaminase 2 (TG2) are a hallmark of celiac disease. We have studied the interaction between TG2 and an anti-TG2 antibody (679-14-E06) derived from a single gut IgA plasma cell of a celiac disease patient. The antibody recognizes one of four identified epitopes targeted by antibodies of plasma cells of the disease lesion. The binding interface was identified by small angle X-ray scattering, ab initio and rigid body modeling using the known crystal structure of TG2 and the crystal structure of the antibody Fab fragment, which was solved at 2.4 Å resolution. The result was confirmed by testing binding of the antibody to TG2 mutants by ELISA and surface plasmon resonance. TG2 residues R116 and H134 were identified to be critical for binding of 679-14-E06 as well as other epitope 1 antibodies. In contrast, antibodies directed toward the two other main epitopes (epitopes 2 and 3) were not affected by these mutations. Molecular dynamics simulations suggest interactions of 679-14-E06 with the N-terminal domain of TG2 via the CDR2 and CDR3 loops of the heavy chain and the CDR2 loop of the light chain. In addition there were contacts of the framework 3 region of the heavy chain with the catalytic domain of TG2. The results provide an explanation for the biased usage of certain heavy and light chain gene segments by epitope 1-specific antibodies in celiac disease. [ABSTRACT FROM AUTHOR]

Published

2015

41. Enhanced B-Cell Receptor Recognition of the Autoantigen Transglutaminase 2 by Efficient Catalytic Self-Multimerization.

Author

Stamnaes, Jorunn, Iversen, Rasmus, du Pré, M. Fleur, Chen, Xi, and Sollid, Ludvig M.

Subjects

*CELIAC disease, *INTESTINAL diseases, *B cell receptors, *AUTOANTIGENS, *TRANSGLUTAMINASES, *PROTEIN-protein interactions, *CATALYTIC activity, *GENETIC regulation

Abstract

A hallmark of the gluten-driven enteropathy celiac disease is autoantibody production towards the enzyme transglutaminase 2 (TG2) that catalyzes the formation of covalent protein-protein cross-links. Activation of TG2-specific B cells likely involves gluten-specific CD4 T cells as production of the antibodies is dependent on disease-associated HLA-DQ allotypes and dietary intake of gluten. IgA plasma cells producing TG2 antibodies with few mutations are abundant in the celiac gut lesion. These plasma cells and serum antibodies to TG2 drop rapidly after initiation of a gluten-free diet, suggestive of extrafollicular responses or germinal center reactions of short duration. High antigen avidity is known to promote such responses, and is also important for breakage of self-tolerance. We here inquired whether TG2 avidity could be a feature relevant to celiac disease. Using recombinant enzyme we show by dynamic light scattering and gel electrophoresis that TG2 efficiently utilizes itself as a substrate due to conformation-dependent homotypic association, which involves the C-terminal domains of the enzyme. This leads to the formation of covalently linked TG2 multimers. The presence of exogenous substrate such as gluten peptide does not inhibit TG2 self-cross-linking, but rather results in formation of TG2-TG2-gluten complexes. The celiac disease autoantibody epitopes, clustered in the N-terminal part of TG2, are conserved in the TG2-multimers as determined by mass spectrometry and immunoprecipitation analysis. TG2 multimers are superior to TG2 monomer in activating A20 B cells transduced with TG2-specific B-cell receptor, and uptake of TG2-TG2-gluten multimers leads to efficient activation of gluten-specific T cells. Efficient catalytic self-multimerization of TG2 and generation of multivalent TG2 antigen decorated with gluten peptides suggest a mechanism by which self-reactive B cells are activated to give abundant numbers of plasma cells in celiac disease. Importantly, high avidity of the antigen could explain why TG2-specific plasma cells show signs of an extrafollicular generation pathway. [ABSTRACT FROM AUTHOR]

Published

2015

42. Response to: "Some considerations about γδ and CD8+ T-cell responses in blood after gluten challenge in treated celiac disease".

Author

Risnes, Louise F., Eggesbø, Linn M., Christophersen, Asbjørn, and Sollid, Ludvig M.

Published

2021

43. Analysis of Celiac Disease Autoreactive Gut Plasma Cells and Their Corresponding Memory Compartment in Peripheral Blood Using High-Throughput Sequencing.

Author

Snir, Omri, Mesin, Luka, Gidoni, Moriah, Lundin, Knut E. A., Yaari, Gur, and Sollid, Ludvig M.

Subjects

*IMMUNOGLOBULIN A, *PLASMA cells, *TRANSGLUTAMINASES, *CELIAC disease, *GLUTEN-free diet, *B cells

Abstract

Autoreactive IgA plasma cells (PCs) specific for the enzyme transglutaminase 2 (TG2) are abundant in the small intestine of patients with active celiac disease (CD), and their number drops in patients treated by dietary gluten elimination. Little is known about their characteristics and their role in the disease. In this study, using high-throughput sequencing of the IgH V region (IGHV) genes, we have studied features of TG2-specific PCs and their related B cell clones in peripheral blood. We found that TG2-specific PCs from both untreated and treated patients have acquired lower number of somatic hypermutation and used focused IGHV repertoire with overrepresentation of the IGHV3-48, IGHV4-59, IGHVS-10-1, and IGHV5-51 gene segments. Furthermore, these PCs were clonally expanded and showed signs of affinity maturation. Lineage trees demonstrated shared clones between gut PCs and blood memory B cells, primarily IgAs. Some trees also involved IgG cells, suggesting that anti-TG2 IgA and IgG responses are related. Similarly to TG2-specific PCs, clonally related memory IgA B cells of blood showed lower mutation rates with biased usage of IGHV3-48 and IGHV5-51. Such memory cells were rare in peripheral blood, yet detectable in most patients assessed by production of anti-TG2 Abs in vitro following stimulation of cells from patients who had been on a long-term gluten-free diet. Thus, the Ab response to TG2 in CD, while maintaining its IGHV gene usage, is dynamically regulated in response to gluten exposure with a low degree of maintenance at both PC and memory B cell levels in patients in remission. [ABSTRACT FROM AUTHOR]

Published

2015

44. Transglutaminase 2 interactions with extracellular matrix proteins as probed with celiac disease autoantibodies.

Author

Cardoso, Inês, Stamnaes, Jorunn, Andersen, Jan Terje, Melino, Gerry, Iversen, Rasmus, and Sollid, Ludvig M.

Subjects

*TRANSGLUTAMINASES, *EXTRACELLULAR matrix proteins, *CELIAC disease, *EPITOPES, *IMMUNOGENETICS

Abstract

Transglutaminases have been implicated in various human diseases. A prominent example is the involvement of transglutaminase 2 ( TG2) in the gluten-sensitive enteropathy celiac disease, where the enzyme is both the target of autoantibodies and responsible for the generation of immunogenic gluten epitopes. Here, we aimed to characterize the microenvironment of TG2 in the extracellular matrix ( ECM) in order to gain insights into the antigenic structures that are recognized by autoantibodies in celiac disease. A panel of TG2-specific mAbs established from gut plasma cells of celiac disease patients was employed as probes to characterize the interactions between TG2 and ECM constituents. With immunofluorescence staining, microplate protein-binding and surface plasmon resonance assays, we found that the main epitope (epitope 1) recognized by TG2-specific gut plasma cells overlaps with the fibronectin ( FN)-binding site of TG2. Furthermore, we found that the same TG2 amino acids that are involved in binding of epitope 1 mAbs are also important for efficient binding of FN. Notably, epitope 1 mAbs recognize TG2 in tissue sections, suggesting that some TG2 in the extracellular matrix has interaction partners in addition to FN. We demonstrate that collagen VI is a strong candidate, on the basis of its tissue expression pattern and ability to bind TG2. Collagen VI may thus serve as a matrix for deposition of TG2 in a context that can also be recognized by epitope 1-targeting autoantibodies. [ABSTRACT FROM AUTHOR]

Published

2015

45. Coeliac disease - from genetic and immunological studies to clinical applications.

Author

Lundin, Knut E. A., Qiao, Shuo-Wang, Snir, Omri, and Sollid, Ludvig M.

Subjects

*CELIAC disease, *LEUCOCYTES, *GLUTEN, *PEPTIDES, *INTESTINAL diseases

Abstract

Coeliac disease is a common and important gastrointestinal disease. It affects at least 1%, most Western European populations and in Nordic countries it is even more frequent. It is strongly associated with certain Human Leukocyte Antigen-DQ genes and triggered by ingestion of wheat gluten and related cereals from rye and barley. The diagnosis relies on a combination of clinical signs, serology and small intestinal biopsy. Work during the last couple of decades has shown that gluten-specific, Human Leukocyte Antigen-DQ-restricted T-cells in the intestinal mucosa are of paramount importance in the disease process. The gluten peptides are chemically modified by the endogenous enzyme transglutaminase 2, the same enzyme that serves as target in today's sensitive serological tests for coeliac disease. The increasing knowledge on the disease process allows for development of improved diagnosis, patient care and new treatment modalities. [ABSTRACT FROM AUTHOR]

Published

2015

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

Author

Iversen, Rasmus, Mysling, Simon, Hnida, Kathrin, Jørgensen, Thomas J. D., and Sollid, Ludvig M.

Subjects

*AUTOANTIBODIES, *EPITOPES, *GLUTEN allergenicity, *CELIAC disease, *DEUTERIUM, *MONOCLONAL antibodies, *PLASMA cells

Abstract

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 Ca2+ 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. [ABSTRACT FROM AUTHOR]

Published

2014

47. HLA-DQ Molecules as Affinity Matrix for Identification of Gluten T Cell Epitopes.

Author

Dørum, Siri, Bodd, Michael, Fallang, Lars-Egil, Bergseng, Elin, Christophersen, Asbjørn, Johannesen, Marie K., Shuo-Wang Qiao, Stamnaes, Jorunn, de Souza, Gustavo A., and Sollid, Ludvig M.

Subjects

*MAJOR histocompatibility complex, *EPITOPES, *CELIAC disease, *T cells, *HLA histocompatibility antigens, *GLUTEN

Abstract

Even though MHC class II is a dominant susceptibility factor for many diseases, culprit T cell epitopes presented by disease-associated MHC molecules remain largely elusive. T cells of celiac disease lesions recognize cereal gluten epitopes presented by the disease-associated HLA molecules DQ2.5, DQ2.2, or DQ8. Employing celiac disease and complex gluten Ag digests as a model, we tested the feasibility of using DQ2.5 and DQ2.2 as an affinity matrix for identification of disease-relevant T cell epitopes. Known gluten T cell epitope peptides were enriched by DQ2.5, whereas a different set of peptides was enriched by DQ2.2. Of 86 DQ2.2-enriched peptides, four core sequences dominated. One of these core sequences is a previously known epitope and two others are novel epitopes. The study provides insight into the selection of gluten epitopes by DQ2.2. Furthermore, the approach presented is relevant for epitope identification in other MHC class II-associated disorders. [ABSTRACT FROM AUTHOR]

Published

2014

48. Treatment of both native and deamidated gluten peptides with an endo-peptidase from Aspergillus niger prevents stimulation of gut-derived gluten-reactive T cells from either children or adults with celiac disease.

Author

Toft-Hansen, Henrik, Rasmussen, Karina S., Staal, Anne, Roggen, Erwin L., Sollid, Ludvig M., Lillevang, Søren T., Barington, Torben, and Husby, Steffen

Subjects

*GLUTEN, *PEPTIDES, *ASPERGILLUS niger, *CELIAC disease, *NEURAL stimulation, *T cells

Abstract

Celiac disease (CD) is characterized by an inappropriate immunological reaction against gluten driven by gluten-specific CD4 + T cells. We screened 25 proteases and tested 10 for their potential to degrade gluten in vitro. Five proteases were further tested for their ability to prevent the proliferative response by a gluten-specific CD4 + T cell clone and seven gluten-reactive T cell lines to protease-digested gluten peptides. A proline-specific endo-peptidase from Aspergillus niger (AnP2) was particularly efficient at diminishing proliferation after stimulation with cleaved antigen, and could completely block the response against both native and deamidated gluten peptides. We found that AnP2 was efficient down to a 1:64 protease:substrate ratio (w:w). When AnP2 was tested in assays using seven gluten-reactive T cell lines from individual CD patients (three adults and four children), the response to gluten was diminished in all cases. Our study indicates a therapeutic benefit of AnP2 to CD patients. [ABSTRACT FROM AUTHOR]

Published

2014

49. Multivalent pIX phage display selects for distinct and improved antibody properties.

Author

Høydahl, Lene S., Nilssen, Nicolay R., Gunnarsen, Kristin S., Pré, M. Fleur du, Iversen, Rasmus, Roos, Norbert, Chen, Xi, Michaelsen, Terje E., Sollid, Ludvig M., Sandlie, Inger, and Løset, Geir Å.

Abstract

Phage display screening readily allows for the identification of a multitude of antibody specificities, but to identify optimal lead candidates remains a challenge. Here, we direct the antibody-capsid fusion away from the signal sequence-dependent secretory SEC pathway in E. coli by utilizing the intrinsic signal sequence-independent property of pIX to obtain virion integration. This approach was combined with the use of an engineered helper phage known to improve antibody pIX display and retrieval. By direct comparison with pIII display, we demonstrate that antibody display using this pIX system translates into substantially improved retrieval of desired specificities with favorable biophysical properties in de novo selection. We show that the effect was due to less E. coli host toxicity during phage propagation conferred by the lack of a signal sequence. This pIX combinatorial display platform provides a generic alternative route for obtaining good binders with high stability and may thus find broad applicability. [ABSTRACT FROM AUTHOR]

Published

2016

50. Gluten-specific antibodies of celiac disease gut plasma cells recognize long proteolytic fragments that typically harbor T-cell epitopes.

Author

Dørum, Siri, Steinsbø, Øyvind, Bergseng, Elin, Arntzen, Magnus Ø., de Souza, Gustavo A., and Sollid, Ludvig M.

Published

2016