A novel unconventional T cell population enriched in Crohn’s disease

Rosati, Elisa; Martini, Gabriela Rios; Pogorelyy, Mikhail V.; Minervina, Anastasia A.; Degenhardt, Frauke; Wendorff, Mareike; Sarı, Soner; Mayr, Gabriele; Fazio, Antonella; Dowds, C. Marie; Hauser, Charlotte; Tran, Florian; Schönfels, Witigo von; Pochhammer, Julius; Salnikova, Maria A.; Jaeckel, Charlot; Gigla, Johannes Boy; Sabet, Sanaz Sedghpour; Hübenthal, Matthias; Schiminsky, Esther; Schreiber, Stefan; Rosenstiel, Philip; Scheffold, Alexander; Lieb, Wolfgang; Bokemeyer, Bernd; Witte, Maria; Aden, Konrad; Hendricks, Alexander; Schafmayer, Clemens; Egberts, Jan-Hendrick; Mamedov, Ilgar Z.; Bächer, Petra; Franke, André

doi:10.1136/gutjnl-2021-325373

Cited by 29 publications

(32 citation statements)

References 50 publications

(95 reference statements)

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“…Only significant p values from a t-test with Holm method for multiple testing correction are shown (*<0.05, **<0.01, ***<0.001, ****<0.0001). (G.) Frequency of CAITlike NKT type II TCRs from Almeida et al (attached to a large cluster on figure 1A) and non-CAIT like NKT type II TCRs in Crohn’s disease and healthy cohorts from Rosati et al 1. Only significant p value (****<0.0001) from a Mann-Whitney U-test is shown.…”

Section: Mainmentioning

confidence: 97%

“…To further investigate the possible role of NKT type II cells in CD, we searched all NKT type II sequences reported in Almeida et al in our previously published TCR data from patients with CD and healthy controls 1 3. Only TCRs from NKT type II cells with the characteristic CAIT TCRalpha chain motif showed significant enrichment in patients with CD, while other TCRs were found in comparable amounts in patients and controls (figure 1G).…”

Section: Mainmentioning

confidence: 99%

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Crohn’s-associated invariant T cells (CAITs) recognise small sulfonate molecules on CD1d

Minervina

Pogorelyy

Paysen

et al. 2022

Gut

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Figure 1 Comparison of natural killer T (NKT) type II and Crohn's-associated invariant T (CAIT) cells. (A) Sequence similarity analysis of NKT type II 2 3 and CAIT T cell receptors (TCRs). Each node corresponds to the unique alpha/beta TCR sequence and edges connect highly similar TCRs (tcrdist metric<150). Larger nodes indicate TCRs used for cloning. TCRdist sequence logos for TCRalpha and TCRbeta chains of TCRs from the cluster are shown at the bottom. (B). Genomic segments and amino acid CDR3 sequences of TCRs picked for experimental validation. Red font indicates differences in CDR3 regions. (C). Chemical structures of phenyl-pentamethyldihydrobenzofuransulfonate (PPBF) and chlorophenyil-pentamethyld ihydrobenzofuransulfonate (ClPPBF). (D.) Gating strategy and representative flow plots for pentamethylbenzofuransulfonates (PBFs) stimulation experiment. (E). Frequency of activated cells reactive to PPBF (top) and ClPPBF (bottom). Only significant p values from a T-test with Holm method for multiple testing correction are shown (*<0.05, **<0.01, ***<0.001, ****<0.0001). (F). Anti-CD1d antibody prevents activation of all four cell lines with PPBF (top) and ClPPBF (bottom). Only significant p values from a t-test with Holm method for multiple testing correction are shown (*<0.05, **<0.01, ***<0.001, ****<0.0001). (G.) Frequency of CAITlike NKT type II TCRs from Almeida et al (attached to a large cluster on figure 1A) and non-CAIT like NKT type II TCRs in Crohn's disease and healthy cohorts from Rosati et al . 1 Only significant p value (****<0.0001) from a Mann-Whitney U-test is shown.

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Section: Mainmentioning

confidence: 97%

Section: Mainmentioning

confidence: 99%

Crohn’s-associated invariant T cells (CAITs) recognise small sulfonate molecules on CD1d

Minervina

Pogorelyy

Paysen

et al. 2022

Gut

Self Cite

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“…The pattern and dynamics of these individual immune cells in liver fibrosis contribute to elucidating the protective mechanism of TCR in the chronic liver injury response ( 36 ). The TCRα chain is significantly enriched in the blood of patients with Crohn’s disease (CD), particularly in CD8+ T cell populations, whereas the potential effects of Crohn’s associated invariant T-cell subpopulations on CD remains to be elucidated ( 37 ). A total of 1650 glutamic acid decarboxylase 65-kilodalton isoform (GAD65)-specific CD4(+) T cells were isolated and 1003 different TCRs were identified in the peripheral blood of 6 patients and 10 patients with type 1 diabetes mellitus who were positive for islet autoantibodies.…”

Section: Chronic Inflammatory Diseasesmentioning

confidence: 99%

Research progress on application of single-cell TCR/BCR sequencing technology to the tumor immune microenvironment, autoimmune diseases, and infectious diseases

Shen

Luo

et al. 2022

Front. Immunol.

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Single-cell omics is the profiling of individual cells through sequencing and other technologies including high-throughput analysis for single-cell resolution, cell classification, and identification as well as time series analyses. Unlike multicellular studies, single-cell omics overcomes the problem of cellular heterogeneity. It provides new methods and perspectives for in-depth analyses of the behavior and mechanism of individual cells in the cell population and their relationship with the body, and plays an important role in basic research and precision medicine. Single-cell sequencing technologies mainly include single-cell transcriptome sequencing, single-cell assay for transposase accessible chromatin with high-throughput sequencing, single-cell immune profiling (single-cell T-cell receptor [TCR]/B-cell receptor [BCR] sequencing), and single-cell transcriptomics. Single-cell TCR/BCR sequencing can be used to obtain a large amount of single-cell gene expression and immunomics data at one time, and combined with transcriptome sequencing and TCR/BCR diversity data, can resolve immune cell heterogeneity. This paper summarizes the progress in applying single-cell TCR/BCR sequencing technology to the tumor immune microenvironment, autoimmune diseases, infectious diseases, immunotherapy, and chronic inflammatory diseases, and discusses its shortcomings and prospects for future application.

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“…Theory supports unknown intestinal antigens could lead to dysregulated proinflammatory T‐cell immune responses. 8 However, it is unclear whether interactions between innate and adaptive immune cells within the gut are through microbe‐associated molecular pattern (MAMP) ‐ pattern recognition receptor (PRR) interactions, processing of intestinal antigens through MHC class II, or both. Investigations have reported that toll‐like receptor and MHC class II pathways can support one another due to similar processing of ligands/antigens within endosomal cellular compartments.…”

mentioning

confidence: 99%

“…Recognizing that GPR65 actions in epithelial cells, 6 macrophages, 7 and CD4 + T cells 5 contribute to the pathogenesis of IBD, this raises the question of whether innate immune cells regulate GPR65‐mediated T‐cell polarization towards proinflammatory T H 1 and T H 17 cells. Theory supports unknown intestinal antigens could lead to dysregulated proinflammatory T‐cell immune responses 8 . However, it is unclear whether interactions between innate and adaptive immune cells within the gut are through microbe‐associated molecular pattern (MAMP) ‐ pattern recognition receptor (PRR) interactions, processing of intestinal antigens through MHC class II, or both.…”

mentioning

confidence: 99%

GPR65, a novel regulator of helper T‐cell polarization in inflammatory bowel disease

Hathaway‐Schrader

Novince

2022

Clinical & Translational Med

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A novel unconventional T cell population enriched in Crohn’s disease

Cited by 29 publications

References 50 publications

Crohn’s-associated invariant T cells (CAITs) recognise small sulfonate molecules on CD1d

Crohn’s-associated invariant T cells (CAITs) recognise small sulfonate molecules on CD1d

Research progress on application of single-cell TCR/BCR sequencing technology to the tumor immune microenvironment, autoimmune diseases, and infectious diseases

GPR65, a novel regulator of helper T‐cell polarization in inflammatory bowel disease

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