Your search keyword '"Katharina Förtsch"' showing total 3 results

1. CD5‐expressing CD8 + T‐cell subsets differ between children with type 1 diabetes and controls

Author

Katharina Förtsch, Maximilian Hoffmann, Sebastian Kummer, Thomas Meissner, Marc Jacobsen, Ertan Mayatepek, Christina Reinauer, Julia Seyfarth, Carsten Döing, Josefine Wadenpohl, and Paul Hehenkamp

Subjects

medicine.diagnostic_test, CD3, Immunology, Cell Biology, Biology, Molecular biology, In vitro, CD19, Flow cytometry, Immune system, immune system diseases, biology.protein, medicine, Immunology and Allergy, Cytotoxic T cell, CD5, CD8

Abstract

Different lymphocyte subsets are involved in autoimmune pathogenesis of type 1 diabetes (T1D). Previous studies suggested a role of CD5-expressing T and B cells including rare unconventional lymphocytes with combined T- and B-cell features [dual expressing (DE) cells]. We performed algorithm-supported multiparameter flow cytometry and quantitative PCR to investigate immune cell subsets and DE cells in children with T1D (n = 20) and matched controls (n = 20). Comparisons of conventional immune cells detected increased proportions of CD3+ T cells in T1D patients, whereas CD19+ B-cell proportions were comparable to controls. Self-organizing maps for flow cytometry analyses (FlowSOM) showed highly similar CD5-expressing B-cell subsets and no differences for DE cells were detected between the study groups by flow cytometry or specific quantitative PCR. Notably, differences in CD8+ T cells were indicated by FlowSOM and similarity-based t-distributed stochastic neighbor embedding (tSNE) analyses. Study group comparisons confirmed significantly reduced CD8+ T-cell proportions with moderate or low CD5 expression in T1D patients. Finally, in vitro experiments showed stable CD5 expression differences of CD8+ T cells after T-cell activation, cytokine stimulation and culture. We observed differences of T-cell coreceptor CD5 expression in T1D patients with potential relevance for immune regulation of CD8+ T-cell activation.

Published

2021

2. Author response for 'Interleukin‐7 dependent non‐classical monocytes and CD40 expression are affected in children with type 1 diabetes'

Author

Marc Jacobsen, Maximilian Hoffmann, Katharina Förtsch, Jürgen Enczmann, Julia Seyfarth, Christina Reinauer, Carsten Döing, Paul Hehenkamp, Thomas Meissner, Sebastian Kummer, Vera Balz, and Ertan Mayatepek

Subjects

Type 1 diabetes, CD40, biology, Expression (architecture), Immunology, biology.protein, medicine, Interleukin, medicine.disease

Published

2021

3. Dominant TNFα and impaired IL‐2 cytokine profiles of CD4 + T cells from children with type‐1 diabetes

Author

Katharina Förtsch, René Deenen, Marc Jacobsen, Julia Seyfarth, Hans-Juergen Laws, Ertan Mayatepek, Beate Karges, Karl Köhrer, Heinz Ahlert, and Thomas Meissner

Subjects

0301 basic medicine, Type 1 diabetes, medicine.medical_treatment, Immunology, Cell Biology, Disease, Biology, medicine.disease, Clinical onset, In vitro, Transcriptome, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Cytokine, medicine, Immunology and Allergy, Tumor necrosis factor alpha, 030215 immunology

Abstract

Aberrantly activated CD4+ T memory cells play a central role in the development of type-1-diabetes. Interleukin-7 promotes generation of autoimmune memory T cells and increased Interleukin-7 availability is associated with type-1-diabetes susceptibility. T-cell-mediated immune pathology at onset of type-1-diabetes is well defined, but characteristics of long-term symptomatic disease stages remain largely elusive. In the present study, memory CD4+ T-cell activation and cytokine expression as well as sensitivity to Interleukin-7 in vitro were compared between patients with type-1-diabetes at clinical onset (n=25), long-term symptomatic disease (median duration 4.5 years, n=19) and matched healthy controls (n=21). T-cell responses of type-1-diabetes patients were characterized by higher frequencies of cytokine and activation marker expressing CD4+ memory T cells as compared to healthy controls. Notably, correction for individual cytokine expression levels revealed qualitative differences of cytokine profiles characterized by significantly increased TNFα and decreased IL-2-expressing T-cell proportions in long-term type-1-diabetes patients. IL-7-mediated T-cell co-stimulation induced quantitative and qualitative cytokine expression differences highly similar to type-1-diabetes-specific profiles. In addition, CD4+ memory T cells from children with long-term type-1-diabetes were more sensitive to in vitro IL-7 co-stimulation. Global transcriptome analysis revealed IL-7 induced expression differences of CD4+ T cells, including increased IL-2R expression and effects on subsequent T-cell receptor activation. We conclude that long-term symptomatic type-1-diabetes patients differed in memory T-cell cytokine profiles and Interleukin-7 co-stimulation. Regulation of IL-2 expression and sensitivity are affected with possible consequences for disease course and severity at long-term type-1-diabetes stages.

Published

2017