Your search keyword '"Cora Hoxha"' showing total 6 results

1. CD16+ as predictive marker for early relapse in aggressive B-NHL/DLBCL patients

Author

Sylvia Zöphel, Nadja Küchler, Johanna Jansky, Cora Hoxha, Gertrud Schäfer, Julius J. Weise, Joanne Vialle, Lea Kaschek, Gebhard Stopper, Hermann Eichler, Daniela Yildiz, Alina Moter, Philipp Wendel, Evelyn Ullrich, Claudia Schormann, Torben Rixecker, Onur Cetin, Frank Neumann, Patrick Orth, Moritz Bewarder, Markus Hoth, Lorenz Thurner, and Eva C. Schwarz

Subjects

aggressive B-NHL (non-Hodgkin B cell lymphoma), diffuse large B cell lymphoma (DLBCL), CD16+ T cell, CD16+ monocyte, antibody-dependent cellular cytotoxicity (ADCC), rituximab, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Assessing the prognosis of patients with aggressive non-Hodgkin B cell lymphoma mainly relies on a clinical risk score (IPI). Standard first-line therapies are based on a chemo-immunotherapy with rituximab, which mediates CD16-dependent antibody-dependent cellular cytotoxicity (ADCC). We phenotypically and functionally analyzed blood samples from 46 patients focusing on CD16+ NK cells, CD16+ T cells and CD16+ monocytes. Kaplan-Meier survival curves show a superior progression-free survival (PFS) for patients having more than 1.6% CD16+ T cells (p = 0.02; HR = 0.13 (0.007–0.67)) but an inferior PFS having more than 10.0% CD16+ monocytes (p = 0.0003; HR = 16.0 (3.1-291.9)) at diagnosis. Surprisingly, no correlation with NK cells was found. The increased risk of relapse in the presence of > 10.0% CD16+ monocytes is reversed by the simultaneous occurrence of > 1.6% CD16+ T cells. The unexpectedly strong protective function of CD16+ T cells could be explained by their high antibody-dependent cellular cytotoxicity as quantified by real-time killing assays and single-cell imaging. The combined analysis of CD16+ monocytes (> 10%) and CD16+ T cells (

Published

2024

2. Identification of molecular candidates which regulate calcium-dependent CD8+ T-cell cytotoxicity

Author

Maryam Nazarieh, Gertrud Schwär, Cora Hoxha, Markus Hoth, Verena Konetzki, Sylvia Zöphel, Volkhard Helms, Eva C. Schwarz, Mohamed Hamed, and Eckart Meese

Subjects

Transcriptome data analyses, Chemistry, Immunology, Cytotoxic efficiency, Real-time killing assay, CTL (cytotoxic T lymphocytes), Immunological synapse, Cell biology, Transcriptome, CTL, Cell killing, Differential expression analyses, Cytotoxic T cell, Calcium, Secretion, Cytotoxicity, Molecular Biology, CD8

Abstract

Cytotoxic CD8+T lymphocytes (CTL) eliminate infected cells or transformed tumour cells by releasing perforin-containing cytotoxic granules at the immunological synapse. The secretion of such granules depends on Ca2+-influx through store operated Ca2+channels, formed by STIM-activated Orai proteins. Whereas molecular mechanisms of the secretion machinery are well understood, much less is known about the molecular machinery that regulates the efficiency of Ca2+-dependent target cell killing. Here, we isolated total RNA from natural killer (NK) cells, non-stimulated CD8+T-cells, and from Staphylococcus aureus enterotoxin A (SEA) stimulated CD8+T-cells (SEA-CTL) and conducted whole genome expression profiling by microarray experiments. Based on differential expression analysis of the transcriptome data and analysis of master regulator genes, we identified 31 candidates which potentially regulate Ca2+-homeostasis in CTL. To investigate a putative function of these candidates in CTL cytotoxicity, we transfected either SEA-stimulated CTL (SEA-CTL) or antigen specific CD8+T-cell clones (CTL-MART-1) with siRNAs specific against the identified candidates and analyzed the killing capacity using a real-time killing assay. In addition, we complemented the analysis by studying the effect of inhibitory substances acting on the candidate proteins if available. Finally, to unmask their involvement in Ca2+dependent cytotoxicity, candidates were also analyzed under Ca2+-limiting conditions. Overall, this strategy led to the identification of KCNN4, RCAN3, CCR5 and BCL2 as potential candidates to regulate the efficiency of Ca2+-dependent target cell killing.

Published

2023

3. Interdependence of sequential cytotoxic T lymphocyte and natural killer cell cytotoxicity against melanoma cells

Author

Kim S. Friedmann, Lea Kaschek, Arne Knörck, Sabrina Cappello, Niklas Lünsmann, Nadja Küchler, Cora Hoxha, Gertrud Schäfer, Sandra Iden, Ivan Bogeski, Carsten Kummerow, Eva C. Schwarz, and Markus Hoth

Subjects

natural killer cells, Physiology, interleukin-6, cytotoxic T lymphocytes, Killer Cells, Natural, resistance, MART-1 Antigen, cytotoxic efficiency, MART-1, Tumor Microenvironment, cancer cells, melanoma, Humans, T-Lymphocytes, Cytotoxic, human leucocyte antigen, immune evasion

Abstract

Cytotoxic T lymphocytes (CTL) and natural killer (NK) cells recognize and eliminate cancer cells. However, immune evasion, downregulation of immune function by the tumour microenvironment and resistance of cancer cells are major problems. Although CTL and NK cells are both important to eliminate cancer, most studies address them individually. We quantified sequential primary human CTL and NK cell cytotoxicity against the melanoma cell line SK-Mel-5. At high effector-to-target ratios, NK cells or melan-A (MART-1)-specific CTL eliminated all SK-Mel-5 cells within 24 h, indicating that SK-Mel-5 cells are not resistant initially. However, at lower effector-to-target ratios, which resemble numbers of the immune contexture in human cancer, a substantial number of SK-Mel-5 cells survived. Pre-exposure to CTL induced resistance in surviving SK-Mel-5 cells to subsequent CTL or NK cell cytotoxicity, and pre-exposure to NK cells induced resistance in surviving SK-Mel-5 cells to NK cells. Higher human leucocyte antigen class I expression or interleukin-6 levels were correlated with resistance to NK cells, whereas reduction in MART-1 antigen expression was correlated with reduced CTL cytotoxicity. The CTL cytotoxicity was rescued beyond control levels by exogenous MART-1 antigen. In contrast to the other three combinations, CTL cytotoxicity against SK-Mel-5 cells was enhanced following NK cell pre-exposure. Our assay allows quantification of sequential CTL and NK cell cytotoxicity and might guide strategies for efficient CTL-NK cell anti-melanoma therapies. KEY POINTS: Cytotoxic T lymphocytes (CTL) and natural killer (NK) cells eliminate cancer cells. Both CTL and NK cells attack the same targets, but most studies address them individually. In a sequential cytotoxicity model, the interdependence of antigen-specific CTL and NK cell cytotoxicity against melanoma is quantified. High numbers of antigen-specific CTL and NK cells eliminate all melanoma cells. However, lower numbers induce resistance if secondary CTL or NK cell exposure follows initial CTL exposure or if secondary NK cell exposure follows initial NK cell exposure. On the contrary, if secondary CTL exposure follows initial NK cell exposure, cytotoxicity is enhanced. Alterations in human leucocyte antigen class I expression and interleukin-6 levels are correlated with resistance to NK cells, whereas a reduction in antigen expression is correlated with reduced CTL cytotoxicity; CTL cytotoxicity is rescued beyond control levels by exogenous antigen. This assay and the results on interdependencies will help us to understand and optimize immune therapies against cancer.

Published

2023

4. Interdependence of CTL and NK cell cytotoxicity against melanoma cells

Author

Markus Hoth, Ivan Bogeski, Sandra Iden, Carsten Kummerow, Gertrud Schwär, Sabrina Cappello, Arne Knörck, Kim S. Friedmann, Cora Hoxha, and Eva C. Schwarz

Subjects

0303 health sciences, Tumor microenvironment, Chemistry, Cell, 3. Good health, 03 medical and health sciences, CTL, 0302 clinical medicine, medicine.anatomical_structure, Immune system, Antigen, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, medicine, Cytotoxic T cell, Cytotoxicity, 030304 developmental biology

Abstract

CTL and NK cells recognize and eliminate cancer cells. However, immune evasion, down regulation of immune function by the tumor microenvironment, or resistance of cancer cells are a major problem. While CTL and NK cells are both important to eliminate cancer, most studies address them individually. In a new experimental human model, we analysed combined primary human CTL and NK cell cytotoxicity against the melanoma cell line SK-Mel-5. At high effector-to-target ratios, MART-1-specific CTL or NK cells eliminated SK-Mel-5 cells within 24 hours indicating that SK-Mel-5 cells are initially not resistant. However, at lower effector-to-target ratios, which resemble conditions of the immune contexture in human cancer, a significant number of SK-Mel-5 cells survived. Whereas CTL pre-exposure induced resistance in surviving SK-Mel-5 cells to subsequent CTL or NK cell cytotoxicity, NK cell pre-exposure induced resistance in surviving SK-Mel-5 cells to NK cells but not to MART-1 specific CTL. In contrast, there was even a slight enhancement of CTL cytotoxicity against SK-Mel-5 cells following NK cell pre-exposure. In all other combinations, resistance to subsequent cytotoxicity was higher, if melanoma cells were pre-exposed to larger numbers of CTL or NK cells. Increases in human leukocyte antigen class I expression correlated with resistance to NK cells, while reduction in MART-1 antigen expression correlated with reduced CTL cytotoxicity. CTL cytotoxicity was rescued beyond control levels by exogenous MART-1 antigen. This study quantifies the interdependence of CTL and NK cell cytotoxicity and may guide strategies for efficient CTL-NK cell anti-melanoma therapies.Key points summaryCytotoxic T lymphocytes (CTL) and natural killer (NK) cells eliminate cancer cells. CTL and NK work in parallel, but most studies address them individually.In a new human experimental model, antigen-specific CTL and NK cell cytotoxicity interdependence against melanoma is shown.Whereas high numbers of antigen-specific CTL and NK cells eliminate all melanoma cells, lower, more physiological numbers induce resistance, in case secondary CTL or NK cell exposure follow initial CTL cell exposure or if secondary NK cell exposure follows initial NK cell exposure; only if secondary CTL exposure follows initial NK cell exposure no resistance of melanoma but even a slight enhancement of cytotoxicity was observed.Alterations in HLA-I expression correlated with resistance to NK cells, while reduction in antigen expression correlated with reduced CTL cytotoxicity. CTL cytotoxicity was rescued beyond control levels by exogenous antigen.The results should help to better understand and optimize immune therapies against cancer.Graphical abstract

Published

2020

5. Syntaxin 8 is required for efficient lytic granule trafficking in cytotoxic T lymphocytes

Author

Shruthi S. Bhat, Arne Knörck, Cora Hoxha, Eva C. Schwarz, Christina Backes, Markus Hoth, Bin Qu, Jens Rettig, Kim S. Friedmann, Petra Leidinger, Andreas Keller, and Eckart Meese

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Time Factors, chemical and pharmacologic phenomena, Endosomes, Cytoplasmic Granules, Transfection, Cell Degranulation, Immunological synapse, Cell Line, 03 medical and health sciences, Lysosomal-Associated Membrane Protein 1, Cytotoxic T cell, Syntaxin, Humans, Molecular Biology, biology, Perforin, Qa-SNARE Proteins, Secretory Vesicles, T-cell receptor, Degranulation, hemic and immune systems, Cell Biology, Molecular biology, Cell biology, CTL, Protein Transport, 030104 developmental biology, Granzyme, biology.protein, RNA Interference, Lysosomes, T-Lymphocytes, Cytotoxic

Abstract

Cytotoxic T lymphocytes (CTL) eliminate pathogen-infected and cancerous cells mainly by polarized secretion of lytic granules (LG, containing cytotoxic molecules like perforin and granzymes) at the immunological synapse (IS). Members of the SNARE (soluble N-ethylmaleimide-sensitive factor attachment protein receptor) family are involved in trafficking (generation, transport and fusion) of vesicles at the IS. Syntaxin 8 (Stx8) is expressed in LG and colocalizes with the T cell receptor (TCR) upon IS formation. Here, we report the significance of Stx8 for human CTL cytotoxicity. We found that Stx8 mostly localized in late, recycling endosomal and lysosomal compartments with little expression in early endosomal compartments. Down-regulation of Stx8 by siRNA resulted in reduced cytotoxicity. We found that following perforin release of the pre-existing pool upon target cell contact, Stx8 down-regulated CTL regenerate perforin pools less efficiently and thus release less perforin compared to control CTL. CD107a degranulation, real-time and end-point population cytotoxicity assays, and high resolution microscopy support our conclusion that Stx8 is required for proper and timely sorting and trafficking of cytotoxic molecules to functional LG through the endosomal pathway in human CTL.

Published

2015

6. Deep characterization of blood cell miRNomes by NGS

Author

Benjamin Meder, Christina Backes, Nicole Ludwig, Petra Leidinger, Arne Knörck, Hermann Eichler, Sabine Müller, Andreas Keller, Thomas Grossmann, Jan Haas, Eva C. Schwarz, Eckart Meese, Isabelle Müller, Martin Hart, Tobias Fehlmann, Andre Franke, Gertrud Schwär, Valentina Galata, Markus Hoth, and Cora Hoxha

Subjects

0301 basic medicine, Cell type, Cell, Biology, Blood cell, 03 medical and health sciences, Cellular and Molecular Neuroscience, microRNA, medicine, Cluster Analysis, Humans, Molecular Biology, Pharmacology, Genetics, Principal Component Analysis, Blood Cells, Base Sequence, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Cell Biology, Biomarker (cell), Gene expression profiling, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Molecular Medicine, Analysis of variance, CD8

Abstract

A systematic understanding of different factors influencing cell type specific microRNA profiles is essential for state-of-the art biomarker research. We carried out a comprehensive analysis of the biological variability and changes in cell type pattern over time for different cell types and different isolation approaches in technical replicates. All combinations of the parameters mentioned above have been measured, resulting in 108 miRNA profiles that were evaluated by next-generation-sequencing. The largest miRNA variability was due to inter-individual differences (34 %), followed by the cell types (23.4 %) and the isolation technique (17.2 %). The change over time in cell miRNA composition was moderate (

Published

2015