Dendritic Cell-Triggered Immune Activation Goes along with Provision of (Leukemia-Specific) Integrin Beta 7-Expressing Immune Cells and Improved Antileukemic Processes.
Elias RacklLin LiLara Kristina KlauerSelda UgurElena PepeldjiyskaCorinna L SeidelCarina GunsiliusMelanie WeinmannFatemeh Doraneh-GardNina ReiterCaroline PlettDaniel Christoph AmbergerPeter BojkoDoris KraemerJörg SchmohlAndreas RankChristoph SchmidHelga Maria SchmetzerPublished in: International journal of molecular sciences (2022)
Integrin beta 7 (β7), a subunit of the integrin receptor, is expressed on the surface of immune cells and mediates cell-cell adhesions and interactions, e.g., antitumor or autoimmune reactions. Here, we analyzed, whether the stimulation of immune cells by dendritic cells (of leukemic derivation in AML patients or of monocyte derivation in healthy donors) leads to increased/leukemia-specific β7 expression in immune cells after T-cell-enriched mixed lymphocyte culture-finally leading to improved antileukemic cytotoxicity. Healthy, as well as AML and MDS patients' whole blood (WB) was treated with Kit-M (granulocyte-macrophage colony-stimulating factor (GM-CSF) + prostaglandin E1 (PGE1)) or Kit-I (GM-CSF + Picibanil) in order to generate DCs (DC leu or monocyte-derived DC), which were then used as stimulator cells in MLC. To quantify antigen/leukemia-specific/antileukemic functionality, a degranulation assay (DEG), an intracellular cytokine assay (INTCYT) and a cytotoxicity fluorolysis assay (CTX) were used. (Leukemia-specific) cell subtypes were quantified via flow cytometry. The Kit treatment of WB (compared to the control) resulted in the generation of DC/DC leu , which induced increased activation of innate and adaptive cells after MLC. Kit-pretreated WB (vs. the control) led to significantly increased frequencies of β7-expressing T-cells, degranulating and intracellular cytokine-producing β7-expressing immune cells and, in patients' samples, increased blast lysis. Positive correlations were found between the Kit-M-mediated improvement of blast lysis (vs. the control) and frequencies of β7-expressing T-cells. Our findings indicate that DC-based immune therapies might be able to specifically activate the immune system against blasts going along with increased frequencies of (leukemia-specific) β7-expressing immune cells. Furthermore, β7 might qualify as a predictor for the efficiency and the success of AML and/or MDS therapies.
Keyphrases
- dendritic cells
- acute myeloid leukemia
- end stage renal disease
- immune response
- newly diagnosed
- chronic kidney disease
- ejection fraction
- bone marrow
- peritoneal dialysis
- regulatory t cells
- prognostic factors
- induced apoptosis
- flow cytometry
- high throughput
- palliative care
- cell therapy
- single cell
- endoplasmic reticulum stress
- escherichia coli
- stem cells
- oxidative stress
- poor prognosis
- multiple sclerosis
- endothelial cells
- cell proliferation
- mesenchymal stem cells
- allogeneic hematopoietic stem cell transplantation
- adipose tissue
- multidrug resistant
- long non coding rna
- patient reported
- reactive oxygen species
- combination therapy