Your search keyword '"Leuhuber K"' showing total 5 results

1. Maintenance of ATP favours apoptosis over necrosis triggered by benzamide riboside.

Author

Grusch, M., Polgar, D., Gfatter, S., Leuhuber, K., Huettenbrenner, S., Leisser, C., Fuhrmann, G., Kassie, F., Steinkellner, H., Smid, K., Peters, G.J., Jayaram, H.N., Klepal, W., Szekeres, T., Knasmuller, S., and Krupitza, G.

Subjects

ADENOSINE triphosphate, BENZAMIDE, APOPTOSIS, NECROSIS

Abstract

A new synthetic drug, benzamide riboside (BR) exhibited strong oncolytic activity against leukemic cells in the 510 µM range. Higher BR-concentrations (20 µM) predominantly induced necrosis which correlated with DNA strand breaks and subsequent depletion of ATP- and dATP levels. Replenishment of the ATP pool by addition of adenosine prevented necrosis and favoured apoptosis. This effect was not a pecularity of BR-treatment, but was reproduced with high concentrations of all trans-retinoic acid (120 µM) and cyanide (20 mM). Glucose was also capable to suppress necrosis and to favour apoptosis of HL-60 cells, which had been treated with necrotic doses of BR and cyanide. Apoptosis eliminates unwanted cells without affecting the microenvironment, whereas necrosis causes severe inflammation of surrounding tissues due to spillage of cell fluids into the peri-cellular space. Thus, the monitoring and maintenance of cellular energy pools during therapeutic drug treatment may help to minimize nonspecific side effects and to improve attempted drug effects. [ABSTRACT FROM AUTHOR]

Published

2002

2. Apoptosis in a tissue-like culture model of human colorectal adenoma cells.

Author

Leuhuber K, Klepal W, Hausott B, and Marian B

Subjects

Adenoma ultrastructure, Antineoplastic Agents, Phytogenic pharmacology, Cell Culture Techniques, Collagen, Colorectal Neoplasms ultrastructure, Drug Evaluation, Preclinical, Quercetin pharmacology, Resveratrol, Stilbenes pharmacology, Tumor Cells, Cultured, Adenoma metabolism, Apoptosis drug effects, Colorectal Neoplasms metabolism, Models, Biological

Abstract

Tissue-like cultures of LT97 human colonic adenoma cells were produced by plating on reconstructed connective tissue supports (CTR) containing colon-associated fibroblasts to form mucosal monolayers and polyp-like structures closely resembling the in vivo situation. Tight cell-cell contacts and a high density of desmosomes were observed in 93.8+/-3.5% of the section area for CTR cultures, but only in 17.8+/-10.0% of the area for cultures on collagen gels (CG) without fibroblasts. While LT97 cultures on plastic shed apoptotic bodies into the medium, they collected at the basal pole of the cell layer in the CTR cultures as is also observed in adenoma tissue. Only a small proportion was released into the medium as shown by the detection of apoptosis specific keratin fragments, which could be increased by 100microM of quercetin and resveratrol. In addition, tissue-like structures altered the relative effectivity of test compounds. As the tissue-like conditions closely resemble the situation in vivo tissue-like cultures are an important step towards the establishment of tissue reconstructs that can replace animal models in the analysis of basic mechanisms of growth control and the testing of tumor promoting and chemopreventive compounds and may even be superior in terms of predictivity as they use human cells.

Published

2006

3. Transferrin ensures survival of ovarian carcinoma cells when apoptosis is induced by TNFalpha, FasL, TRAIL, or Myc.

Author

Fassl S, Leisser C, Huettenbrenner S, Maier S, Rosenberger G, Strasser S, Grusch M, Fuhrmann G, Leuhuber K, Polgar D, Stani J, Tichy B, Nowotny C, and Krupitza G

Subjects

Apoptosis Regulatory Proteins, Fas Ligand Protein, Female, Humans, Ovarian Neoplasms metabolism, TNF-Related Apoptosis-Inducing Ligand, Apoptosis physiology, Cell Survival physiology, Membrane Glycoproteins physiology, Ovarian Neoplasms pathology, Proto-Oncogene Proteins c-myc physiology, Transferrin physiology, Tumor Necrosis Factor-alpha physiology

Abstract

The activation of Myc induces apoptosis of human ovarian adenocarcinoma N.1 cells when serum factors are limited. However, the downstream mechanism that is triggered by Myc is unknown. Myc-activation and treatment with the proapoptotic ligands TNFalpha, FasL, and TRAIL induced H-ferritin expression under serum-deprived conditions. H-ferritin chelates intracellular iron and also intracellular iron sequestration by deferoxamine-induced apoptosis of N.1 cells. Supplementation of serum-free medium with holo-transferrin blocked apoptosis of N.1 cells that was induced by Myc-activation or by treatment with TNFalpha, FasL, and TRAIL, whereas apotransferrin did not prevent apoptosis. This suggests that intracellular iron depletion was a trigger for apoptosis and that transferrin-bound iron rescued N.1 cells. Furthermore, apoptosis of primary human ovarian carcinoma cells, which was induced by TNFalpha, FasL, and TRAIL, was also inhibited by holo-transferrin. The data suggest that Myc-activation, FasL, TNFalpha, and TRAIL disturbed cellular iron homeostasis, which triggered apoptosis of ovarian carcinoma cells and that transferrin iron ensured survival by re-establishing this homeostasis.

Published

2003

4. Transferrin Ensures Survival of Ovarian Carcinoma Cells Subjected to Deferoxamine, TNFA, FASL, Trail or MYC -Activation.

Author

Rosenberger G, Grusch M, Fuhrmann G, Leuhuber K, Polgar D, Krupitza G, and Krupitza G

Published

2001

5. Inverse hierarchy of vimentin epitope expression in primary cultures of chicken and rat astrocytes: a double-immunofluorescence study.

Author

Gereben B, Leuhuber K, Rausch WD, Gálfi P, Jancsik V, and Rudas P

Subjects

Animals, Blotting, Western, Cells, Cultured, Chick Embryo, Fluorescent Antibody Technique, Rats, Rats, Sprague-Dawley, Species Specificity, Astrocytes immunology, Epitopes analysis, Vimentin immunology

Abstract

Vimentin contributes to the cytoskeleton of different cell-types, among them glial cells. We report here that different forms of this protein, distinguishable by the monoclonal antibodies Vim3B4 and V9, are species-specifically expressed in cultures of glial fibrillary acidic protein (GFAP) positive, primary astrocytes of the chicken and rat. Most cells in the cultures co-expressed GFAP and one of the two vimentin epitopes. The Vim3B4 positive epitope was present in chicken astrocytes, while the V9 positive was not. Inverse situation was found in the astrocytes of rat. In vitro age of the cells did not influence the hierarchy of vimentin epitope expression with respect to species-specificity. Our result shows that the different vimentin expression program of cultured astrocytes of the chicken and rat is preserved under in vitro conditions. The presented data support the concept of the species-specific regulation of vimentin forms in glial cells of the central nervous system.

Published

1998