Your search keyword '"Roland Goldbrunner"' showing total 4 results

1. Malignant gliomas actively recruit bone marrow stromal cells by secreting angiogenic cytokines.

Author

Tobias Birnbaum, Julia Roider, Christoph Schankin, Claudio Padovan, Christian Schichor, Roland Goldbrunner, and Andreas Straube

Abstract

Abstract  The transplantation of progenitor cells is a promising new approach for the treatment of gliomas. Marrow stromal cells (MSC) are possible candidates for such a cell-based therapy, since they are readily and autologously available and show an extensive tropism to gliomas in vitro and in vivo. However, the signals that guide the MSC are still poorly understood. In this study, we show that gliomas have the capacity to actively attract MSC by secreting a multitude of angiogenic cytokines. We demonstrate that interleukin-8 (IL-8), transforming growth factor-1 (TGF-1) and neurotrophin-3 (NT-3) contribute to this glioma-directed tropism of human MSC. Together with the finding that vascular endothelial growth factor (VEGF) is another MSC-attracting factor secreted by glioma cells, these data support the hypothesis that gliomas use their angiogenic pathways to recruit mesenchymal progenitor cells. [ABSTRACT FROM AUTHOR]

Published

2007

2. Acute morphological sequelae of photodynamic therapy with 5-aminolevulinic acid in the C6 spheroid model.

Author

Reinhold Baumgartner, Karl Bise, Michael Heide, Richard Meier, Susanne Stocker, Ronald Sroka, Roland Goldbrunner, and Walter Stummer

Abstract

AbstractObjective??Aminolevulinic acid (ALA)-mediated photodynamic therapy (PDT) may represent a treatment option for malignant brain tumors. We used a three-dimensional cell culture system, the C6 glioma spheroid model, to study acute effects of PDT and how they might be influenced by treatment conditions.Methods??Spheroids were incubated for 4?h in 100??g/ml ALA in 5% CO2in room air or 95% O2with subsequent irradiation using a diode laser (??=?635?nm, 40?mW/cm2, total fluence 25?J/cm2). Control groups were ?laser only?, ?ALA only?, and ?no drug no light?. Annexin V-FITC, a marker used for detection of apoptosis, propidium iodide (PI), a marker for necrotic cells and H 33342, a chromatin stain, were used for morphological characterization of PDT effects by confocal laser scanning and fluorescence microscopy. Hematoxylin?eosin staining and TdT-FragEL (TUNEL) assay were used on cryosections. Growth kinetics were followed for 8?days after PDT.Results??PDT after incubation in 5% CO2provided incomplete cell death and growth delay in spheroids of >350??m diameter. However, complete cell death and growth arrest occurred in smaller spheroids (<350??m). Incubation in 95% O2with subsequent PDT resulted in complete cell death and growth arrest regardless of spheroid size. In incompletely damaged spheroids viable cells were restricted to spheroid centers. The rate of cell death in all control groups was negligible. Cell death was accompanied by annexin/PI costaining, but there was also evidence for annexin V-FITC staining without PI uptake.Conclusions??PDT of experimental glioma results in rapid and significant cell death that could be verified as acute necrosis immediately after irradiation. This effect depended on O2concentration and spheroid size. [ABSTRACT FROM AUTHOR]

Published

2007

3. Isolation and Culture of Microvascular Endothelial Cells from Gliomas of Different WHO Grades.

Author

Sabine Miebach, Stefan Grau, Vera Hummel, Peter Rieckmann, Joerg-Christian Tonn, and Roland Goldbrunner

Abstract

Gliomas are the most common intrinsic brain tumors. The degree of vascularization corresponds to malignancy and is related to prognosis. In order to retrieve information about tumor behavior in situ, the use of primary tissue material for experiments is advantageous. With increasing evidence for the importance of microenvironment and vascularization in tumor biology, we concentrated on the isolation of endothelial cells (EC) from primary tumor material to investigate the role of endothelium within tumor tissue. [ABSTRACT FROM AUTHOR]

Published

2006

4. The brain slice chamber, a novel variation of the Boyden Chamber Assay, allows time-dependent quantification of glioma invasion into mammalian brain in vitro.

Author

Christian Schichor, Siglinde Kerkau, Theresa Visted, Rudolf Martini, Rolf Bjerkvig, Jörg Tonn, and Roland Goldbrunner

Abstract

Glioma cell invasion occurs in a complex micromilieu consisting of neural and glial cells, myelinated fiber tracts, blood vessels and extracellular matrix proteins. The present work describes the brain slice chamber (BSC) as a novel experimental model for assessing invasion of glioma cells into adult mammalian white and gray matter on the basis of the well known Boyden chamber system. As a matrix for invasive tumor cells we used freshly prepared brain tissue from adult pigs. The tissue was sectioned into 40 ?m slices that were mechanically fixed to a millipore filter. The neural structures and the three-dimensional architecture of the slice was preserved as verified by immunohistochemistry, light- and electron microscopy. Human U-373 and U87 astrocytoma cells stably transfected with green fluorescent protein (GFP) were assessed for their invasiveness into the brain-slices during a 24 h period. Invasion of U-87 GFP cells was quantified at different time intervals by confocal laser scanning microscopy showing more intense invasion into white compared to gray matter. Two cytostatics (vincristin and paclitaxel) which both are known to affect the cytoskeleton, inhibited glioma cell invasion in a dose dependent manner, which makes the presented model system suitable for functional experiments. In conclusion, the BSC represents a valid and rapid experimental model that may be used to describe the invasive behavior of glioma cells within the preserved three-dimensional structure of mammalian brain tissue in vitro. [ABSTRACT FROM AUTHOR]

Published

2005