Showing total 23 results

1. [Pseudoprogression or pseudoresponse: a challenge for the diagnostic imaging in Glioblastoma multiforme].

Author

Payer F

Subjects

Angiogenesis Inhibitors adverse effects, Angiogenesis Inhibitors therapeutic use, Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized, Antineoplastic Agents, Alkylating adverse effects, Antineoplastic Agents, Alkylating therapeutic use, Bevacizumab, Brain pathology, Brain radiation effects, Combined Modality Therapy, Cranial Irradiation, Dacarbazine adverse effects, Dacarbazine analogs & derivatives, Dacarbazine therapeutic use, Diagnosis, Differential, Diffusion Magnetic Resonance Imaging, Disease Progression, Humans, Image Processing, Computer-Assisted, Magnetic Resonance Angiography, Magnetic Resonance Imaging, Magnetic Resonance Spectroscopy, Positron-Emission Tomography, Radiation Injuries diagnosis, Sensitivity and Specificity, Temozolomide, Tumor Burden, Brain Neoplasms diagnosis, Brain Neoplasms therapy, Diagnostic Imaging, Glioblastoma diagnosis, Glioblastoma therapy

Abstract

This methodological paper on magnetic resonance tomography imaging recalls the assessment criteria on therapy response of Glioblastoma multiforme as defined by David Macdonald in 1990 that have remained State of the Art since their first publication. It defines the terms "pseudoprogression", "radiation induced necrosis" and "pseudoresponse". These phenomena are seen increasingly since the introduction of radiochemotherapy with Temozolomide as treatment standard in glioblastoma and since the use of antiangiogenetic therapy in malignant gliomas. Therefore, the assessment criteria have been recently updated with the newly proposed "RANO criteria (Response assessment in Neuro-Oncology)". Furthermore, the potential of additional information to conventional MR by MR perfusion, MR diffusion and MR spectroscopy is briefly discussed.

Published

2011

2. Tumor-Wirtszellen-Interaktion im Mikromilieu: neue Angriffspunkte für die Therapie?

Author

Sevenich, Lisa and Heiland, Dieter Henrik

Published

2024

3. [Rare tumors of the parotid gland. Lymphadenoma of a sebaceous gland and extracranial metastasis from glioblastoma].

Author

Kühn U, Köhler HH, and Jecker P

Subjects

Adenoma pathology, Aged, Biopsy, Needle, Brain Neoplasms pathology, Diagnosis, Differential, Glioblastoma pathology, Humans, Male, Middle Aged, Parotid Gland pathology, Parotid Neoplasms pathology, Ultrasonography, Adenoma diagnosis, Brain Neoplasms diagnostic imaging, Glioblastoma diagnostic imaging, Glioblastoma secondary, Parotid Neoplasms diagnostic imaging, Parotid Neoplasms secondary, Temporal Lobe pathology

Abstract

Tumors of the parotid gland can be benign or malignant lesions.The pathophysiology of rare tumors of the parotid gland is often not sufficiently explored in this paper two rare histological entities are described. In one patient a benign sebaceous lymph-adenoma was histologically diagnosed. This type of tumor accounts for only 0.196 of all adenomas. The international literature is not conclusive about whether the tumor originates in the parotid gland itself or in the parotid lymph nodes. The second patient presented with a metastasis from a glioblastoma in the parotid gland. Again, the mechanism for metastasis of an intra-cerebral tumor to the parotid gland remains unknown. Iatrogenic seeding during a neurosurgical intervention is a probable explanation. The actual clinical course of his patient and the cases described in literature render surgical removal of such a metastasis questionable.

Published

2003

4. Die WHO-Klassifikation der Tumoren des zentralen Nervensystems 2021: Neuerungen zur Diagnostik diffuser Gliome und deren Bedeutung für die klinische Praxis

Author

Weller, Michael, Knobbe-Thomsen, Christiane B., Le Rhun, Emilie, and Reifenberger, Guido

Published

2022

5. Immuntherapien bei Gliomen

Author

Ochs, K., Bunse, L., Mildenberger, I., Wick, W., and Platten, M.

Published

2018

6. Immuntherapien bei Gliomen

Author

Ochs, Katharina, Bunse, Lukas, Mildenberger, Iris, Wick, Wolfgang, and Platten, Michael

Published

2017

7. Personalisierte Gliomtherapie

Author

Wick, W. and Hau, P.

Published

2015

8. Saures Gliafaserprotein beim Patienten mit akuten Schlaganfallsymptomen: Diagnostischer Marker einer Hirnblutung

Author

Foerch, C., Pfeilschifter, W., Zeiner, P., and Brunkhorst, R.

Published

2014

9. Anwendungen der Ultrahochfeld-MRT in der Neuroonkologie

Author

Radbruch, A. and Schlemmer, H.-P.

Published

2013

10. Stellenwert der Tumorresektion in der interdisziplinären Behandlung hirneigener Tumoren

Author

Ringel, F., Gempt, J., Buchmann, N., Krieg, S., Pape, H., Shiban, E., Ryang, Y.-M., and Meyer, B.

Published

2011

11. Chemotherapie bei Gliomen

Author

Wick, W., Winkler, F., and Platten, M.

Published

2011

12. Hochmaligne Gliome im Kindes- und Jugendalter

Author

Kramm, C., Rausche, U., Butenhoff, S., Kühnöl, C., Kunze, C., Kortmann, R., Wolff, J., and van Gool, S.

Published

2008

13. Molekulare Diagnostik von Gliomen

Author

Hasselblatt, M.

Published

2008

14. Thermotherapie mit magnetischen Nanopartikeln

Author

Jordan, A., Maier-Hauff, K., Wust, P., Rau, B., and Johannsen, M.

Published

2007

15. Diagnostik und Therapie des Glioblastoms: Standards und neue Entwicklungen

Author

Weller, M., Tonn, J. C., Ernemann, U., Wiestler, O. D., and Bamberg, M.

Published

2006

16. Lokoregionäre Hyperthermie: Standards und neue Entwicklungen

Author

Hildebrandt, Bert, Rau, Beate, Gellermann, Johanna, Kerner, Thoralf, Nicolaou, Annett, Blohmer, Jens-Uwe, Trappe, Ralf Ulrich, Riess, Hanno, and Wust, Peter

Published

2004

17. Seltene Parotistumoren: Talgdrüsenlymphadenom und extrakranielle Glioblastommetastase

Author

Kühn, U., Köhler, H. H., and Jecker, P.

Published

2003

18. Aktuelle Standards in der Behandlung maligner Gliome

Author

Weller, Michael and Wick, Wolfgang

Published

2008

19. Verbessern superparamagnetische Kontrastmittel die MR- tomographische Abgrenzbarkeit experimenteller Gliome?

Author

Egelhof, T., Delbeck, N., Hartmann, M., Roth, S. U., Elste, V., Heiland, S., and Sartor, K.

Published

1998

20. [Pseudoprogression or pseudoresponse: a challenge for the diagnostic imaging in Glioblastoma multiforme]

Author

Franz, Payer

Subjects

Diagnostic Imaging, Magnetic Resonance Spectroscopy, Brain Neoplasms, Antibodies, Monoclonal, Brain, Angiogenesis Inhibitors, Antibodies, Monoclonal, Humanized, Combined Modality Therapy, Magnetic Resonance Imaging, Sensitivity and Specificity, Tumor Burden, Bevacizumab, Dacarbazine, Diagnosis, Differential, Diffusion Magnetic Resonance Imaging, Positron-Emission Tomography, Disease Progression, Image Processing, Computer-Assisted, Temozolomide, Humans, Cranial Irradiation, Glioblastoma, Radiation Injuries, Antineoplastic Agents, Alkylating, Magnetic Resonance Angiography

Abstract

This methodological paper on magnetic resonance tomography imaging recalls the assessment criteria on therapy response of Glioblastoma multiforme as defined by David Macdonald in 1990 that have remained State of the Art since their first publication. It defines the terms "pseudoprogression", "radiation induced necrosis" and "pseudoresponse". These phenomena are seen increasingly since the introduction of radiochemotherapy with Temozolomide as treatment standard in glioblastoma and since the use of antiangiogenetic therapy in malignant gliomas. Therefore, the assessment criteria have been recently updated with the newly proposed "RANO criteria (Response assessment in Neuro-Oncology)". Furthermore, the potential of additional information to conventional MR by MR perfusion, MR diffusion and MR spectroscopy is briefly discussed.

Published

2010

21. Fremdgentransfer in Glioblastomzellen mittels Listeria monocytogenes-Vektoren

Author

Schulz, Chris and Justus Liebig University Giessen

Subjects

ddc:610, glioblastoma, Glioblastom, gene transfer, bacteria, Gentransfer, Bakterien

Abstract

In dieser Arbeit werden Experimente zum Gentransfer in humane Glioblastomzellen mit einem Genvektorsystem, basierend auf dem fakultativ intrazellulären Bakterium Listeria moncytogenes 1/2a, beschrieben. Die Untersuchung der Listerieninvasion in 2 etablierte Gliomzellinien sowie 27 Primärkulturen intraoperativ entnommener Hirntumorpräparate zeigte, daß L.monocytogenes in der Lage ist, humane Hirntumorzellen zu invadieren. Die stärkste absolute Listerien-Wildtypinvasion wurde dabei unter den astrozytären Tumorzellen beobachtet. Die Invasion in diese Tumorzellen war deutlich von der Aktivität der bakteriellen invasiven Virulenzgene Internalin A und B abhängig. Die plasmidgesteuerte Überexpression dieser Virulenzgene in den verwendeten Listerienstämmen resultierte gegenüber Wildtyplisterien in einer auf 215% gesteigerten mittleren Invasion in astrozytäre Tumorzellen. Durch Deletion beider Internalingene hingegen wurde die bakterielle Invasion in astrozytäre Zellen im Mittel auf 50% reduziert. Als Reportergene des Fremdgentransfers wurden lacZ und EGFP gewählt. Mit hierfür konstruierten Plasmidvektoren konnte per Lipofektion in astrozytäre Zellen die intrazelluläre Fremdgenaktivität festgestellt werden. Durch Transformation der Plasmidvektoren in Listeria monocytogenes1/2a wurden komplementierte Listerien-Stämme generiert, deren Eignung zum vektoriellen Fremdgentransfer in astrozytäre Zellen zu untersuchen war. Derart komplementierte Wildtypstämme von Listeria monocytogenes waren in der Lage, die gewählten Reportergene in humane Zellen zu transportieren. Transferraten von bis zu 70% wurden in Zellen der epithelialen Zellinie 293T beobachtet. Die Transfereffizienz in den untersuchten astrozytären Zellen lag zwischen 3-5%. Eine Transferrate von mehr als 10% sollte für einen therapeutischen Gentransfer (von beispielsweise Suizidgenen) angestrebt werden. Unter anderem durch Veränderung der Virulenzfaktorausstattung des Vektors, spezifiziertes Targeting der Wirtszelle und durch Optimierung der Fremdgene für die intrazelluläre Transkription und Translation könnte eine weitere Steigerung der Transfereffizienz erreicht werden., Experiments for gene transfer into human glioblastoma cells using the facultative intracellular bacterium listeria monocytogenes are described in the presented paper. Examination of bacterial invasion into stable glioblastoma cells and primary cell cultures of different intracranial tumors did show, that listeria are able to enter these cells, depending on the cell origin and the existing bacterial virulence factors. The strongest absolute invasion of wild type listeria monocytogenes was observed in cells of astrocytic origin. Using bacterial mutants with deletion of the virulence genes internalin A and B results in a distinct reduced invasion in astrocytic cells (50%), whereas overexpression of this genes by a privileged transcribed plasmid could essentially increase the invasion number of the listeria mutants (215%). For the gene transfer studies two reporter genes, lacZ and EGFP, in special constructed plasmids were used. Via lipofection these reporter gene containing plasmids were conducted into human cells and the activity of the foreign genes was observed by fluorescens microscopy and the b-galactosidase staining assay. These reporter gene containing plasmids were transfered to listeria monocytogenes protoplasts and after culturing of the bacteria a complete bacterial gene transfer vector system was created, able to invade human brain tumor cells and to deliver the foreign genes. More than 70% of 293T cells, a human renal epithelial cell line, could succesfully transfected in the developed transfer procedure. However in glioblastoma cells this transfer rate could not increased up to 10%. This number should be reached at least to detect significant therapeutic effects, for instance in suicide gene transfer protocols. By optimizing more factors of the three interacting instances (bacterium, plasmid vector and host cell) a higher transfer rate could result.

Published

2006

22. Foreign gene transfer into glioblastoma cells using listeria monocytogenes vector systems

Author

Schulz, Chris and Neurochirurgische Klinik und Institut für Mikrobiologie

Subjects

glioblastoma, ddc:610, Glioblastom, gene transfer, bacteria, Medical sciences Medicine, Gentransfer, Bakterien

Abstract

In dieser Arbeit werden Experimente zum Gentransfer in humane Glioblastomzellen mit einem Genvektorsystem, basierend auf dem fakultativ intrazellulären Bakterium Listeria moncytogenes 1/2a, beschrieben. Die Untersuchung der Listerieninvasion in 2 etablierte Gliomzellinien sowie 27 Primärkulturen intraoperativ entnommener Hirntumorpräparate zeigte, daß L.monocytogenes in der Lage ist, humane Hirntumorzellen zu invadieren. Die stärkste absolute Listerien-Wildtypinvasion wurde dabei unter den astrozytären Tumorzellen beobachtet. Die Invasion in diese Tumorzellen war deutlich von der Aktivität der bakteriellen invasiven Virulenzgene Internalin A und B abhängig. Die plasmidgesteuerte Überexpression dieser Virulenzgene in den verwendeten Listerienstämmen resultierte gegenüber Wildtyplisterien in einer auf 215% gesteigerten mittleren Invasion in astrozytäre Tumorzellen. Durch Deletion beider Internalingene hingegen wurde die bakterielle Invasion in astrozytäre Zellen im Mittel auf 50% reduziert. Als Reportergene des Fremdgentransfers wurden lacZ und EGFP gewählt. Mit hierfür konstruierten Plasmidvektoren konnte per Lipofektion in astrozytäre Zellen die intrazelluläre Fremdgenaktivität festgestellt werden. Durch Transformation der Plasmidvektoren in Listeria monocytogenes1/2a wurden komplementierte Listerien-Stämme generiert, deren Eignung zum vektoriellen Fremdgentransfer in astrozytäre Zellen zu untersuchen war. Derart komplementierte Wildtypstämme von Listeria monocytogenes waren in der Lage, die gewählten Reportergene in humane Zellen zu transportieren. Transferraten von bis zu 70% wurden in Zellen der epithelialen Zellinie 293T beobachtet. Die Transfereffizienz in den untersuchten astrozytären Zellen lag zwischen 3-5%. Eine Transferrate von mehr als 10% sollte für einen therapeutischen Gentransfer (von beispielsweise Suizidgenen) angestrebt werden. Unter anderem durch Veränderung der Virulenzfaktorausstattung des Vektors, spezifiziertes Targeting der Wirtszelle und durch Optimierung der Fremdgene für die intrazelluläre Transkription und Translation könnte eine weitere Steigerung der Transfereffizienz erreicht werden. Experiments for gene transfer into human glioblastoma cells using the facultative intracellular bacterium listeria monocytogenes are described in the presented paper. Examination of bacterial invasion into stable glioblastoma cells and primary cell cultures of different intracranial tumors did show, that listeria are able to enter these cells, depending on the cell origin and the existing bacterial virulence factors. The strongest absolute invasion of wild type listeria monocytogenes was observed in cells of astrocytic origin. Using bacterial mutants with deletion of the virulence genes internalin A and B results in a distinct reduced invasion in astrocytic cells (50%), whereas overexpression of this genes by a privileged transcribed plasmid could essentially increase the invasion number of the listeria mutants (215%). For the gene transfer studies two reporter genes, lacZ and EGFP, in special constructed plasmids were used. Via lipofection these reporter gene containing plasmids were conducted into human cells and the activity of the foreign genes was observed by fluorescens microscopy and the b-galactosidase staining assay. These reporter gene containing plasmids were transfered to listeria monocytogenes protoplasts and after culturing of the bacteria a complete bacterial gene transfer vector system was created, able to invade human brain tumor cells and to deliver the foreign genes. More than 70% of 293T cells, a human renal epithelial cell line, could succesfully transfected in the developed transfer procedure. However in glioblastoma cells this transfer rate could not increased up to 10%. This number should be reached at least to detect significant therapeutic effects, for instance in suicide gene transfer protocols. By optimizing more factors of the three interacting instances (bacterium, plasmid vector and host cell) a higher transfer rate could result.

Published

2006

23. [Rare tumors of the parotid gland. Lymphadenoma of a sebaceous gland and extracranial metastasis from glioblastoma]

Author

U, Kühn, H H, Köhler, and P, Jecker

Subjects

Adenoma, Diagnosis, Differential, Male, Brain Neoplasms, Biopsy, Needle, Humans, Parotid Gland, Middle Aged, Glioblastoma, Temporal Lobe, Aged, Parotid Neoplasms, Ultrasonography

Abstract

Tumors of the parotid gland can be benign or malignant lesions.The pathophysiology of rare tumors of the parotid gland is often not sufficiently explored in this paper two rare histological entities are described. In one patient a benign sebaceous lymph-adenoma was histologically diagnosed. This type of tumor accounts for only 0.196 of all adenomas. The international literature is not conclusive about whether the tumor originates in the parotid gland itself or in the parotid lymph nodes. The second patient presented with a metastasis from a glioblastoma in the parotid gland. Again, the mechanism for metastasis of an intra-cerebral tumor to the parotid gland remains unknown. Iatrogenic seeding during a neurosurgical intervention is a probable explanation. The actual clinical course of his patient and the cases described in literature render surgical removal of such a metastasis questionable.

Published

2003