Search

Your search keyword '"Volker Ehemann"' showing total 125 results
Start Over Author "Volker Ehemann"
125 results on '"Volker Ehemann"'

1. Flow Cytometry Detection of Sperm DNA Fragmentation and Apoptotic Markers in the Semen of Infertile Males

Author

Huda Mossa Omran, Moiz Bakhiet, and Volker Ehemann

Subjects
Gynecology and obstetrics, RG1-991
Abstract

The effect of sperm molecular defects on fertilization and pregnancy outcome after assisted reproductive therapy (ART) is widely documented by both research and clinical societies. Sperm DNA fragmentation and abnormal chromatin condensation represent critical causes of male infertility. Advanced androgenic techniques for accurately identifying molecular defects help in selecting an appropriate treatment strategy. Additionally, specific markers of apoptosis are increasingly important in predicting male infertility. The ability of flow cytometry to estimate the quantity of sperm with DNA fragmentation or damage and multifactor measurements in immotile sperm have made this developed technique essential in fertility centers. The study is aimed at assessing the level of DNA fragmentation and apoptosis by measuring flow cytometry using new techniques. Flow cytometry analysis revealed a varying degree of DNA damage. It was able to quantify the degree of impairment even in samples with minimal DNA fragmentation. DNA damage was observed even in samples that were considered normal with a routine semen analysis. Flow cytometry was sensitive to changes in sperm apoptosis. Elevated p53 activity levels were associated with high DNA fragmentation. Meanwhile, B-cell lymphoma 2 (Bcl-2) activities showed a different pattern. In conclusion, flow cytometry for sperm DNA fragmentation and markers of apoptosis can be a valuable tool in assisted reproductive centers.

Published
2021
Full Text
View/download PDF

2. Binding of the Phage Display Derived Peptide CaIX-P1 on Human Colorectal Carcinoma Cells Correlates with the Expression of Carbonic Anhydrase IX

Author

Uwe Haberkorn, Jürgen Debus, Nuh N. Rahbari, Susanne Krämer, Volker Ehemann, Shoaib Rana, and Vasileios Askoxylakis

Subjects
peptide, phage display, colorectal carcinoma, targeting, imaging, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Phage display represents an attractive screening strategy for the identification of novel, specific binding ligands that could be used for tumor targeting. Recently, a new peptide (CaIX-P1) with affinity for human carbonic anhydrase IX (CAIX) was identified and evaluated. The aim of the present study is to characterize the properties of CaIX-P1 for targeting human colorectal carcinoma and investigate the correlation of peptide binding with the expression of carbonic anhydrase IX. Human colorectal carcinoma HCT116 and HT29 cells were investigated for CAIX expression using Western Blot analysis. Binding and competition studies of 125I-radiolabeled CaIX-P1 were performed on HCT116 cells in vitro. FACS analysis and fluorescence microscopy studies were carried out after cell incubation with fluorescein-labeled CaIX-P1 and rhodamine-labeled anti-human CAIX-mAb. Our studies revealed an enhanced in vitro expression of carbonic anhydrase IX in HCT116 and HT29 cells with increasing cell density. Binding of 125I-labeled-CaIX-P1 on HCT116 cells increased with increasing cell density and correlated to the CAIX expression. FACS analysis demonstrated a correlation of cell labeling between FITC-CaIX-P1 and rhodamine-labeled anti-CAIX-mAb in both HCT116 and HT29 cells. The results of our study indicate that the phage display identified peptide CaIX-P1 might be an attractive candidate for the development of a ligand targeting CAIX in colorectal cancer.

Published
2012
Full Text
View/download PDF

3. Treatment of glioblastoma multiforme cells with temozolomide-BioShuttle ligated by the inverse Diels-Alder ligation chemistry

Author

Klaus Braun, Manfred Wiessler, Volker Ehemann, Ruediger Pipkorn, Herbert Spring, and et al

Subjects
Therapeutics. Pharmacology, RM1-950
Abstract

Klaus Braun1, Manfred Wiessler1, Volker Ehemann2, Ruediger Pipkorn3, Herbert Spring4, Juergen Debus5, Bernd Didinger5, Mario Koch3, Gabriele Muller6, Waldemar Waldeck61German Cancer Research Center, Dept of Imaging and Radiooncology, Heidelberg, Germany; 2University of Heidelberg, Institute of Pathology, Heidelberg, Germany; 3German Cancer Research Center, Central Peptide Synthesis Unit, Heidelberg, Germany; 4German Cancer Research Center, Dept of Structural Analysis of Gene Structure and Function, Heidelberg, Germany; 5University of Heidelberg, Dept of Radiation Oncology, Heidelberg, Germany; 6German Cancer Research Center,Division of Biophysics of Macromolecules, Heidelberg, GermanyAbstract: Recurrent glioblastoma multiforme (GBM), insensitive against most therapeutic interventions, has low response and survival rates. Temozolomide (TMZ) was approved for second-line therapy of recurrent anaplastic astrocytoma. However, TMZ therapy in GBM patients reveals properties such as reduced tolerability and inauspicious hemogram. The solution addressed here concerning GBM therapy consolidates and uses the potential of organic and peptide chemistry with molecular medicine. We enhanced the pharmacologic potency with simultaneous reduction of unwanted adverse reactions of the highly efficient chemotherapeutic TMZ. The TMZ connection to transporter molecules (TMZ-BioShuttle) was investigated, resulting in a much higher pharmacological effect in glioma cell lines and also with reduced dose rate. From this result we can conclude that a suitable chemistry could realize the ligation of pharmacologically active, but sensitive and highly unstable pharmaceutical ingredients without functional deprivation. The TMZ-BioShuttle dramatically enhanced the potential of TMZ for the treatment of brain tumors and is an attractive drug for combination chemotherapy.Keywords: drug delivery, carrier molecules, facilitated transport, glioblastoma multiforme, temozolomide

Published
2009

5. Stathmin regulates keratinocyte proliferation and migration during cutaneous regeneration.

Author

Sabrina Schmitt, Kai Safferling, Kathi Westphal, Manuel Hrabowski, Ute Müller, Peter Angel, Lars Wiechert, Volker Ehemann, Benedikt Müller, Stefan Holland-Cunz, Damian Stichel, Nathalie Harder, Karl Rohr, Günter Germann, Franziska Matthäus, Peter Schirmacher, Niels Grabe, and Kai Breuhahn

Subjects
Medicine, Science
Abstract

Cutaneous regeneration utilizes paracrine feedback mechanisms to fine-tune the regulation of epidermal keratinocyte proliferation and migration. However, it is unknown how fibroblast-derived hepatocyte growth factor (HGF) affects these mutually exclusive processes in distinct cell populations. We here show that HGF stimulates the expression and phosphorylation of the microtubule-destabilizing factor stathmin in primary human keratinocytes. Quantitative single cell- and cell population-based analyses revealed that basal stathmin levels are important for the migratory ability of keratinocytes in vitro; however, its expression is moderately induced in the migration tongue of mouse skin or organotypic multi-layered keratinocyte 3D cultures after full-thickness wounding. In contrast, clearly elevated stathmin expression is detectable in hyperproliferative epidermal areas. In vitro, stathmin silencing significantly reduced keratinocyte proliferation. Automated quantitative and time-resolved analyses in organotypic cocultures demonstrated a high correlation between Stathmin/phospho-Stathmin and Ki67 positivity in epidermal regions with proliferative activity. Thus, activation of stathmin may stimulate keratinocyte proliferation, while basal stathmin levels are sufficient for keratinocyte migration during cutaneous regeneration.

Published
2013
Full Text
View/download PDF

6. Sensitivity of malignant peripheral nerve sheath tumor cells to TRAIL is augmented by loss of NF1 through modulation of MYC/MAD and is potentiated by curcumin through induction of ROS.

Author

David E Reuss, Jana Mucha, Christian Hagenlocher, Volker Ehemann, Lan Kluwe, Victor Mautner, and Andreas von Deimling

Subjects
Medicine, Science
Abstract

Malignant peripheral nerve sheath tumor (MPNST) is a rare aggressive form of sarcoma often associated with the tumor syndrome neurofibromatosis type 1 (NF1). We investigated the effects of tumor necrosis factor-related apoptosis inducing ligand (TRAIL) on NF1 associated MPNST and determinants of TRAIL sensitivity. MPNST cell lines with complete neurofibromin deficiency were sensitive to apoptotic cell death induced by TRAIL whereas MPNST cells with retained neurofibromin expression or normal human Schwann cells were resistant. Increased sensitivity to TRAIL was associated with overexpression of death receptors, especially DR5. Re-expression of the GAP related domain of neurofibromin (NF1-GRD) suppressed DR5 expression and decreased sensitivity to TRAIL. We show that death receptor expression and TRAIL sensitivity critically depend on c-MYC and that c-MYC amounts are increased by MEK/ERK and PI3K/AKT signalling pathways which are suppressed by neurofibromin. Furthermore PI3K/AKT signalling strongly suppresses the MYC-antagonist MAD1 which significantly contributes to TRAIL sensitivity. Re-expression of the NF1-GRD decreased c-MYC and increased MAD1 amounts suggesting that neurofibromin influences TRAIL sensitivity at least in part by modulating the MYC/MAX/MAD network. The phytochemical curcumin further increased the sensitivity of neurofibromin deficient MPNST cells to TRAIL. This was presumably mediated by ROS, as it correlated with increased ROS production, was blocked by N-acetylcysteine and mimicked by exogenous ROS.

Published
2013
Full Text
View/download PDF

7. Data from High Skp2 Expression Characterizes High-Risk Neuroblastomas Independent of MYCN Status

Author

Manfred Schwab, Javed Khan, Axel Benner, Ivo Leuschner, Karen Ernestus, Benedikt Brors, Volker Ehemann, Ruprecht Wiedemeyer, Rainer König, Matthias Fischer, Werner Lutz, Jun S. Wei, Kai-Oliver Henrich, and Frank Westermann

Abstract

Purpose: Amplified MYCN oncogene defines a subgroup of neuroblastomas with poor outcome. However, a substantial number of MYCN single-copy neuroblastomas exhibits an aggressive phenotype similar to that of MYCN-amplified neuroblastomas even in the absence of high MYCN mRNA and/or protein levels.Experimental Design: To identify shared molecular mechanisms that mediate the aggressive phenotype in MYCN-amplified and single-copy high-risk neuroblastomas, we defined genetic programs evoked by ectopically expressed MYCN in vitro and analyzed them in high-risk versus low-risk neuroblastoma tumors (n = 49) using cDNA microarrays. Candidate gene expression was validated in a separate cohort of 117 patients using quantitative PCR, and protein expression was analyzed in neuroblastoma tumors by immunoblotting and immunohistochemistry.Results: We identified a genetic signature characterized by a subset of MYCN/MYC and E2F targets, including Skp2, encoding the F-box protein of the SCFSkp2 E3-ligase, to be highly expressed in high-risk neuroblastomas independent of amplified MYCN. We validated the findings for Skp2 and analyzed its expression in relation to MYCN and E2F-1 expression in a separate cohort (n = 117) using quantitative PCR. High Skp2 expression proved to be a highly significant marker of dire prognosis independent of both MYCN status and disease stage, on the basis of multivariate analysis of event-free survival (hazard ratio, 3.54; 95% confidence interval, 1.56-8.00; P = 0.002). Skp2 protein expression was inversely correlated with expression of p27, the primary target of the SCFSkp2 E3-ligase, in neuroblastoma tumors.Conclusion: Skp2 may have a key role in the progression of neuroblastomas and should make an attractive target for therapeutic approaches.

Published
2023

9. Supplementary Table 1 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Table 1 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

11. Data from CAMTA1, a 1p36 Tumor Suppressor Candidate, Inhibits Growth and Activates Differentiation Programs in Neuroblastoma Cells

Author

Frank Westermann, Manfred Schwab, Rainer König, Axel Benner, Matthias Fischer, Daniel Muth, Sina Gogolin, Hedwig Deubzer, Volker Ehemann, Johannes Schulte, Tobias Bauer, and Kai-Oliver Henrich

Abstract

A distal portion of human chromosome 1p is often deleted in neuroblastomas and other cancers and it is generally assumed that this region harbors one or more tumor suppressor genes. In neuroblastoma, a 261 kb region at 1p36.3 that encompasses the smallest region of consistent deletion pinpoints the locus for calmodulin binding transcription activator 1 (CAMTA1). Low CAMTA1 expression is an independent predictor of poor outcome in multivariate survival analysis, but its potential functionality in neuroblastoma has not been explored. In this study, we used inducible cell models to analyze the impact of CAMTA1 on neuroblastoma biology. In neuroblastoma cells that expressed little endogenous CAMTA1, its ectopic expression slowed cell proliferation, increasing the relative proportion of cells in G1/G0 phases of the cell cycle, inhibited anchorage-independent colony formation, and suppressed the growth of tumor xenografts. CAMTA1 also induced neurite-like processes and markers of neuronal differentiation in neuroblastoma cells. Further, retinoic acid and other differentiation- inducing stimuli upregulated CAMTA1 expression in neuroblastoma cells. Transciptome analysis revealed 683 genes regulated on CAMTA1 induction and gene ontology analysis identified genes consistent with CAMTA1-induced phenotypes, with a significant enrichment for genes involved in neuronal function and differentiation. Our findings define properties of CAMTA1 in growth suppression and neuronal differentiation that support its assignment as a 1p36 tumor suppressor gene in neuroblastoma. Cancer Res; 71(8); 3142–51. ©2011 AACR.

Published
2023

12. Data from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Dynamic instability of the microtubule network modulates processes such as cell division and motility, as well as cellular morphology. Overexpression of the microtubule-destabilizing phosphoprotein stathmin is frequent in human malignancies and represents a promising therapeutic target. Although stathmin inhibition gives rise to antineoplastic effects, additional and functionally redundant microtubule-interacting proteins may attenuate the efficiency of this therapeutic approach. We have systematically analyzed the expression and potential protumorigenic effects of stathmin family members in human non–small cell lung cancer (NSCLC). Both stathmin and stathmin-like 3 (SCLIP) were overexpressed in adenocarcinoma as well as squamous cell carcinoma (SCC) tissues and induced tumor cell proliferation, migration, and matrix invasion in respective cell lines. Accordingly, reduced stathmin and SCLIP levels affected cell morphology and were associated with a less malignant phenotype. Combined inhibition of both factors caused additive effects on tumor cell motility, indicating partial functional redundancy. Because stathmin and SCLIP expression significantly correlated in NSCLC tissues, we searched for common upstream regulators and identified the far upstream sequence element-binding protein-1 (FBP-1) as a pivotal inducer of several stathmin family members. Our results indicate that the coordinated overexpression of microtubule-destabilizing factors by FBP-1 is a critical step to facilitate microtubule dynamics and subsequently increases proliferation and motility of tumor cells. [Cancer Res 2009;69(6):2234–43]

Published
2023

13. Supplementary Figure 4 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure 4 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

14. Supplementary Table 1 from CAMTA1, a 1p36 Tumor Suppressor Candidate, Inhibits Growth and Activates Differentiation Programs in Neuroblastoma Cells

Author

Frank Westermann, Manfred Schwab, Rainer König, Axel Benner, Matthias Fischer, Daniel Muth, Sina Gogolin, Hedwig Deubzer, Volker Ehemann, Johannes Schulte, Tobias Bauer, and Kai-Oliver Henrich

Abstract

Supplementary Table 1 from CAMTA1, a 1p36 Tumor Suppressor Candidate, Inhibits Growth and Activates Differentiation Programs in Neuroblastoma Cells

Published
2023

15. Supplementary Figure 5 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure 5 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

16. Supplementary Figure Legends 1-5 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure Legends 1-5 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

17. Supplementary Figure 2 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure 2 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

18. Supplementary Figure 1 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure 1 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

20. Supplementary Figure 3 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Author

Kai Breuhahn, Peter Schirmacher, Peter Huber, Ruprecht Kuner, Philipp Albert Schnabel, Volker Ehemann, Georg Gdynia, Roland Penzel, Hans Hoffmann, Michael Meister, Thomas Muley, Martina Keith, Michaela Bissinger, Arne Warth, Esther Herpel, Mona Malz, and Stephan Singer

Abstract

Supplementary Figure 3 from Coordinated Expression of Stathmin Family Members by Far Upstream Sequence Element-Binding Protein-1 Increases Motility in Non–Small Cell Lung Cancer

Published
2023

21. Data from Transcriptional Repression of SKP2 Is Impaired in MYCN-Amplified Neuroblastoma

Author

Frank Westermann, Manfred Schwab, Paul Gillespie, Volker Ehemann, Kai-Oliver Henrich, Matthias Fischer, Sina Gogolin, Claudia Beisel, Julia Batzler, Christina Pöhler, Emily Beckett, Isabella Eckerle, Seda Ghazaryan, and Daniel Muth

Abstract

The cell cycle regulator, SKP2, is overexpressed in various cancers and plays a key role in p27 degradation, which is involved in tumor cell dedifferentiation. Little is known about the mechanisms leading to impaired SKP2 transcriptional control in tumor cells. We used neuroblastoma as a model to study SKP2 regulation because SKP2 transcript levels gradually increase with aggressiveness of neuroblastoma subtypes. The highest SKP2 levels are found in neuroblastomas with amplified MYCN. Accordingly, we found 5.5-fold (range, 2–9.5) higher SKP2 core promoter activity in MYCN-amplified cells. Higher SKP2 core promoter activity in MYCN-amplified cells is mediated through a defined region at the transcriptional start site. This region includes a specific E2F-binding site that makes SKP2 activation largely independent of mitogenic signals integrated through the SP1/ELK-1 site. We show by chromatin immunoprecipitation that SKP2 activation through the transcriptional start site in MYCN-amplified cells is associated with the low abundance of pRB-E2F1 complexes bound to the SKP2 promoter. Transcriptional control of SKP2 through this regulatory mechanism can be reestablished in MYCN-amplified cells by restoring pRB activity using selective small compound inhibitors of CDK4. In contrast, doxorubicin or nutlin-3 treatment—both leading to p53-p21 activation—or CDK2 inhibition had no effect on SKP2 regulation in MYCN-amplified cells. Together, this implies that deregulated MYCN protein levels in MYCN-amplified neuroblastoma cells activate SKP2 through CDK4 induction, abrogating repressive pRB-E2F1 complexes bound to the SKP2 promoter. Cancer Res; 70(9); 3791–802. ©2010 AACR.

Published
2023

22. NIR-Cyanine Dye Linker: a Promising Candidate for Isochronic Fluorescence Imaging in Molecular Cancer Diagnostics and Therapy Monitoring

Author

Klaus Braun, Hans-Hermann Schrenk, Jürgen Debus, Volker Ehemann, Manfred Wiessler, Dorde Komljenovic, Ruediger Pipkorn, and Waldemar Waldeck

Subjects
Fluorescence-lifetime imaging microscopy, inverse Diels-Alder reaction, Medicine (miscellaneous), multimodal imaging, Antineoplastic Agents, Nanotechnology, Peptide, 02 engineering and technology, solid phase peptide synthesis, 010402 general chemistry, near infrared imaging, 01 natural sciences, molecular diagnostics, chemistry.chemical_compound, Tetrazine, Cell Line, Tumor, Neoplasms, Peptide synthesis, Animals, Molecular Targeted Therapy, Precision Medicine, Cyanine, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Fluorescent Dyes, chemistry.chemical_classification, Click chemistry, Chemistry, Optical Imaging, 021001 nanoscience & nanotechnology, Combinatorial chemistry, Rats, 0104 chemical sciences, Molecular Diagnostic Techniques, fluorescent dye, 0210 nano-technology, Linker, Research Paper, Conjugate
Abstract

Personalized anti-cancer medicine is boosted by the recent development of molecular diagnostics and molecularly targeted drugs requiring rapid and efficient ligation routes. Here, we present a novel approach to synthetize a conjugate able to act simultaneously as an imaging and as a chemotherapeutic agent by coupling functional peptides employing solid phase peptide synthesis technologies. Development and the first synthesis of a fluorescent dye with similarity in the polymethine part of the Cy7 molecule whose indolenine-N residues were substituted with a propylene linker are described. Methylating agent temozolomide is functionalized with a tetrazine as a diene component whereas Cy7-cell penetrating peptide conjugate acts as a dienophilic reaction partner for the inverse Diels-Alder click chemistry-mediated ligation route yielding a theranostic conjugate, 3-mercapto-propionic-cyclohexenyl-Cy7-bis-temozolomide-bromide-cell penetrating peptide. Synthesis route described here may facilitate targeted delivery of the therapeutic compound to achieve sufficient local concentrations at the target site or tissue. Its versatility allows a choice of adequate imaging tags applicable in e.g. PET, SPECT, CT, near-infrared imaging, and therapeutic substances including cytotoxic agents. Imaging tags and therapeutics may be simultaneously bound to the conjugate applying click chemistry. Theranostic compound presented here offers a solid basis for a further improvement of cancer management in a precise, patient-specific manner.

Published
2016

23. Concomitant expression of far upstream element (FUSE ) binding protein (FBP ) interacting repressor (FIR) and its splice variants induce migration and invasion of non-small cell lung cancer (NSCLC) cells

Author

Michael Meister, Arne Warth, Volker Ehemann, Thomas Muley, Alistair M. Middleton, Peter Schirmacher, Yi Yin, Dirk Drasdo, Franziska Matthäus, Kai Breuhahn, J Schmitt, Michael Bovet, Stephan Singer, Margarita González-Vallinas, Benedikt Müller, Esther Herpel, Mona Malz, and Damian Stichel

Subjects
Gene isoform, Pathology, medicine.medical_specialty, Cell growth, Cell, non-small cell lung cancer (NSCLC), Repressor, Biology, medicine.disease, 3. Good health, Pathology and Forensic Medicine, Exon, medicine.anatomical_structure, medicine, Cancer research, Gene silencing, Transcription factor
Abstract

Transcription factors integrate a variety of oncogenic input information, facilitate tumour growth and cell dissemination, and therefore represent promising therapeutic target structures. Because over-expression of DNA-interacting far upstream element binding protein (FBP) supports non-small cell lung cancer (NSCLC) migration, we asked whether its repressor, FBP-interacting repressor (FIR) is functionally inactivated and how FIR might affect NSCLC cell biology. Different FIR splice variants were highly expressed in the majority of NSCLCs, with the highest levels in tumours carrying genomic gains of chromosome 8q24.3, which contained the FIR gene locus. Nuclear FIR expression was significantly enriched at the invasion front of primary NSCLCs, but this did not correlate with tumour cell proliferation. FIR accumulation was associated with worse patient survival and tumour recurrence; in addition, FIR over-expression significantly correlated with lymph node metastasis in squamous cell carcinomas (SCCs). In vitro, we applied newly developed methods and modelling approaches for the quantitative and time-resolved description of the pro-migratory and pro-invasive capacities of SCC cells. siRNA-mediated silencing of all FIR variants significantly reduced the speed and directional movement of tumour cells in all phases of migration. Furthermore, sprouting efficiency and single cell invasiveness were diminished following FIR inhibition. Interestingly, the silencing of FIR isoforms lacking exon 2 (FIRΔexon2) alone was sufficient to reduce lateral migration and invasion. In summary, by using scale-spanning data derived from primary human tissues, quantitative cellular analyses and mathematical modelling, we have demonstrated that concomitant over-expression of FIR and its splice variants drives NSCLC migration and dissemination. Copyright © 2015 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2015

24. The HMGB1 protein sensitizes colon carcinoma cells to cell death triggered by pro-apoptotic agents

Author

Chengcheng Christine Zhang, Wilfried Roth, Volker Ehemann, and Georg Gdynia

Subjects
Cancer Research, Programmed cell death, medicine.medical_treatment, Cell, Apoptosis, chemical and pharmacologic phenomena, Biology, Piperazines, Nitrophenols, TNF-Related Apoptosis-Inducing Ligand, medicine, Humans, Cytotoxic T cell, HMGB1 Protein, Sulfonamides, Biphenyl Compounds, Cell cycle, Glycyrrhizic Acid, HCT116 Cells, Recombinant Proteins, Cell biology, Cytokine, medicine.anatomical_structure, Proto-Oncogene Proteins c-bcl-2, Oncology, Colonic Neoplasms, Cancer research, Signal transduction, Apoptosis Regulatory Proteins, Intracellular
Abstract

The HMGB1 protein has multiple functions in tumor biology and can act both as a transcription factor and as a cytokine. HMGB1 is released during cell death, and in our previous studies we demonstrated that HMGB1 induces a distinct, necrosis-like cell death in glioblastoma. In epithelial malignant tumors such as colorectal cancer (CRC), the HMGB1-dependent effects show cross-talk with apoptotic signal transduction. Treatment of CRC cells with low concentrations of recombinant HMGB1 results in dose-dependent cytotoxicity which is morphologically characterized by the formation of giant mitochondria and does not share features of apoptosis. HMGB1-triggered cell death is associated with intracellular ROS release, and overexpression of Bcl-2 blocks both the increase of ROS as well as HMGB1-dependent cell death. Importantly, treatment with recombinant HMGB1 or overexpression of endogenous HMGB1 strongly sensitizes CRC cells to the cytotoxic activity of the pro-apoptotic death ligand TRAIL as well as the small molecule Bcl-2 family inhibitor ABT‑737. Moreover, treatment of CRC cells with TRAIL or ABT‑737 induces a release of endogenous HMGB1 into the extracellular space, and preincubation with glycyrrhizin, an HMGB1 inhibitor, significantly inhibits induction of cell death by TRAIL and ABT‑737, suggesting that HMGB1 functionally contributes to the execution of cell death triggered by pro-apoptotic agents. Finally, we investigated the expression of HMGB1 in human CRC tumor samples and found that loss of HMGB1 expression is associated with a more aggressive phenotype and a more advanced stage of disease in patients with CRC. Altogether, our findings demonstrate a functional link between cytotoxic signaling cascades triggered by HMGB1 and pro-apoptotic agents leading to an HMGB1-dependent sensitization to CRC cell death. Thus, a further evaluation of recombinant HMGB1 as part of an experimental combination treatment of CRC seems warranted.

Published
2014

25. Protumorigenic role of Timeless in hepatocellular carcinoma

Author

Volker Ehemann, Peter Schemmer, Heba M. El-Zawahry, Nahla Elgohary, R Pellegrino, Magdy M. Saber, Ahmed A. Zeeneldin, Peter Schirmacher, Thomas Longerich, Olaf Neumann, Robert Geffers, and Helmholtz Centre for infection research, Inhoffenstr. 7, 38124 Braunschweig, Germany.

Subjects
Adult, Male, Cancer Research, Carcinoma, Hepatocellular, Adolescent, Carcinogenesis, Timeless, Cell, EEF1A2, Cell Cycle Proteins, Biology, Peptide Elongation Factor 1, medicine, Protein biosynthesis, Humans, RNA, Small Interfering, Aged, Gene knockdown, Liver Neoplasms, Intracellular Signaling Peptides and Proteins, Middle Aged, Cell cycle, HCCS, Gene Expression Regulation, Neoplastic, Checkpoint Kinase 2, medicine.anatomical_structure, Oncology, Cancer research, Phosphorylation, Female
Abstract

The mammalian timeless (TIM) protein interacts with proteins of the endogenous clock and essentially contributes to the circadian rhythm. In addition, TIM is involved in maintenance of chromosome integrity, growth control and development. Thus, we hypothesized that TIM may exert a potential protumorigenic function in human hepatocarcinogenesis. TIM was overexpressed in a subset of human HCCs both at the mRNA and the protein level. siRNA-mediated knockdown of TIM reduced cell viability due to the induction of apoptosis and G2 arrest. The latter was mediated via CHEK2 phosphorylation. In addition, siRNA-treated cells showed a significantly reduced migratory capacity and reduced expression levels of various proteins. Mechanistically, TIM directly interacts with the eukaryotic elongation factor 1A2 (EEF1A2), which binds to actin filaments to promote tumor cell migration. siRNA-mediated knockdown of TIM reduced EEF1A2 protein levels thereby affecting ribosomal protein biosynthesis. Thus, overexpression of TIM exerts oncogenic function in human HCCs, which is mediated via CHEK2 and EEF1A2.

Published
2014

26. p19-INK4d inhibits neuroblastoma cell growth, induces differentiation and is hypermethylated and downregulated in MYCN-amplified neuroblastomas

Author

Axel Benner, Volker Ehemann, Stefan M. Pfister, Daniel Dreidax, Sebastian Bender, Sven Lindner, Maral Saadati, Matthias Fischer, Johannes H. Schulte, Christina Schröder, Thomas Schwarzl, Steffen Bannert, Christopher C. Oakes, Frank Westermann, Kai-Oliver Henrich, and David J. Duffy

Subjects
Adult, Male, Antimetabolites, Antineoplastic, Adolescent, Nervous System Neoplasms, Medizin, Tretinoin, Biology, Decitabine, N-Myc Proto-Oncogene Protein, Epigenesis, Genetic, Neuroblastoma, chemistry.chemical_compound, Cell Line, Tumor, Genetics, medicine, Humans, Cyclin-Dependent Kinase Inhibitor p19, Child, neoplasms, Molecular Biology, Genetics (clinical), Neoplasm Staging, Neurons, Oncogene Proteins, Regulation of gene expression, Infant, Newborn, Infant, Nuclear Proteins, Cell Differentiation, General Medicine, DNA Methylation, Cell cycle, medicine.disease, Survival Analysis, Demethylating agent, Gene Expression Regulation, Neoplastic, chemistry, Child, Preschool, embryonic structures, DNA methylation, Azacitidine, Cancer research, Female, Signal transduction, CDK inhibitor, Signal Transduction
Abstract

Uncontrolled cell cycle entry, resulting from deregulated CDK-RB1-E2F pathway activity, is a crucial determinant of neuroblastoma cell malignancy. Here we identify neuroblastoma-suppressive functions of the p19-INK4d CDK inhibitor and uncover mechanisms of its repression in high-risk neuroblastomas. Reduced p19-INK4d expression was associated with poor event-free and overall survival and neuroblastoma risk factors including amplified MYCN in a set of 478 primary neuroblastomas. High MYCN expression repressed p19-INK4d mRNA and protein levels in different neuroblastoma cell models with conditional MYCN expression. MassARRAY and 450K methylation analyses of 105 primary neuroblastomas uncovered a differentially methylated region within p19-INK4d. Hypermethylation of this region was associated with reduced p19-INK4d expression. In accordance, p19-INK4d expression was activated upon treatment with the demethylating agent, 2'-deoxy-5-azacytidine, in neuroblastoma cell lines. Ectopic p19-INK4d expression decreased viability, clonogenicity and the capacity for anchorage-independent growth of neuroblastoma cells, and shifted the cell cycle towards the G1/0 phase. p19-INK4d also induced neurite-like processes and markers of neuronal differentiation. Moreover, neuroblastoma cell differentiation, induced by all-trans retinoic acid or NGF-NTRK1-signaling, activated p19-INK4d expression. Our findings pinpoint p19-INK4d as a neuroblastoma suppressor and provide evidence for MYCN-mediated repression and for epigenetic silencing of p19-INK4d by DNA hypermethylation in high-risk neuroblastomas.

Published
2014

27. Flow cytometric characterization of tumor subpopulations in three sublines of the dunning R3327 rat prostate tumor model

Author

Eric W. Hahn, Peter E. Huber, Peter Peschke, Jürgen Debus, Volker Ehemann, Christin Glowa, and Christian P. Karger

Subjects
Pathology, medicine.medical_specialty, Cluster of differentiation, medicine.diagnostic_test, CD24, Urology, Cell, CD44, Cell cycle, Biology, Cell sorting, Flow cytometry, medicine.anatomical_structure, Oncology, Prostate, Cancer research, medicine, biology.protein
Abstract

BACKGROUND Subsets of tumor cells were characterized by mapping DNA ploidy patterns in correlation with established cell surface markers in three non-treated sublines of the Dunning R3327 prostate tumor system representing different progressional stages. METHODS Flow cytometry was used to analyze DNA-index, cell cycle distribution as well as multiparametric aquisition of single and combined cell surface markers in single cell suspensions of frozen tumor tissues. RESULTS The three Dunning prostate tumor sublines clearly differ in their ploidy status. In addition each tumor subline displays a characteristic cell surface marker profile, which is correlated with the cell cycle phase and the amount of genomic alterations. CONCLUSIONS In a feasibility study we have shown that cross-reacting antibodies to human cell surface markers stain discrete tumor subpopulations in three sublines of the Dunning tumor model. Although it remains presently uncertain, which cell surface markers are most suitable for cell sorting to display cancer initiating (CIC) properties following subcutaneous or orthotopic grafting, the model may be useful for mechanistic investigations of putative stem-like tumor subpopulations and their significance in response to radio- or chemotherapy. Prostate 73: 1710–1720, 2013. © 2013 Wiley Periodicals, Inc.

Published
2013

28. Radiosensitization by histone deacetylase inhibition in an osteosarcoma mouse model

Author

Jürgen Debus, Wilko Weichert, Claudia Blattmann, Peter E. Huber, Volker Ehemann, E. Roth, M. Thiemann, A. Christmann, Amir Abdollahi, Andreas E. Kulozik, Albrecht Stenzinger, and Susanne Oertel

Subjects
Cell Survival, Angiogenesis, Bone Neoplasms, Mice, SCID, Radiation Tolerance, Mice, In vivo, Cell Line, Tumor, Radioresistance, Animals, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Radiosensitivity, Osteosarcoma, business.industry, Dose-Response Relationship, Radiation, Radiotherapy Dosage, Chemoradiotherapy, Fas receptor, medicine.disease, Histone Deacetylase Inhibitors, Treatment Outcome, Oncology, Apoptosis, Cancer research, Histone deacetylase, Radiotherapy, Conformal, business
Abstract

Osteosarcomas (OS) are highly malignant and radioresistant tumors. Histone deacetylase inhibitors (HDACi) constitute a novel class of anticancer agents. We sought to investigate the effect of combined treatment with suberoylanilide hydroxamic acid (SAHA) and radiotherapy in OS in vivo. Clonogenic survival of human OS cell lines as well as tumor growth delay of OS xenografts were tested after treatment with either vehicle, radiotherapy (XRT), SAHA, or XRT and SAHA. Tumor proliferation, necrosis, microvascular density, apoptosis, and p53/p21 were monitored by immunohistochemistry. The CD95 pathway was performed by flow cytometry, caspase (3/7/8) activity measurements, and functional inhibition of CD95 death signaling. Combined treatment with SAHA and XRT markedly reduced the surviving fraction of OS cells as compared to XRT alone. Likewise, dual therapy significantly inhibited OS tumor growth in vivo as compared to XRT alone, reflected by reduced tumor proliferation, impaired angiogenesis, and increased apoptosis. Addition of HDACi to XRT led to elevated p53, p21, CD95, and CD95L expression. Inhibition of CD95 signaling reduced HDACi- and XRT-induced apoptosis. Our data show that HDACi increases the radiosensitivity of osteosarcoma cells at least in part via ligand-induced apoptosis. HDACi thus emerge as potentially useful treatment components of OS.

Published
2013

29. Low p14ARF expression in neuroblastoma cells is associated with repressed histone mark status, and enforced expression induces growth arrest and apoptosis

Author

Daniel Muth, Manfred Schwab, Jessica Theißen, Larissa Savelyeva, Frank Westermann, Matthias Fischer, Marc Zapatka, Christina Schroeder, Volker Ehemann, Daniel Dreidax, Elisa M. Hess, Lena M. Brueckner, and Sina Gogolin

Subjects
Male, congenital, hereditary, and neonatal diseases and abnormalities, Gene Expression, Loss of Heterozygosity, Apoptosis, Epigenetic Repression, Biology, Histones, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, p14arf, Cell Line, Tumor, Tumor Suppressor Protein p14ARF, Genetics, medicine, Humans, E2F1, Epigenetics, Promoter Regions, Genetic, neoplasms, Molecular Biology, Cyclin-Dependent Kinase Inhibitor p16, Genetics (clinical), 030304 developmental biology, Comparative Genomic Hybridization, 0303 health sciences, Proto-Oncogene Proteins c-mdm2, General Medicine, medicine.disease, G1 Phase Cell Cycle Checkpoints, eye diseases, Chromatin, Histone, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Mdm2, Female, sense organs, Tumor Suppressor Protein p53, Chromatin immunoprecipitation, Gene Deletion
Abstract

The TP53 tumor suppressor pathway is abrogated by TP53 mutations in the majority of human cancers. Increased levels of wild-type TP53 in aggressive neuroblastomas appear paradox but are tolerated by tumor cells due to co-activation of the TP53 ubiquitin ligase, MDM2. The role of the MDM2 antagonist, p14(ARF), in controlling the TP53-MDM2 balance in neuroblastoma is unresolved. In the present study, we show that conditional p14(ARF) expression substantially suppresses viability, clonogenicity and anchorage-independent growth in p14(ARF)-deficient or MYCN-amplified neuroblastoma cell lines. Furthermore, ectopic 14(ARF) expression induced accumulation of cells in the G1 phase and apoptosis, which was paralleled by accumulation of TP53 and its targets. Comparative genomic hybridization analysis of 193 primary neuroblastomas detected one homozygous deletion of CDKN2A (encoding both p14(ARF) and p16(INK4A)) and heterozygous loss of CDKN2A in 22% of tumors. Co-expression analysis of p14(ARF) and its transactivator, E2F1, in a set of 68 primary tumors revealed only a weak correlation, suggesting that further regulatory mechanisms govern p14(ARF) expression in neuroblastomas. Intriguingly, analyses utilizing chromatin immunoprecipitation revealed different histone mark-defined epigenetic activity states of p14(ARF) in neuroblastoma cell lines that correlated with endogenous p14(ARF) expression but not with episomal p14(ARF) promoter reporter activity, indicating that the native chromatin context serves to epigenetically repress p14(ARF) in neuroblastoma cells. Collectively, the data pinpoint p14(ARF) as a critical factor for efficient TP53 response in neuroblastoma cells and assign p14(ARF) as a neuroblastoma suppressor candidate that is impaired by genomic loss and epigenetic repression.

Published
2013

30. Binding of the Phage Display Derived Peptide CaIX-P1 on Human Colorectal Carcinoma Cells Correlates with the Expression of Carbonic Anhydrase IX

Author

Shoaib Rana, Jürgen Debus, Volker Ehemann, Uwe Haberkorn, Vasileios Askoxylakis, Susanne Krämer, and Nuh N. Rahbari

Subjects
Phage display, Cell, Peptide binding, Peptide, Plasma protein binding, Biology, Article, Catalysis, Inorganic Chemistry, lcsh:Chemistry, HT29 Cells, peptide, phage display, colorectal carcinoma, targeting, imaging, Antigens, Neoplasm, Peptide Library, medicine, Humans, Physical and Theoretical Chemistry, Carbonic Anhydrase IX, Peptide library, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, Carbonic Anhydrases, chemistry.chemical_classification, Organic Chemistry, Antibodies, Monoclonal, General Medicine, HCT116 Cells, Molecular biology, In vitro, digestive system diseases, Computer Science Applications, Kinetics, medicine.anatomical_structure, Microscopy, Fluorescence, Biochemistry, chemistry, lcsh:Biology (General), lcsh:QD1-999, Colorectal Neoplasms, Peptides, Protein Binding
Abstract

Phage display represents an attractive screening strategy for the identification of novel, specific binding ligands that could be used for tumor targeting. Recently, a new peptide (CaIX-P1) with affinity for human carbonic anhydrase IX (CAIX) was identified and evaluated. The aim of the present study is to characterize the properties of CaIX-P1 for targeting human colorectal carcinoma and investigate the correlation of peptide binding with the expression of carbonic anhydrase IX. Human colorectal carcinoma HCT116 and HT29 cells were investigated for CAIX expression using Western Blot analysis. Binding and competition studies of 125I-radiolabeled CaIX-P1 were performed on HCT116 cells in vitro. FACS analysis and fluorescence microscopy studies were carried out after cell incubation with fluorescein-labeled CaIX-P1 and rhodamine-labeled anti-human CAIX-mAb. Our studies revealed an enhanced in vitro expression of carbonic anhydrase IX in HCT116 and HT29 cells with increasing cell density. Binding of 125I-labeled-CaIX-P1 on HCT116 cells increased with increasing cell density and correlated to the CAIX expression. FACS analysis demonstrated a correlation of cell labeling between FITC-CaIX-P1 and rhodamine-labeled anti-CAIX-mAb in both HCT116 and HT29 cells. The results of our study indicate that the phage display identified peptide CaIX-P1 might be an attractive candidate for the development of a ligand targeting CAIX in colorectal cancer.

Published
2012

31. Theranostic cRGD-BioShuttle Constructs Containing Temozolomide- and Cy7 For NIR-Imaging and Therapy

Author

Ute Hennrich, Wolfhard Semmler, Klaus Braun, Volker Ehemann, Manfred Wiessler, Waldemar Waldeck, Twan Lammers, Jörg Peter, Liji Cao, and Rüdiger Pipkorn

Subjects
High interest, targeted Therapy, medicine.medical_treatment, Medicine (miscellaneous), Bioinformatics, Targeted therapy, Temozolomide, medicine, BioShuttle, Ligation chemistry, targeted Imaging, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Click-Chemistry, RGD, business.industry, inverse Diels Alder Reaction, Theranostics, Imaging agent, NIR Imaging, Cancer research, Click chemistry, business, Cyclic RGD, Human breast, Research Paper, medicine.drug, NIR Optical Imaging
Abstract

Theranostics 1, 381-394 (2011). doi:10.7150/thno/v01p0381, Published by Ivyspring, Wyoming, NSW

Published
2011

32. Theranostic cRGD-BioShuttle Constructs Containing Temozolomide- and Cy7 For NIR-Imaging and Therapy

Author

Manfred Wiessler, Ute Hennrich, Rüdiger Pipkorn, Waldemar Waldeck, Liji Cao, Jörg Peter, Volker Ehemann, Wolfhard Semmler, Twan Lammers, Klaus Braun

Subjects
lcsh:R, lcsh:Medicine
Abstract

Innovative and personalized therapeutic approaches result from the identification and control of individual aberrantly expressed genes at the transcriptional and post-transcriptional level. Therefore, it is of high interest to establish diagnostic, therapeutic and theranostic strategies at these levels. In the present study, we used the Diels-Alder Reaction with inverse electron demand (DARinv) click chemistry to prepare a series of cyclic RGD-BioShuttle constructs. These constructs carry the near-infrared (NIR) imaging agent Cy7 and the chemotherapeutic agent temozolomide (TMZ). We evaluated their uptake by and their efficacy against integrin αvβ3-expressing MCF7 human breast carcinoma cells. In addition, using a mouse phantom, we analyzed the suitability of this targeted theranostic agent for NIR optical imaging. We observed that the cyclic RGD-based carriers containing TMZ and/or Cy7 were effectively taken up by αvβ3-expressing cells, that they were more effective than free TMZ in inducing cell death, and that they could be quantitatively visualized using NIR fluorescence imaging. Therefore, these targeted theranostic agents are considered to be highly suitable systems for improving disease diagnosis and therapy.

Published
2011

33. A cyclic-RGD-BioShuttle functionalized with TMZ by DARinv 'Click Chemistry' targeted to αvβ3 integrin for therapy

Author

Klaus Braun, Peter Lorenz, Waldemar Waldeck, Gabriele Müller, Tobias Bäuerle, Rüdiger Pipkorn, Heinz Fleischhacker, Volker Ehemann, and Manfred Wiessler

Subjects
medicine.medical_treatment, targeted Therapy, Cell, Uterine Cervical Neoplasms, Adaptor Systems, Breast Neoplasms, Biology, Peptides, Cyclic, Targeted therapy, Flow cytometry, Inhibitory Concentration 50, Cell Line, Tumor, medicine, Temozolomide, Humans, BioShuttle, Ligation chemistry, Antineoplastic Agents, Alkylating, Cycloaddition, Cell Size, Integrin alphaVbeta3, Click-Chemistry, Linker Systems, RGD, Microscopy, Confocal, medicine.diagnostic_test, inverse Diels Alder Reaction, General Medicine, Flow Cytometry, Dacarbazine, Cell killing, medicine.anatomical_structure, Targeted drug delivery, Tetrazines, Immunology, Click chemistry, Cancer research, Female, Conjugate, Research Paper, HeLa Cells
Abstract

Clinical experiences often document, that a successful tumor control requires high doses of drug applications. It is widely believed that unavoidable adverse reactions could be minimized by using gene-therapeutic strategies protecting the tumor-surrounding healthy tissue as well as the bone-marrow. One new approach in this direction is the use of "Targeted Therapies" realizing a selective drug targeting to gain effectual amounts at the target site, even with drastically reduced application doses. MCF-7 breast cancer cells expressing the α(v)β(3) [alpha(v)beta(3)] integrin receptor are considered as appropriate candidates for such a targeted therapy. The modularly composed BioShuttle carrier consisting of different units designed to facilitate the passage across the cell membranes and for subcellular addressing of diagnostic and/or therapeutic molecules could be considered as an eligible delivery platform. Here we used the cyclic RGD-BioShuttle as a carrier for temozolomide (TMZ) at the α(v)β(3) integrin receptor realizing local TMZ concentrations sufficient for cell killing. The IC50 values are 12 µMol/L in the case of cRGD-BioShuttle-TMZ and 100 µMol/L for underivatized TMZ, which confirms the advantage of TMZ reformulation to realize local concentrations sufficient for cell killing. Our paper focuses on the design, synthesis and application of the cRGD-BioShuttle conjugate composed of the cyclic RGD, a α(v)β(3) integrin-ligand, ligated to the cytotoxic drug TMZ. The ligation was carried out by the Diels Alder Reaction with inverse electron demand (DAR(inv)).

Published
2010

34. Enhancement of Radiation Response in Osteosarcoma and Rhabomyosarcoma Cell Lines by Histone Deacetylase Inhibition

Author

Olaf Witt, Susanne Oertel, Jürgen Debus, Marc Bischof, Volker Ehemann, Klaus J. Weber, Andreas E. Kulozik, Claudia Blattmann, Peter E. Huber, Hedwig E. Deubzer, and Markus Thiemann

Subjects
Radiation-Sensitizing Agents, Cancer Research, DNA Repair, Cell Survival, Somatic cell, DNA repair, Apoptosis, Hydroxamic Acids, Radiation Tolerance, Flow cytometry, Cell Line, Tumor, Rhabdomyosarcoma, medicine, Humans, Radiology, Nuclear Medicine and imaging, Ku Autoantigen, Vorinostat, Tumor Stem Cell Assay, Osteosarcoma, Photons, Radiation, medicine.diagnostic_test, Cell growth, business.industry, Valproic Acid, Cell Cycle, Antigens, Nuclear, Cell cycle, Flow Cytometry, medicine.disease, DNA-Binding Proteins, Histone Deacetylase Inhibitors, Oncology, Cancer research, Carrier Proteins, business, medicine.drug
Abstract

Purpose Histone deacetylase inhibitors (HDACIs) can enhance the sensitivity of cells to photon radiation treatment (XRT) by altering numerous molecular pathways. We investigated the effect of pan-HDACIs such as suberoylanilide hydroxamic acid (SAHA) on radiation response in two osteosarcoma (OS) and two rhabdomyosarcoma (RMS) cell lines. Methods and Materials Clonogenic survival, cell cycle analysis, and apoptosis were examined in OS (KHOS-24OS, SAOS2) and RMS (A-204, RD) cell lines treated with HDACI and HDACI plus XRT, respectively. Protein expression was investigated via immunoblot analysis, and cell cycle analysis and measurement of apoptosis were performed using flow cytometry. Results SAHA induced an inhibition of cell proliferation and clonogenic survival in OS and RMS cell lines and led to a significant radiosensitization of all tumor cell lines. Other HDACI such as M344 and valproate showed similar effects as investigated in one OS cell line. Furthermore, SAHA significantly increased radiation-induced apoptosis in the OS cell lines, whereas in the RMS cell lines radiation-induced apoptosis was insignificant with and without SAHA. In all investigated sarcoma cell lines, SAHA attenuated radiation-induced DNA repair protein expression (Rad51, Ku80). Conclusion Our results show that HDACIs enhance radiation action in OS and RMS cell lines. Inhibition of DNA repair, as well as increased apoptosis induction after exposure to HDACIs, can be mechanisms of radiosensitization by HDACIs.

Published
2010

35. Analysis of signaling pathways related to cell proliferation stimulated by insulin analogs in human mammary epithelial cell lines

Author

Harald Enzmann, Ashish Shukla, Jean Grisouard, Alexander Hermani, Doris Mayer, and Volker Ehemann

Subjects
Cancer Research, medicine.medical_specialty, MAP Kinase Signaling System, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Immunoblotting, Breast Neoplasms, Receptor, IGF Type 1, Phosphatidylinositol 3-Kinases, Endocrinology, Insulin receptor substrate, Internal medicine, Tumor Cells, Cultured, medicine, Animals, Humans, Insulin, RNA, Messenger, Enzyme Inhibitors, Phosphorylation, RNA, Small Interfering, Mammary Glands, Human, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Proliferation, biology, Reverse Transcriptase Polymerase Chain Reaction, Receptor, Insulin, IRS2, Cell biology, Insulin receptor, Oncology, biology.protein, Regular insulin, Cattle, Female, Signal transduction, Proto-Oncogene Proteins c-akt, Signal Transduction
Abstract

Insulin and insulin analogs stimulate proliferation of human mammary epithelial cells. We identified and analyzed the signaling pathways related to cell proliferation induced by regular insulin and by four insulin analogs presently approved for therapeutical use. Benign and malignant mammary cell lines showing different insulin receptor (IR) and IGF-I receptor (IGF-IR) expression patterns were studied. Cell proliferation was studied by crystal violet staining (BrdU-FACS analysis). Activation of insulin and IGF signaling pathways was studied by analysis of the phosphorylation status of IGF-IR and of key signaling proteins of the phosphoinositide 3-kinase (PI3K)/Akt and MAP kinase pathways, by the use of specific PI3K and MAP kinase inhibitors, and by silencing of IR and IGF-IR. Lantus stimulated the growth of MCF7 cells, which show high IGF-IR/IR ratio, significantly at 0.3 nmol/l, while regular insulin (Actrapid and bovine insulin) and other insulin analogs (Novorapid, Humalog, and Levemir) stimulated cell growth at 1.5–15 nmol/l concentrations. No difference between Lantus and the other insulin analogs was observed regarding growth stimulation of MCF10A cells showing low IGF-IR/IR ratio. Growth stimulation of MCF7 cells by Lantus was mainly due to strong activation of the IGF-IR and the MAP kinase pathway. Regular insulin and other insulin analogs tested activated mainly the IR and the PI3K/Akt pathway. We conclude that unlike regular insulin and other insulin analogs, Lantus strongly activates the IGF-IR and the MAP kinase pathway in MCF7 cells and is a strong mitogen for cells characterized by a high-IGF-IR/IR ratio.

Published
2009

36. High-Resolution Flow Cytometry: a Suitable Tool for Monitoring Aneuploid Prostate Cancer Cells after TMZ and TMZ-BioShuttle Treatment

Author

Klaus Braun, Volker Ehemann, Manfred Wiessler, Ruediger Pipkorn, Bernd Didinger, Gabriele Mueller, Waldemar Waldeck

Subjects
lcsh:R, lcsh:Medicine
Abstract

If metastatic prostate cancer gets resistant to antiandrogen therapy, there are few treatment options, because prostate cancer is not very sensitive to cytostatic agents. Temozolomide (TMZ) as an orally applicable chemotherapeutic substance has been proven to be effective and well tolerated with occasional moderate toxicity especially for brain tumors and an application to prostate cancer cells seemed to be promising. Unfortunately, TMZ was inefficient in the treatment of symptomatic progressive hormone-refractory prostate cancer (HRPC). The reasons could be a low sensitivity against TMZ the short plasma half-life of TMZ, non-adapted application regimens and additionally, the aneuploid DNA content of prostate cancer cells suggesting different sensitivity against therapeutical interventions e.g. radiation therapy or chemotherapy. Considerations to improve this unsatisfying situation resulted in the realization of higher local TMZ concentrations, sufficient to kill cells regardless of intrinsic cellular sensitivity and cell DNA-index. Therefore, we reformulated the TMZ by ligation to a peptide-based carrier system called TMZ-BioShuttle for intervention. The modular-composed carrier consists of a transmembrane transporter (CPP), connected to a nuclear localization sequence (NLS) cleavably-bound, which in turn was coupled with TMZ. The NLS-sequence allows an active delivery of the TMZ into the cell nucleus after transmembrane passage of the TMZ-BioShuttle and intra-cytoplasm enzymatic cleavage and separation from the CPP. This TMZ-BioShuttle could contribute to improve therapeutic options exemplified by the hormone refractory prostate cancer. The next step was to syllogize a qualified method monitoring cell toxic effects in a high sensitivity under consideration of the ploidy status. The high-resolution flow cytometric analysis showed to be an appropriate system for a better detection and distinction of several cell populations dependent on their different DNA-indices as well as changes in proliferation of cell populations after chemotherapeutical treatment.

Published
2009

37. TMZ-BioShuttle – a reformulated Temozolomide

Author

Waldemar Waldeck, Manfred Wiessler, Volker Ehemann, Ruediger Pipkorn, Herbert Spring, Juergen Debus, Bernd Didinger, Gabriele Mueller, Joerg Langowski, Klaus Braun

Subjects
lcsh:R, lcsh:Medicine
Abstract

There is a large number of effective cytotoxic drugs whose side effect profile, efficacy, and long-term use in man are well understood and documented over decades of use in clinical routine e.g. in the treatment of recurrent glioblastoma multiforme (GBM) and the hormone-refractory prostate cancer (HRPC). Both cancers are insensitive against most chemotherapeutic interventions; they have low response rates and poor prognoses. Some cytotoxic agents can be significantly improved by using modern technology of drug delivery or formulation. We succeeded to enhance the pharmacologic potency with simultaneous reduction of unwanted adverse reactions of the highly efficient chemotherapeutic temozolomide (TMZ) as an example. The TMZ connection to transporter molecules (TMZ-BioShuttle) resulted in a much higher pharmacological effect in glioma cell lines while using reduced doses. This permits the conclusion that a suitable chemistry could realize the ligation of pharmacologically active, but sensitive and highly unstable pharmaceutical ingredients without functional deprivation. The re-formulation of TMZ to TMZ-BioShuttle achieved a nearly 10-fold potential of the established pharmaceutic TMZ far beyond the treatment of brain tumors cells and results in an attractive reformulated drug with enhanced therapeutic index.

Published
2008

38. TMZ-BioShuttle – a reformulated Temozolomide

Author

Herbert Spring, Juergen Debus, Volker Ehemann, Waldemar Waldeck, Gabriele Mueller, Ruediger Pipkorn, Bernd Didinger, Joerg Langowski, Manfred Wiessler, and Klaus Braun

Subjects
Male, Drug, Side effect, Carrier Molecules, Chemistry, Pharmaceutical, media_common.quotation_subject, Dacarbazine, Nuclear Localization Signals, DNA Fragmentation, Pharmacology, Prostate cancer, Therapeutic index, Cell Line, Tumor, Temozolomide, Tumor Cells, Cultured, Humans, Medicine, BioShuttle, Antineoplastic Agents, Alkylating, Cell Proliferation, media_common, Drug Carriers, Glioblastoma multiforme (GBM), Dose-Response Relationship, Drug, business.industry, Cell Cycle, Prostatic Neoplasms, General Medicine, facilitated Transport, medicine.disease, Peptide Fragments, Temozolomide (TMZ), Reformulation, Drug delivery, Cancer research, Comet Assay, Carrier Proteins, Glioblastoma, Drug Delivery, business, Drug carrier, Research Paper, medicine.drug
Abstract

There is a large number of effective cytotoxic drugs whose side effect profile, efficacy, and long-term use in man are well understood and documented over decades of use in clinical routine e.g. in the treatment of recurrent glioblastoma multiforme (GBM) and the hormone-refractory prostate cancer (HRPC). Both cancers are insensitive against most chemotherapeutic interventions; they have low response rates and poor prognoses. Some cytotoxic agents can be significantly improved by using modern technology of drug delivery or formulation. We succeeded to enhance the pharmacologic potency with simultaneous reduction of unwanted adverse reactions of the highly efficient chemotherapeutic temozolomide (TMZ) as an example. The TMZ connection to transporter molecules (TMZ-BioShuttle) resulted in a much higher pharmacological effect in glioma cell lines while using reduced doses. This permits the conclusion that a suitable chemistry could realize the ligation of pharmacologically active, but sensitive and highly unstable pharmaceutical ingredients without functional deprivation. The re-formulation of TMZ to TMZ-BioShuttle achieved a nearly 10-fold potential of the established pharmaceutic TMZ far beyond the treatment of brain tumors cells and results in an attractive reformulated drug with enhanced therapeutic index.

Published
2008

39. Suppression of polyploidy by the BRCA2 protein

Author

W. Hofmann, Siegfried Scherneck, Manfred Schwab, Katrin Arnold, Volker Ehemann, Andreas Claas, Evgeny Sagulenko, Vitaliya Sagulenko, and Larissa Savelyeva

Subjects
Cyclin-Dependent Kinase Inhibitor p21, Cancer Research, Cell cycle checkpoint, endocrine system diseases, Genome integrity, Aurora B kinase, Breast Neoplasms, Protein Serine-Threonine Kinases, Biology, Retinoblastoma Protein, Polyploidy, Breast cancer, Aurora Kinases, medicine, Aurora Kinase B, Humans, skin and connective tissue diseases, neoplasms, Alleles, In Situ Hybridization, Fluorescence, BRCA2 Protein, Cell Nucleus, Nucleotides, Cell Cycle, medicine.disease, female genital diseases and pregnancy complications, Cell biology, Gene Expression Regulation, Neoplastic, Oncology, Cancer research, Breast cancer cells, biological phenomena, cell phenomena, and immunity, Apoptosis Regulatory Proteins, E2F1 Transcription Factor, Intracellular
Abstract

Mounting evidence implicates BRCA2 not only in maintenance of genome integrity but also in cell-cycle checkpoints. However, the contribution of BRCA2 in the checkpoints is still far from being understood. Here, we demonstrate that breast cancer cells MX-1 are unable to maintain genome integrity, which results in gross polyploidization. We generated MX-1 clones, stably expressing BRCA2, and found that BRCA2 acts to suppress polyploidy. Compared with MX-1, the ectopically BRCA2-expressing cells had different intracellular levels of Aurora A, Aurora B, p21, E2F-1, and pRb, suggesting a BRCA2-mediated suppression of polyploidy via stabilization of the checkpoint proteins levels.

Published
2007

40. Protumorigenic overexpression of stathmin/Op18 by gain-of-function mutation in p53 in human hepatocarcinogenesis

Author

A Brauckhoff, Sebastian Vreden, Martina Keith, Volker Ehemann, Stephan Singer, Peter Schirmacher, and Kai Breuhahn

Subjects
Small interfering RNA, Carcinoma, Hepatocellular, Cell Survival, Stathmin, macromolecular substances, medicine.disease_cause, Cell Movement, Cell Line, Tumor, medicine, Humans, RNA, Small Interfering, Cell Proliferation, Cisplatin, Mutation, Hepatology, biology, Liver Neoplasms, HCCS, Cell Transformation, Neoplastic, Apoptosis, Tumor progression, Cell culture, Cancer research, biology.protein, Tumor Suppressor Protein p53, medicine.drug
Abstract

The microtubule (MT)-destabilizing protein stathmin/Op18 has previously been described to be negatively regulated by p53 and to be highly expressed in several tumor entities. However, little is known about its expression profile, functional or therapeutic relevance, and regulation in human hepatocarcinogenesis. Here we demonstrate cytoplasmic overexpression of stathmin in premalignant lesions (dysplastic nodules; DNs) and hepatocellular carcinomas (HCCs), which significantly correlated with tumor progression, proliferation, and activation of other protumorigenic factors (e.g., nuclear p53). Inhibition of stathmin expression by gene-specific short interfering RNA (siRNA) was associated with a significant reduction of MT-dependent cellular functions such as tumor cell viability, proliferation, migration, and increased apoptosis in HCC cells. Loss of stathmin expression increased responsiveness of tumor cells to the treatment with cytostatic drugs targeting MT-stability (paclitaxel, vinblastine) and to DNA cross-linking agents (cisplatin). Surprisingly, inducible expression of p53wt in p53-negative HCC cells as well as a reduction of p53wt by siRNA in p53wt-positive cells did not alter stathmin expression. However, stathmin was down-regulated after siRNA-based reduction of p53mut/Y220C and p53mut/R213Q expression in different tumor cell types. Conclusion: Our results demonstrate that overexpression of stathmin is an early protumorigenic event in human hepatocarcinogenesis, and its up-regulation can be mediated by gain-of-function mutations in p53. Thus, stathmin represents a potential therapeutic target, for example, by increasing responsiveness of tumor cells to treatment with chemotherapeutic agents after reduction of stathmin bioactivity. (HEPATOLOGY 2007.)

Published
2007

41. High Skp2 Expression Characterizes High-Risk Neuroblastomas Independent of MYCN Status

Author

Kai Oliver Henrich, Matthias Fischer, Werner Lutz, Javed Khan, Jun S. Wei, Axel Benner, Ivo Leuschner, Benedikt Brors, Karen Ernestus, Volker Ehemann, Rainer König, Ruprecht Wiedemeyer, Frank Westermann, and Manfred Schwab

Subjects
Risk, Cancer Research, Candidate gene, Gene Expression Profiling, Genes, myc, Biology, medicine.disease, Immunohistochemistry, Gene expression profiling, Neuroblastoma, Real-time polymerase chain reaction, Oncology, Gene expression, SKP2, medicine, Cancer research, Humans, RNA, Messenger, S-Phase Kinase-Associated Proteins, neoplasms, Gene, E2F1 Transcription Factor, Oligonucleotide Array Sequence Analysis
Abstract

Purpose: Amplified MYCN oncogene defines a subgroup of neuroblastomas with poor outcome. However, a substantial number of MYCN single-copy neuroblastomas exhibits an aggressive phenotype similar to that of MYCN-amplified neuroblastomas even in the absence of high MYCN mRNA and/or protein levels. Experimental Design: To identify shared molecular mechanisms that mediate the aggressive phenotype in MYCN-amplified and single-copy high-risk neuroblastomas, we defined genetic programs evoked by ectopically expressed MYCN in vitro and analyzed them in high-risk versus low-risk neuroblastoma tumors (n = 49) using cDNA microarrays. Candidate gene expression was validated in a separate cohort of 117 patients using quantitative PCR, and protein expression was analyzed in neuroblastoma tumors by immunoblotting and immunohistochemistry. Results: We identified a genetic signature characterized by a subset of MYCN/MYC and E2F targets, including Skp2, encoding the F-box protein of the SCFSkp2 E3-ligase, to be highly expressed in high-risk neuroblastomas independent of amplified MYCN. We validated the findings for Skp2 and analyzed its expression in relation to MYCN and E2F-1 expression in a separate cohort (n = 117) using quantitative PCR. High Skp2 expression proved to be a highly significant marker of dire prognosis independent of both MYCN status and disease stage, on the basis of multivariate analysis of event-free survival (hazard ratio, 3.54; 95% confidence interval, 1.56-8.00; P = 0.002). Skp2 protein expression was inversely correlated with expression of p27, the primary target of the SCFSkp2 E3-ligase, in neuroblastoma tumors. Conclusion: Skp2 may have a key role in the progression of neuroblastomas and should make an attractive target for therapeutic approaches.

Published
2007

42. Non-specific effects of siRNAs on tumor cells with implications on therapeutic applicability using RNA interference

Author

Tanja Nussbaum, Darjus F. Tschaharganeh, Kai Breuhahn, Volker Ehemann, and Peter Schirmacher

Subjects
Cancer Research, Small interfering RNA, Carcinoma, Hepatocellular, Cell Survival, Apoptosis, Biology, Transfection, Cell Line, Pathology and Forensic Medicine, Cell Movement, RNA interference, Interferon, Cell Line, Tumor, medicine, Humans, Gene silencing, Viability assay, RNA, Small Interfering, Cell Proliferation, Cell Cycle, Liver Neoplasms, General Medicine, Cell cycle, Cell biology, Gene Expression Regulation, Neoplastic, RNA silencing, Oncology, RNA Interference, Interferons, medicine.drug
Abstract

Elimination of protein expression using RNA interference (RNAi) significantly improves the understanding of gene function and represents a promising technique for the treatment of diseases such as cancer and neurological disorders. Accumulating evidence suggests the so-called interferon-independent non-specific gene silencing of short interfering RNA (siRNA); however, its biological and functional cellular consequences are largely unidentified. We therefore analyzed the effects of different nonsense siRNAs on characteristic bio-parameters such as cell viability, proliferation, cell cycle distribution, apoptosis, and migration of tumor cells. All analyzed cellular aspects have been observed to be significantly affected by the presence of siRNA in an interferon-independent manner: viability, mitosis, and motility were significantly diminished and programmed cell death was significantly elevated. Moreover, all cell cycle stages (G0/G1-, G2/M-, and S-phase) were moderately shifted. Together, these results support the hypothesis that siRNA, due to sequence-specific cellular consequences, modulate bio-functionality independent of the target sequence. This phenomenon affects the design of siRNA experiments for future in vitro but also for in vivo tests as well as for potential therapeutic and preventive strategies. Moreover, monitoring interferon response after transfection of siRNAs is necessary but not sufficient to exclude potential off-target effects in non-diseased cells.

Published
2007

43. BioShuttle-mediated Plasmid Transfer

Author

Klaus Braun, Leonie von Brasch, Ruediger Pipkorn, Volker Ehemann, Juergen Jenne, Herbert Spring, Juergen Debus, Bernd Didinger, Werner Rittgen, Waldemar Waldeck

Subjects
lcsh:R, lcsh:Medicine
Abstract

An efficient gene transfer into target tissues and cells is needed for safe and effective treatment of genetic diseases like cancer. In this paper, we describe the development of a transport system and show its ability for transporting plasmids. This non-viral peptide-based BioShuttle-mediated transfer system consists of a nuclear localization address sequence realizing the delivery of the plasmid phNIS-IRES-EGFP coding for two independent reporter genes into nuclei of HeLa cells. The quantification of the transfer efficiency was achieved by measurements of the sodium iodide symporter activity. EGFP gene expression was measured with Confocal Laser Scanning Microscopy and quantified with biostatistical methods by analysis of the frequency of the amplitude distribution in the CLSM images. The results demonstrate that the “BioShuttle”-Technology is an appropriate tool for an effective transfer of genetic material carried by a plasmid.

Published
2007

44. Differential effects of CLDR and PDR brachytherapy on cell cycle progression in a syngeneic rat prostate tumour model

Author

Ivan Zuna, Klaus J. Weber, Jürgen Debus, Volker Ehemann, Peter Peschke, and Wolfgang Harms

Subjects
Male, Radiological and Ultrasound Technology, business.industry, medicine.medical_treatment, Brachytherapy, Cell Cycle, Cell cycle progression, Prostatic Neoplasms, Radiotherapy Dosage, Cell cycle, Low-Dose Rate Brachytherapy, Rats, Rat Prostate, medicine.anatomical_structure, Prostate, Radioresistance, medicine, Animals, Radiology, Nuclear Medicine and imaging, Pulsed-Dose Rate Brachytherapy, Nuclear medicine, business
Abstract

The study consisted of two treatment arms comparing the effects of CLDR (continuous low dose rate) and PDR (pulsed dose rate) brachytherapy on cell cycle progression in a radioresistant rat prostate tumour model.Interstitial PDR and CLDR brachytherapy (both 192-Ir, 0.75 Gy/h) were administered to Dunning prostate R3327-AT1 carcinomas transplanted subcutaneously into the thigh of Copenhagen rats. Increasing doses of up to 20 as well as up to 40 Gy were applied. Cell cycle distributions of the aneuploid tumour cell subpopulations were determined at 4 h (3 Gy), 24 h (18 Gy), 48 h (20 and 36 Gy), as well as during the subsequent redistribution period (20 and 40 Gy) at 72, 96, and 120 h. Tumours either implemented with an empty tubing system (n=5) or under undisturbed growth (n=5) served as controls. Three animals were irradiated per time point and exposure condition. At least two flow cytometrical analyses were carried out per animal.The aneuploid cells possessed a constant DNA-Index of 1.9+/-0.06. In contrast to sham-treated controls, the aneuploid cell fraction with G2/M DNA content was significantly increased (p0.05) after initiation of both, CLDR and PDR brachytherapy. However, CLDR resulted in an earlier accumulation of tumour cells in G2/M (24 h: 28% CLDR vs. 19% PDR, p0.05) with a concomitant reduction of cells in G1, whereas PDR yielded delayed, but then more pronounced cell cycle changes, particularly expressed during the redistribution period after both 20 and 40 Gy.CLDR and PDR brachytherapy showed differential effects on cell cycle progression. The induction of a significantly earlier but also less persistent G2/M cell cycle arrest after CLDR compared to PDR brachytherapy implies that a substantially higher fraction of tumour cells are irradiated in G2/M after CLDR.

Published
2006

45. Effects of Local Application of Growth and Differentiation Factor-5 (GDF-5) in a Full-thickness Cartilage Defect Model

Author

Wiltrud Richter, Martin Jung, Rainer Ries, Christoph Lill, Consolato Sergi, Stefanie Adolf, Hans-Georg Simank, Christina Eckhardt, and Volker Ehemann

Subjects
Cartilage, Articular, Pathology, medicine.medical_specialty, Bone Regeneration, Time Factors, Clinical Biochemistry, Biocompatible Materials, Matrix (biology), Collagen Type I, Fetus, Endocrinology, Growth Differentiation Factor 5, medicine, Animals, Bone regeneration, Cells, Cultured, Osteoblasts, Chemistry, Cartilage, Regeneration (biology), Skull, Histology, Cell Biology, Anatomy, Flow Cytometry, Recombinant Proteins, Extracellular Matrix, Rats, Disease Models, Animal, medicine.anatomical_structure, Bone Morphogenetic Proteins, embryonic structures, Fibrocartilage, Female, Full thickness, Rabbits, Tomography, X-Ray Computed
Abstract

Our purpose in this study was to investigate the effects of growth and differentiation factor-5 (GDF-5) on cartilage and subchondral bone in a rabbit model harboring an osteochondral defect for a period of 6 months. Absorbable composites were implanted in adult rabbits (18 controls, 18 animals with collagen-I matrix, and 18 animals with matrix plus GDF-5). After 4, 8, or 24 weeks the specimens were studied by histology, microcomputed tomography (microCT) and flow-cytometric analysis (FACS). Implantation of GDF-5 resulted in an improved histological appearance. This was the result of significantly improved defect filling at 4 and 8 weeks. At 24 weeks, however, there was no difference between the groups. The histological examination disclosed a predominance of fibrocartilage, and remodeled subchondral bone was also observed. MicroCT documented normal bone density in all groups, excluding subchondral sclerosis. At 24 weeks, FACS analysis revealed high apoptotic activity in the GDF-5-treated group. As far as we are aware, this is the first report of the effects of GDF-5 in a full-thickness cartilage defect model. We assume that recombinant GDF-5 contained on the carrier is probably able to accelerate the regeneration of the osteochondral defect owing to its availability. However, control of the protein delivery may require further investigation.

Published
2004

46. Centrosomal aberrations in primary invasive breast cancer are associated with nodal status and hormone receptor expression

Author

Ulf Krause, Anthony D. Ho, Andreas Schneeweiss, Hans-Peter Sinn, Kai Neben, Tanja Khbeis, Volker Ehemann, Alwin Krämer, and Gunther Bastert

Subjects
Cancer Research, Pathology, medicine.medical_specialty, Proliferation index, Mammary gland, Aneuploidy, Biology, medicine.disease, Metastasis, medicine.anatomical_structure, Breast cancer, Oncology, medicine, Carcinoma, Immunohistochemistry, Lymph node
Abstract

Our purpose was to assess the presence of centrosomal aberrations as measured by immunohistochemistry in primary invasive breast cancer and their association with established and proposed prognostic factors. Tissue sections of 103 primary invasive breast cancers were examined using centrosome-specific antibodies to pericentrin and gamma-tubulin. At least 3 different tumor regions per case were examined to determine maximum centrosomal aberration levels, which represent the proportion of cells with abnormal centrosomes in the region with the highest percentage of cells with centrosomal aberrations. The chi(2) test was performed to evaluate the association of maximum centrosomal aberration levels with patient age; tumor size; nodal status; nuclear grade; hormone receptor and Her2/neu expression; proportion of Ki67-, p53- and Bcl-2-positive tumor cells; DNA index; S-phase fraction; and proliferation index. With pericentrin immunohistochemistry, maximum centrosomal aberration levels >35% were detectable in 92 of the 103 breast carcinomas (89%). We found a highly significant correlation of maximum centrosomal aberration levels above 35% with axillary nodal tumor involvement (p 35% were also associated with an increased DNA index (p = 0.006). In a subset of patients, additional staining of centrosomes with a monoclonal anti-gamma-tubulin antibody essentially confirmed these results. In primary invasive breast cancer, centrosomal aberrations are associated with those factors predicting a more aggressive course of disease. This might indicate a fundamental role of centrosomal dysfunction in disease evolution, possibly as a result of chromosome missegregation during mitosis.

Published
2003

47. The enhancement of neutron irradiation of HeLa-S cervix carcinoma cells by cell–nucleus-addressed deca-p-boronophenylalanine

Author

Waldemar Waldeck, Andreas Eisenmenger, Gerd Wolber, Klaus Braun, Isabell Braun, Ralf Rastert, Joürgen Debus, Stefan Heckl, Rüdiger Pipkorn, Jürgen Jenne, Heike Corban-Wilhelm, and Volker Ehemann

Subjects
Boron Compounds, inorganic chemicals, Radiation-Sensitizing Agents, Cell Survival, Phenylalanine, medicine.medical_treatment, Molecular Sequence Data, Active Transport, Cell Nucleus, Uterine Cervical Neoplasms, Linear energy transfer, chemistry.chemical_element, Boron Neutron Capture Therapy, Mass Spectrometry, HeLa, Drug Discovery, medicine, Humans, Amino Acid Sequence, Boron, Cell Nucleus, Pharmacology, Microscopy, Confocal, biology, Carcinoma, Organic Chemistry, Radiochemistry, technology, industry, and agriculture, General Medicine, Flow Cytometry, biology.organism_classification, Neutron temperature, Radiation therapy, Neutron capture, Cell killing, chemistry, Cell culture, Female, HeLa Cells
Abstract

Boron neutron capture therapy (BNCT) is an experimental treatment modality which depends on a sufficient cellular uptake of Boron ((10)B) followed by an exposure to a thermal neutron beam from a nuclear reactor. High energetic particles (4He and 7Li) are created during the neutron capture reaction and produce DNA damages, which lead to cell killing. Regarding BNCT, the short radiation range of He- and Li-particles is decisive for the distribution of (10)B. Until now, BNCT has been lacking for therapeutically effective concentrations of (10)B. Twenty-four hours after the combined use of our 'Bioshuttle'-p-borono-phenylalanine(10)-constructs ('Bioshuttle'-p-BPA(10)) and neutron-irradiation, an obvious reduction of the radiation-resistant HeLa-S cells could be observed. No cells were alive 72 h after the incubation with 'Bioshuttle'-p-BPA(10) followed by neutron irradiation. A post-mitotic cell death could be assumed based on flow cytometrical data.

Published
2003

48. Flow cytometric detection of spontaneous apoptosis in human breast cancer using the TUNEL-technique

Author

Herwart F. Otto, Volker Ehemann, Adelheid Lange, Jaromir Sykora, and Jorge Vera-Delgado

Subjects
Cell Nucleus, Cancer Research, TUNEL assay, medicine.diagnostic_test, Apoptotic DNA fragmentation, Apoptosis, Breast Neoplasms, DNA, DNA Fragmentation, Biology, Cell cycle, Flow Cytometry, Molecular biology, Cell cycle phase, Flow cytometry, Oncology, Terminal deoxynucleotidyl transferase, In Situ Nick-End Labeling, medicine, Humans, DNA fragmentation, Lymphocytes, Cytometry, Cell Division
Abstract

Microscopic detection of structural alterations is the most reliable method to identify apoptotic cells, which however, does not allow any correlation with cell cycle phases. Discrimination of individual cells within solid human tumors undergoing apoptotic death is possible by flow cytometry where apoptotic cells appear in a hypodiploid sub G0/1-peak as a consequence of partial DNA loss. To refer induction of apoptosis to cell cycle phases we adopted the terminal deoxynucleotidyl transferase nick-end-labelling (TUNEL) technique to flow cytometry which enables the detection of cellular DNA content and DNA fragmentation by multiparametric analysis. One thousand seven hundred human breast carcinomas were screened. In 40 cases (2.3%) of 1700 carcinomas we detected a hypodiploid sub -G0/1 apoptotic peak. The spontaneous apoptotic fractions within individual tumors ranged between 1.5 and 25%. A correlation (r(2)=0.78) was found between apoptotic cells in sub-G0/1-peak measured by DNA-cytometry and TUNEL positive cells measured by multiparametric cytometry, because TUNEL reaction signed also cells with strand breaks. High proliferation indices correspond well (r(2)=0.807) with the increased amount of TUNEL positive cells. Multiparametric flow cytometry for the combined determination of DNA-content and DNA-fragmentation by TUNEL offers not only the advantage of a higher apoptosis sensitivity but also enables the quantification of DNA fragmentation related to any cell cycle phase.

Published
2003

49. Preferential radiosensitization in p53-mutated human tumour cell lines by pentoxifylline-mediated disruption of the G2/M checkpoint control

Author

Jürgen Debus, Volker Ehemann, W Waldeck, Peter Peschke, A M Strunz, and M Kissel

Subjects
G2 Phase, Time Factors, Cell Survival, Mitosis, Radiation-Protective Agents, Biology, Radiation Tolerance, Pentoxifylline, Flow cytometry, G2/M checkpoint, P53 status, Tumor Cells, Cultured, medicine, Humans, Radiology, Nuclear Medicine and imaging, Irradiation, Cell survival, Radiological and Ultrasound Technology, medicine.diagnostic_test, Cell Cycle, Dose-Response Relationship, Radiation, Flow Cytometry, Kinetics, Dose–response relationship, Cell culture, Immunology, Cancer research, Tumor Suppressor Protein p53, medicine.drug
Abstract

There is evidence that the duration of the G2/M delay following irradiation is correlated with cell survival. We studied the radiosensitizing potential of pentoxifylline (PTX) and the PTX-mediated modulation of cell-cycle progression dependent on the p53 status of various human tumour cell lines.The cellular radiosensitivity of human MCF-7 (wild-type p53) and HT-29 (p53-defective) tumour cells, which were exposed to PTX (2 mM) immediately after gamma-irradiation was determined by colony forming assay. The influence on cell cycle progression after irradiation (6 Gy) was assessed by flow cytometric analysis using p53 wild-type MCF-7 and HPR600 cells, and p53-defective HT-29 and WiDr cells.Clonogenic survival assays up to 8 Gy demonstrated that p53-defective HT-29 cells (sensitizer enhancement ratio [SER]=1.54) were sensitized by PTX (2 mM) to a significantly higher degree than p53 wild-type MCF-7 (SER=1.14) cells. Exposure of irradiated (6 Gy) cells to PTX (2 mM) resulted in abrogation of the radiation-induced G2/M arrest in the p53-defective HT-29 and WiDr cells, whereas the p53 wild-type-expressing MCF-7 and HPR600 cells showed less significant impairment of the G2/M checkpoint. In HT-29 cells, the rate of transition into mitosis was even higher than in the sham-treated control cells. G2/M abrogation was accompanied by an increase of apoptosis only in HPR600 cells.Since PTX was less effective in cells expressing intact p53, the application of PTX suggests a promising strategy of pharmacological disruption of the G2/M checkpoint control by which preferentially radiation-resistant tumours with defective p53 function might be rendered more sensitive to ionizing radiation.

Published
2002

50. Decreased Apoptosis Despite Severe CD4 Depletion in the Thymus of a Human Immunodeficiency Virus-1 Infected Child

Author

T. Boehler, Shelina Kassam, Volker Ehemann, Herwart F. Otto, Consolato Sergi, and Jürgen Brunner

Subjects
CD4-Positive T-Lymphocytes, Male, T cell, Human immunodeficiency virus (HIV), Apoptosis, HIV Infections, Thymus Gland, CD8-Positive T-Lymphocytes, Biology, medicine.disease_cause, In Situ Nick-End Labeling, medicine, Humans, Perivascular space, Child, TUNEL assay, Cell growth, Molecular biology, CD4 Lymphocyte Count, medicine.anatomical_structure, Pediatrics, Perinatology and Child Health, Immunology, HIV-1, Immunohistochemistry, CD8
Abstract

Thymic epithelial space (TES), where thymopoiesis is located, and thymic perivascular space (PVS), where T lymphocytes are pooled, appear differentially involved in human immunodeficiency virus 1 (HIV-1)-infected children. The decline of CD4+ T cells during HIV-1 infection is probably due to a relative predominance of CD4+ T cell destruction on cell proliferation. Antiretroviral therapy (ART) typically increases circulating CD4+ T cell counts, but it is debated whether ART reduces the destruction of existing CD4+ T cells or enhances the production of new cells. We report on postmortem flow-cytometry, immunohistochemistry, and terminal deoxynucleotide transferase (TdT)-mediated dUTP nick-end labeling (TUNEL) studies performed on thymus of an 11-year-old vertically HIV-1 infected child receiving ART. Thymus tissue sections showed that CD4+ and CD8+ cells were more numerous in PVS than in TES (p=0.0334 for CD4+ cells, p

Published
2011

Catalog

Books, media, physical & digital resources
See catalog results