Your search keyword '"Karin Schmelz"' showing total 28 results

1. X‐linked inhibitor of apoptosis protein represents a promising therapeutic target for relapsed/refractory ALL

Author

Michela Carlet, Karin Schmelz, Jenny Vergalli, Tobias Herold, Daniela Senft, Vindi Jurinovic, Thomas Hoffmann, Jutta Proba, Nina Weichert, Christian Junghanß, Mareike Roth, Georg Eschenburg, Malwine Barz, Günter Henze, Cornelia Eckert, Angelika Eggert, Johannes Zuber, Patrick Hundsdoerfer, and Irmela Jeremias

Subjects

PDX, relapsed/refractory acute lymphoblastic leukemia, smac mimetics, therapeutic target, XIAP, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Acute lymphoblastic leukemia (ALL) represents the most frequent malignancy in children, and relapse/refractory (r/r) disease is difficult to treat, both in children and adults. In search for novel treatment options against r/r ALL, we studied inhibitor of apoptosis proteins (IAP) and Smac mimetics (SM). SM‐sensitized r/r ALL cells towards conventional chemotherapy, even upon resistance against SM alone. The combination of SM and chemotherapy‐induced cell death via caspases and PARP, but independent from cIAP‐1/2, RIPK1, TNFα or NF‐κB. Instead, XIAP was identified to mediate SM effects. Molecular manipulation of XIAP in vivo using microRNA‐30 flanked shRNA expression in cell lines and patient‐derived xenograft (PDX) models of r/r ALL mimicked SM effects and intermediate XIAP knockdown‐sensitized r/r ALL cells towards chemotherapy‐induced apoptosis. Interestingly, upon strong XIAP knockdown, PDX r/r ALL cells were outcompeted in vivo, even in the absence of chemotherapy. Our results indicate a yet unknown essential function of XIAP in r/r ALL and reveal XIAP as a promising therapeutic target for r/r ALL.

Published

2023

2. Spatial and temporal intratumour heterogeneity has potential consequences for single biopsy-based neuroblastoma treatment decisions

Author

Karin Schmelz, Joern Toedling, Matt Huska, Maja C. Cwikla, Louisa-Marie Kruetzfeldt, Jutta Proba, Peter F. Ambros, Inge M. Ambros, Sengül Boral, Marco Lodrini, Celine Y. Chen, Martin Burkert, Dennis Guergen, Annabell Szymansky, Kathy Astrahantseff, Annette Kuenkele, Kerstin Haase, Matthias Fischer, Hedwig E. Deubzer, Falk Hertwig, Patrick Hundsdoerfer, Anton G. Henssen, Roland F. Schwarz, Johannes H. Schulte, and Angelika Eggert

Subjects

Science

Abstract

Neuroblastoma is a devastating tumour in children. Here, the authors analyse multi-region patient samples using genomics and transcriptomics, revealing temporal and spatial heterogeneity and questioning the reliability of single-biopsy based diagnostics.

Published

2021

3. Parallel sequencing of extrachromosomal circular DNAs and transcriptomes in single cancer cells

Author

Rocío Chamorro González, Thomas Conrad, Maja C. Stöber, Robin Xu, Mădălina Giurgiu, Elias Rodriguez-Fos, Katharina Kasack, Lotte Brückner, Eric van Leen, Konstantin Helmsauer, Heathcliff Dorado Garcia, Maria E. Stefanova, King L. Hung, Yi Bei, Karin Schmelz, Marco Lodrini, Stefan Mundlos, Howard Y. Chang, Hedwig E. Deubzer, Sascha Sauer, Angelika Eggert, Johannes H. Schulte, Roland F. Schwarz, Kerstin Haase, Richard P. Koche, and Anton G. Henssen

Subjects

Cancer Research, Genetics, Technology Platforms

Abstract

Extrachromosomal DNAs (ecDNAs) are common in cancer, but many questions about their origin, structural dynamics and impact on intratumor heterogeneity are still unresolved. Here we describe single-cell extrachromosomal circular DNA and transcriptome sequencing (scEC&T-seq), a method for parallel sequencing of circular DNAs and full-length mRNA from single cells. By applying scEC&T-seq to cancer cells, we describe intercellular differences in ecDNA content while investigating their structural heterogeneity and transcriptional impact. Oncogene-containing ecDNAs were clonally present in cancer cells and drove intercellular oncogene expression differences. In contrast, other small circular DNAs were exclusive to individual cells, indicating differences in their selection and propagation. Intercellular differences in ecDNA structure pointed to circular recombination as a mechanism of ecDNA evolution. These results demonstrate scEC&T-seq as an approach to systematically characterize both small and large circular DNA in cancer cells, which will facilitate the analysis of these DNA elements in cancer and beyond.

Published

2023

4. X-linked inhibitor of apoptosis protein represents a promising therapeutic target for relapsed/refractory ALL

Author

Michela Carlet, Karin Schmelz, Jenny Vergalli, Tobias Herold, Daniela Senft, Vindi Jurinovic, Thomas Hoffmann, Jutta Proba, Nina Weichert, Christian Junghanß, Mareike Roth, Georg Eschenburg, Malwine Barz, Günter Henze, Cornelia Eckert, Angelika Eggert, Johannes Zuber, Patrick Hundsdoerfer, and Irmela Jeremias

Subjects

Molecular Medicine, Pdx, Relapsed/refractory Acute Lymphoblastic Leukemia, Smac Mimetics, Therapeutic Target, Xiap

Abstract

Acute lymphoblastic leukemia (ALL) represents the most frequent malignancy in children, and relapse/refractory (r/r) disease is difficult to treat, both in children and adults. In search for novel treatment options against r/r ALL, we studied inhibitor of apoptosis proteins (IAP) and Smac mimetics (SM). SM-sensitized r/r ALL cells towards conventional chemotherapy, even upon resistance against SM alone. The combination of SM and chemotherapy-induced cell death via caspases and PARP, but independent from cIAP-1/2, RIPK1, TNFα or NF-κB. Instead, XIAP was identified to mediate SM effects. Molecular manipulation of XIAP invivo using microRNA-30 flanked shRNA expression in cell lines and patient-derived xenograft (PDX) models of r/r ALL mimicked SM effects and intermediate XIAP knockdown-sensitized r/r ALL cells towards chemotherapy-induced apoptosis. Interestingly, upon strong XIAP knockdown, PDX r/r ALL cells were outcompeted invivo, even in the absence of chemotherapy. Our results indicate a yet unknown essential function of XIAP in r/r ALL and reveal XIAP as a promising therapeutic target for r/r ALL.

Published

2022

5. Multiplexed Quantification of Four Neuroblastoma DNA Targets in a Single Droplet Digital PCR Reaction

Author

Rasmus B. Linke, Karin Schmelz, Joern Toedling, Constantin Peitz, Angelika Eggert, Matthias Fischer, Clemens Messerschmidt, Maddalena Grimaldi, Hedwig E. Deubzer, Dieter Beule, Johannes H. Schulte, Marco Lodrini, Kathy Astrahantseff, Ulrich Keilholz, and Annika Sprüssel

Subjects

0301 basic medicine, DNA Copy Number Variations, Sensitivity and Specificity, Pathology and Forensic Medicine, Neuroblastoma, 03 medical and health sciences, chemistry.chemical_compound, Exon, 0302 clinical medicine, Cell Line, Tumor, Reference genes, Blood plasma, medicine, Humans, Anaplastic Lymphoma Kinase, Digital polymerase chain reaction, Liquid biopsy, Alleles, N-Myc Proto-Oncogene Protein, Liquid Biopsy, Reproducibility of Results, Exons, medicine.disease, Molecular biology, Data Accuracy, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Mutation, Molecular Medicine, Primer (molecular biology), Cell-Free Nucleic Acids, Multiplex Polymerase Chain Reaction, DNA

Abstract

The detection and characterization of cell-free DNA (cfDNA) in peripheral blood from neuroblastoma patients may serve as a minimally invasive approach to liquid biopsy. Major challenges in the analysis of cfDNA purified from blood samples are small sample volumes and low cfDNA concentrations. Droplet digital PCR (ddPCR) is a technology suitable for analyzing low levels of cfDNA. Reported here are two quadruplexed ddPCR assay protocols that reliably quantify MYCN and ALK copy numbers in a single reaction together with the two reference genes, NAGK and AFF3, and accurately estimate ALKF1174L (exon 23 position 3522, C>A) and ALKR1275Q (exon 25 position 3824, G>A) mutant allele fractions using cfDNA as input. The separation of positive and negative droplets was optimized for detecting two targets in each ddPCR fluorescence channel by the adjustment of the probe and primer concentrations of each target molecule. The quadruplexed assays were validated using a panel of 10 neuroblastoma cell lines and paired blood plasma and primary neuroblastoma samples from nine patients. Accuracy and sensitivity thresholds in quadruplexed assays corresponded well with those from the respective duplexed assays. Presented are two robust quadruplexed ddPCR protocols applicable in the routine clinical setting and that require only minimal plasma volumes for the assessment of MYCN and ALK oncogene status.

Published

2020

6. Extrachromosomal circular DNA drives oncogenic genome remodeling in neuroblastoma

Author

Eric Blanc, Annika Winkler, F Hertwig, Katharina Kasack, Joern Toedling, Filippos Klironomos, Victor Bardinet, Konstantin Helmsauer, Johannes H. Schulte, Anton G. Henssen, Patrick Hundsdörfer, Theresa M Thole, Natalie Timme, Ian C. MacArthur, Richard Koche, David Torrents, Elias Rodriguez-Fos, Nina Thiessen, Claudia Röefzaad, Montserrat Puiggròs, Hedwig E. Deubzer, Jessica Theissen, Karin Schmelz, Dieter Beule, Roland F. Schwarz, Carolina Rosswog, Steffen Fuchs, Rocio Chamorro, Annette Künkele, Angelika Eggert, Heathcliff Dorado Garcia, Sascha Sauer, Martin Burkert, Annabell Szymansky, Jesper L.V. Maag, Natalia Munoz-Perez, Matthias Fischer, and Yi Bei

Subjects

Carcinogenesis, Somatic cell, Extrachromosomal Inheritance, Biology, Extrachromosomal circular DNA, Genome, Article, Transcriptome, Neuroblastoma, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Extrachromosomal DNA, Tumor Cells, Cultured, Genetics, medicine, Humans, 030304 developmental biology, Gene Rearrangement, Recombination, Genetic, 0303 health sciences, Genome, Human, Oncogenes, Gene rearrangement, medicine.disease, chemistry, DNA, Circular, 030217 neurology & neurosurgery, DNA

Abstract

Extrachromosomal circularization of DNA is an important genomic feature in cancer. The structure, composition and genome-wide frequency of extrachromosomal circular DNA, however, have not yet been extensively profiled. Here, we combined genomic and transcriptomic approaches to describe the landscape of extrachromosomal circular DNA in neuroblastoma, a tumor arising in childhood from primitive cells of the sympathetic nervous system. Our analysis identifies and characterizes a wide catalog of somatically acquired and undescribed extrachromosomal circular DNAs. Moreover, we find that extrachromosomal circular DNAs are an unanticipated major source of somatic rearrangements, contributing to oncogenic remodeling through chimeric circularization and reintegration of circular DNA into the linear genome. Cancer-causing lesions can emerge out of circle-derived rearrangements and are associated with adverse clinical outcome. It is highly probable that circle-derived rearrangements represent an ongoing mutagenic process. Thus, extrachromosomal circular DNAs represent a multi-hit mutagenic process, with important functional and clinical implications for the origins of genomic remodeling in cancer.

Published

2019

7. Discovery of Spatial Peptide Signatures for Neuroblastoma Risk Assessment by MALDI Mass Spectrometry Imaging

Author

Oliver Klein, Senguel Boral, Angelika Eggert, Karin Schmelz, Kathy Astrahantseff, Patrick Hundsdoerfer, Johannes H. Schulte, and Zhiyang Wu

Subjects

chemistry.chemical_classification, Cancer Research, Multivariate statistics, Multivariate analysis, peptide signatures, Univariate, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, risk assessment, Peptide, intratumor heterogeneity, Computational biology, Biology, medicine.disease, Mass spectrometry imaging, Article, neuroblastoma, Oncology, chemistry, Tumor progression, Neuroblastoma, medicine, MALDI-MSI, Risk assessment, RC254-282

Abstract

Simple Summary The childhood tumor, neuroblastoma, has a broad clinical presentation. Risk assessment at diagnosis is particularly difficult in molecularly heterogeneous high-risk cases. Here we investigate the potential of imaging mass spectrometry to directly detect intratumor heterogeneity on the protein level in tissue sections. We show that this approach can produce discriminatory peptide signatures separating high- from low- and intermediate-risk tumors, identify 8 proteins aassociated with these signatures and validate two marker proteins using tissue immunostaining that have promise for further basic and translational research in neuroblastoma. We provide proof-of-concept that mass spectrometry-based technology could assist early risk assessment in neuroblastoma and provide insights into peptide signature-based detection of intratumor heterogeneity. Abstract Risk classification plays a crucial role in clinical management and therapy decisions in children with neuroblastoma. Risk assessment is currently based on patient criteria and molecular factors in single tumor biopsies at diagnosis. Growing evidence of extensive neuroblastoma intratumor heterogeneity drives the need for novel diagnostics to assess molecular profiles more comprehensively in spatial resolution to better predict risk for tumor progression and therapy resistance. We present a pilot study investigating the feasibility and potential of matrix-assisted laser desorption/ionization mass spectrometry imaging (MALDI-MSI) to identify spatial peptide heterogeneity in neuroblastoma tissues of divergent current risk classification: high versus low/intermediate risk. Univariate (receiver operating characteristic analysis) and multivariate (segmentation, principal component analysis) statistical strategies identified spatially discriminative risk-associated MALDI-based peptide signatures. The AHNAK nucleoprotein and collapsin response mediator protein 1 (CRMP1) were identified as proteins associated with these peptide signatures, and their differential expression in the neuroblastomas of divergent risk was immunohistochemically validated. This proof-of-concept study demonstrates that MALDI-MSI combined with univariate and multivariate analysis strategies can identify spatially discriminative risk-associated peptide signatures in neuroblastoma tissues. These results suggest a promising new analytical strategy improving risk classification and providing new biological insights into neuroblastoma intratumor heterogeneity.

Published

2021

8. Abstract 1693: Dissecting intercellular extrachromosomal circular DNA heterogeneity in single cancer cells with scEC&T-seq

Author

Rocio Chamorro Gonzalez, Thomas Conrad, Robin Xu, Madalina Giurgiu, Maja Cwikla, Katharina Kasack, Lotte Brückner, Eric van Leen, Elias Rodriguez-Fos, Konstantin Helmsauer, Heathcliff Dorado Garcia, Yi Bei, Karin Schmelz, Sascha Sauer, Angelika Eggert, Johannes H. Schulte, Roland F. Schwarz, Kerstin Haase, Richard P. Koche, and Anton G. Henssen

Subjects

Cancer Research, Oncology

Abstract

Extrachromosomal DNA circularization is a common event in cancer cells and frequently serves as a vehicle for cancer oncogene amplification. Random segregation of oncogene-containing extrachromosomal circular DNA promotes rapid intercellular heterogeneity, conferring tumors the ability to rapidly evolve and escape therapy. Smaller, copy-number neutral extrachromosomal circular DNAs are also abundantly identified in both healthy and malignant tissues, but their function in cancer is still unknown. Understanding how extrachromosomal circular DNAs contribute to intercellular heterogeneity in cancer cells remains crucial, however methods for an unbiased characterization of extrachromosomal circular DNAs in single cells are lacking. We introduce scEC&T-seq (single cell extrachromosomal circular DNA and transcriptomic sequencing), a method for parallel detection of extrachromosomal circular DNAs and full-length mRNA in single cells. We demonstrate the ability of our method to isolate and detect extrachromosomal circular DNAs genome-wide from all range of sizes in single cells. We observed that whereas large oncogene-containing circular DNAs are clonally present in most cancer cells, only a very small fraction of small circular DNAs are recurrently identified in single cells, indicating yet unknown prerequisites for maintenance and propagation. Our method was able to capture and recapitulate the structural complexity of oncogene-containing extrachromosomal circular DNAs in single cells, and the matching transcriptomic data allowed us to identify fusion transcripts resulting from the rearranged extrachromosomal structures. In addition, we observed that whereas the main structure of extrachromosomal circular DNAs is mostly stable in single cells, intercellular differences in extrachromosomal circular DNAs’ content can drive differences in oncogene transcription levels in single cells. We envision that by integrating extrachromosomal circular DNA and mRNA sequencing, our method will not only be useful to investigate the impact of intercellular heterogeneity in extrachromosomal circular DNA in tumor evolution, but also to interrogate its function in other biological and pathological processes. Citation Format: Rocio Chamorro Gonzalez, Thomas Conrad, Robin Xu, Madalina Giurgiu, Maja Cwikla, Katharina Kasack, Lotte Brückner, Eric van Leen, Elias Rodriguez-Fos, Konstantin Helmsauer, Heathcliff Dorado Garcia, Yi Bei, Karin Schmelz, Sascha Sauer, Angelika Eggert, Johannes H. Schulte, Roland F. Schwarz, Kerstin Haase, Richard P. Koche, Anton G. Henssen. Dissecting intercellular extrachromosomal circular DNA heterogeneity in single cancer cells with scEC&T-seq [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 1693.

Published

2022

9. Abstract A02: Patient-derived xenograft models of neuroblastoma as improvement for the prediction of targeted therapies for childhood cancer

Author

Angelika Eggert, Jens Hoffmann, Georg Seifert, Hedwig E. Deubzer, Anton G. Henssen, Wolfgang Walther, Jana Rolff, Patrick Hundsdörfer, Karin Schmelz, Dennis Gürgen, and Johannes H. Schulte

Subjects

Cancer Research, Vincristine, business.industry, Dacarbazine, Cancer, medicine.disease, Pediatric cancer, Gemcitabine, Transplantation, Oncology, Docetaxel, Neuroblastoma, Cancer research, Medicine, business, medicine.drug

Abstract

Introduction: Highly variable clinical outcomes including immediate fatal progression to spontaneous regression are characteristically observed for neuroblastoma (NB), a pediatric cancer arising from progenitors of the sympathetic nervous system. Pronounced rates of relapse and fast-evolving resistance against standard-of-care (SOC) treatments, together with a high degree of mutational mobility and heterogeneity, indicate the need for more precise and molecular targeted strategies. Aim: Patient-derived xenograft (PDX) models closely resemble human tumor biology from primary tissue and could be utilized for predictive preclinical testing. For this aim we established a cohort of 10 NB PDX models from 33 primary human tissue samples obtained from the Charité University Clinic. Specimen originated from proliferating areas while possible necrotic lesions had been removed prior to subcutaneous transplantation to immunodeficient NOG mice. After documenting stable growth over 3-4 initial passages, NB PDX models were screened for sensitivity to SOC drugs including actinomycin D, dacarbazine, docetaxel, doxorubicin, etoposide, ifosfamide, gemcitabine, and vincristine. Results: Characteristic NB pathology of all PDX was verified using HE and IHC staining of FFPE tumor sections comparing individual passages. Post-transplant lymphoproliferative disorder (PTLD) was excluded analyzing hCD45 specific marker. Depending on traceable somatic mutations, NB PDX doubling times dramatically varied between 4 days in aggressive, 8 days in intermediate, and up to 18 days in slowly growing tumors. Not surprisingly, high-risk NB tumors with confirmed MYCN amplification and ALK mutation exhibited the fastest growth in our cohort. In contrast, doubling rates of tumors with single ALK mutation or TERT rearrangement were not significantly different compared to the slowest PDX models without driver mutations. Most effective treatment response was observed for vincristine, leading to stable disease or partial regression in 5 out of 8 models (63%) achieving a tumor growth inhibition (TGI) of 70%, whereas all models were insensitive against dacarbazine treatment with a TGI of 33%, respectively. Conclusion: Currently, whole-exome sequencing of all models is performed. Molecular analysis will enable prediction of more precise therapeutic strategies. We will use our NB PDX to validate targeted treatment effects of recent pipeline drugs. As part of the European Innovative Therapies for Children with Cancer-Paediatric Preclinical Proof of Concept Platform (ITCC-P4) consortium, these findings will be correlated with predictions of the NB PDX molecular profile to achieve valuable benefit for pediatric patients. Citation Format: Dennis Gürgen, Jana Rolff, Johannes H. Schulte, Hedwig E. Deubzer, Karin Schmelz, Anton G. Henssen, Patrick Hundsdörfer, Georg Seifert, Angelika Eggert, Wolfgang Walther, Jens Hoffmann. Patient-derived xenograft models of neuroblastoma as improvement for the prediction of targeted therapies for childhood cancer [abstract]. In: Proceedings of the AACR Special Conference on the Evolving Landscape of Cancer Modeling; 2020 Mar 2-5; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2020;80(11 Suppl):Abstract nr A02.

Published

2020

10. Publisher Correction: Extrachromosomal circular DNA drives oncogenic genome remodeling in neuroblastoma

Author

Joern Toedling, Victor Bardinet, Angelika Eggert, Carolina Rosswog, Natalia Munoz-Perez, Steffen Fuchs, Anton G. Henssen, Jesper L.V. Maag, Theresa M Thole, Johannes H. Schulte, Dieter Beule, Matthias Fischer, David Torrents, Filippos Klironomos, Heathcliff Dorado Garcia, Hedwig E. Deubzer, Annabell Szymansky, Montserrat Puiggròs, Natalie Timme, Ian C. MacArthur, Eric Blanc, Annika Winkler, Rocio Chamorro, Annette Künkele, F Hertwig, Karin Schmelz, Yi Bei, Roland F. Schwarz, Katharina Kasack, Richard Koche, Martin Burkert, Sascha Sauer, Patrick Hundsdörfer, Elias Rodriguez-Fos, Nina Thiessen, Jessica Theissen, Claudia Röefzaad, and Konstantin Helmsauer

Subjects

Neuroblastoma, Genetics, medicine, Computational biology, Biology, Extrachromosomal circular DNA, medicine.disease, Genome

Published

2020

11. Reactivating TP53 signaling by the novel MDM2 inhibitor DS-3032b as a therapeutic option for high-risk neuroblastoma

Author

Joern Toedling, Angelika Eggert, Jasmin Wünschel, Jutta Proba, Annette Künkele, Viktor Arnhold, Patrick Hundsdoerfer, Karin Schmelz, Johannes H. Schulte, Annika Winkler, and Hedwig E. Deubzer

Subjects

0301 basic medicine, Cancer Research, Cell cycle checkpoint, medicine.medical_treatment, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, In vivo, Neuroblastoma, MYCN, Medicine, neoplasms, biology, business.industry, apoptosis, medicine.disease, targeted therapy, pediatric tumors, CDKN1A, 030104 developmental biology, Oncology, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Mdm2, MDM2 Inhibitor DS-3032b, business, G1 phase, Research Paper

Abstract

Fewer than 50% of patients with high-risk neuroblastoma survive five years after diagnosis with current treatment protocols. Molecular targeted therapies are expected to improve survival. Although MDM2 has been validated as a promising target in preclinical models, no MDM2 inhibitors have yet entered clinical trials for neuroblastoma patients. Toxic side effects, poor bioavailability and low efficacy of the available MDM2 inhibitors that have entered phase I/II trials drive the development of novel MDM2 inhibitors with an improved risk-benefit profile. We investigated the effect of the novel MDM2 small molecular inhibitor, DS-3032b, on viability, proliferation, senescence, migration, cell cycle arrest and apoptosis in a panel of six neuroblastoma cell lines with different TP53 and MYCN genetic backgrounds, and assessed efficacy in a murine subcutaneous model for high-risk neuroblastoma. Re-analysis of existing expression data from 476 primary neuroblastomas showed that high-level MDM2 expression correlated with poor patient survival. DS-3032b treatment enhanced TP53 target gene expression and induced G1 cell cycle arrest, senescence and apoptosis. CRISPR-mediated MDM2 knockout in neuroblastoma cells mimicked DS-3032b treatment. TP53 signaling was selectively activated by DS-3032b in neuroblastoma cells with wildtype TP53, regardless of the presence of MYCN amplification, but was significantly reduced by TP53 mutations or expression of a dominant-negative TP53 mutant. Oral DS-3032b administration inhibited xenograft tumor growth and prolonged mouse survival. Our in vitro and in vivo data demonstrate that DS-3032b reactivates TP53 signaling even in the presence of MYCN amplification in neuroblastoma cells, to reduce proliferative capacity and cause cytotoxicity.

Published

2017

12. XIAP expression is post-transcriptionally upregulated in childhood ALL and is associated with glucocorticoid response in T-cell ALL

Author

Karin Schmelz, Isabell Dietrich, Cornelia Eckert, Günter Henze, and Patrick Hundsdoerfer

Subjects

Apoptosis Inhibitor, business.industry, Hematology, Inhibitor of apoptosis, Peripheral blood mononuclear cell, XIAP, medicine.anatomical_structure, Oncology, Downregulation and upregulation, Apoptosis, Pediatrics, Perinatology and Child Health, medicine, Cancer research, Bone marrow, business, Glucocorticoid, medicine.drug

Abstract

Background Resistance to glucocorticoid induced apoptosis is one of the major risk factors for relapse and poor outcome in childhood acute lymphoblastic leukemia (ALL). Overexpression of X-linked inhibitor of apoptosis protein (XIAP) has been shown to be associated with chemotherapy resistance in several malignancies. Procedure XIAP protein and mRNA expression were determined in leukemic blasts of 51 childhood ALL patients and normal bone marrow mononuclear cells. XIAP expression was correlated with glucocorticoid response and outcome. Results XIAP protein but not mRNA expression was found to be highly increased in childhood ALL compared to control bone marrow mononuclear cells (MNC) (median: 3.5 vs. 0.14 ng/105 MNC, P

Published

2010

13. Epigenetic and genetic analysis of the survivin promoter in acute myeloid leukemia

Author

Ingo Tamm, Karin Schmelz, Bernd Dörken, and Mandy Wagner

Subjects

Cancer Research, Survivin, Bisulfite sequencing, Biology, Inhibitor of apoptosis, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Epigenesis, Genetic, Inhibitor of Apoptosis Proteins, Cell Line, Tumor, hemic and lymphatic diseases, Humans, Epigenetics, Promoter Regions, Genetic, neoplasms, Polymorphism, Single-Stranded Conformational, DNA Primers, Base Sequence, Myeloid leukemia, Promoter, Hematology, Methylation, DNA Methylation, Molecular biology, Neoplasm Proteins, Leukemia, Myeloid, Acute, Oncology, DNA methylation, Cancer research, Microtubule-Associated Proteins

Abstract

Survivin, an inhibitor of apoptosis (IAP) protein plays a dual role in regulation of mitosis and inhibition of apoptosis. Survivin is expressed in embryonic and fetal organs as well as in most human cancers, but not in normal differentiated adult tissues. In this study we investigated the molecular mechanism involved in overexpression of survivin in acute myeloid leukemia (AML). We used methylation specific PCR (MSP) and bisulfite sequencing to analyze the methylation status of the survivin promoter in primary AML samples and normal peripheral blood mononuclear cells (PBMCs). Both, in patients with de novo AML and normal control samples an unmethylated survivin promoter was present. Mutational analysis of the proximal survivin promoter revealed three single nucleotide polymorphisms (SNPs), where the frequently occurred polymorphism (G/C) at position -31 was detectable in both, AML blasts and healthy PBMCs and showed no significant impact on prognosis in de novo AML patients. These results suggest that the methylation status of the survivin promoter and occurrence of these SNPs within the promoter region of the survivin gene appear to be of minor importance in leukemogenesis.

Published

2008

14. Transcriptional regulation of humansurvivinby early growth response (Egr)-1 transcription factor

Author

Mandy Wagner, Ingo Tamm, Bernd Dörken, and Karin Schmelz

Subjects

Cancer Research, Programmed cell death, Oncology, Apoptosis, Transcription (biology), Survivin, Transcriptional regulation, Cancer research, Biology, Signal transduction, Inhibitor of apoptosis, neoplasms, Transcription factor

Abstract

Survivin, a member of the inhibitor of apoptosis protein family, is involved in both, inhibition of apoptosis and regulation of cell division. Because of the tumor-specific expression of survivin, the reduction of its expression is an important therapeutic option in the treatment of malignant diseases. Thus, we analyzed the transcriptional regulation of survivin in order to establish survivin as a target gene for new therapeutic approaches. Here, we describe a novel regulatory region within the survivin promoter. After treatment with phorbol 12-myristate-13-acetate, the early growth response (Egr)-1 transcription factor binds to the sequence 5′GAGGGGGCG 3′ within the human survivin promoter in vitro and in entire cells. In reporter-gene assays and overexpression experiments, survivin is downregulated following exogenous expression of wildtype Egr-1. Using p53 wildtype and mutated cell lines, we show that Egr-1 negatively regulates survivin expression and sensitizes cell lines to TRAIL-induced apoptosis. © 2007 Wiley-Liss, Inc.

Published

2007

15. In vivo expression of survivin and its splice variant survivin-2B: Impact on clinical outcome in acute myeloid leukemia

Author

Ingo Tamm, Christian Wuchter, Bernd Dörken, Mandy Wagner, Karin Schmelz, and Wolf-Dieter Ludwig

Subjects

Adult, Male, Cancer Research, Survivin, Apoptosis, Biology, Inhibitor of apoptosis, Disease-Free Survival, Immunophenotyping, Inhibitor of Apoptosis Proteins, In vivo, Gene expression, Humans, splice, RNA, Messenger, neoplasms, Aged, Neoplasm Staging, Myeloid leukemia, DNA, Neoplasm, Middle Aged, Prognosis, Neoplasm Proteins, Alternative Splicing, Oncology, Leukemia, Myeloid, Case-Control Studies, Acute Disease, Immunology, Cancer research, Female, Microtubule-Associated Proteins

Abstract

Survivin, a member of the inhibitor of apoptosis protein family, is expressed in most human cancers, but undetectable in normal differentiated adult tissue in vivo. Because of this cancer-related expression, survivin is a promising target for cancer therapy. To determine the expression and prognostic role of survivin in acute myeloid leukemia (AML), we investigated the mRNA expression pattern of survivin and of the splice variants survivin-2B and survivin-DeltaEx3 in adult (n = 74) and children (n = 31) with de novo AML using RT-PCR. Survivin was the predominant transcript variant in AML cells, whereas significantly lower levels of survivin-2B and survivin-DeltaEx3 were observed (p < or = 0.0001). Neither expression of survivin nor of any splice variant correlated with maturation stage (FAB subtypes, immunophenotype) or cytogenetic risk groups. For AML cases treated according to AMLCG92 (adult) and AML-BFM93 (children) protocols, respectively, expression patterns were correlated with clinical data: in adult AML (n = 51), low expression of survivin-2B correlated with a better overall survival (p = 0.05; mean survival time 19 months vs. 9 months) and a better eventfree survival (p < or = 0.01; 27 months vs. 10 months). In childhood AML (n = 31), high survivin-DeltaEx3 expression was associated with a shorter overall survival (p < or = 0.05; 24 months vs. 43 months). We conclude that certain survivin splice variants have potential prognostic impact for long-term therapy outcome in adult as well as childhood de novo AML.

Published

2006

16. 5-Aza-2′-deoxycytidine induces p21WAF expression by demethylation of p73 leading to p53-independent apoptosis in myeloid leukemia

Author

Bernd Dörken, Mandy Wagner, Ingo Tamm, and Karin Schmelz

Subjects

Cancer Research, Time Factors, Myeloid, Apoptosis, Cell Cycle Proteins, Biochemistry, Membrane Potentials, hemic and lymphatic diseases, Genes, Tumor Suppressor, Promoter Regions, Genetic, Caspase, Caspase 3, Reverse Transcriptase Polymerase Chain Reaction, Chemistry, Cell Cycle, Cytochromes c, Nuclear Proteins, Myeloid leukemia, U937 Cells, Hematology, Methylation, Cell cycle, Flow Cytometry, Mitochondria, Up-Regulation, DNA-Binding Proteins, Leukemia, Myeloid, Acute, Leukemia, medicine.anatomical_structure, Oncology, Caspases, DNA methylation, Azacitidine, G1 phase, medicine.drug, Cyclin-Dependent Kinase Inhibitor p21, Programmed cell death, Blotting, Western, Immunology, Decitabine, HL-60 Cells, chemical and pharmacologic phenomena, Biology, Transfection, Peripheral blood mononuclear cell, Cell Line, Tumor, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, mental disorders, medicine, Humans, Sulfites, RNA, Messenger, neoplasms, Tumor Suppressor Proteins, G1 Phase, Epithelial Cells, Tumor Protein p73, Cell Biology, DNA Methylation, medicine.disease, Microscopy, Fluorescence, Cell culture, Myelodysplastic Syndromes, Leukocytes, Mononuclear, biology.protein, Cancer research, RNA, CpG Islands, Tumor Suppressor Protein p53, HeLa Cells

Abstract

The DNA methylation inhibitor 5′-Aza-2-deoxycytidine (5-Aza-CdR) has significant therapeutic value for the treatment of patients with myelodysplastic syndrome (MDS), acute and chronic myeloid leukemia (AML and CML). The demethylating effect of 5-Aza-CdR has been well characterized. In contrast, less is known about the molecular events downstream of the methylation inhibition effect. We found that 5-Aza-CdR induces apoptosis in AML cells (both, p53 mutant and wildtype) but not in epithelial or normal peripheral blood mononuclear cells (PBMC). Cell death was accompanied by activation of the mitochondrial apoptosis pathway as shown by early release of cytochrome c and AIF and loss of the mitochondrial membrane potential Δψm. Activation of caspase-3 but not -6 and -8 was detectable using western blot analysis and measurement of caspase enzymatic activity. 5-Aza-CdR treatment resulted in the induction of p21 which correlated with the arrest of AML cells in the G1 cell cycle phase. Induction of p21 expression was independent of its promoter methylation status but was mediated by 5-Aza-CdR-induced reexpression of the tumor suppressor p73, a known upstream regulator of p21. The p73 promoter was hypermethylated in AML cell lines and in primary AML cells but not in epithelial cells which were resistent towards 5-Aza-CdR. Therefore, 5-Aza-CdR-mediated specific killing of myeloid cells might be dependent on its ability to revert p73 promoter methylation and to reexpress p73 mRNA. In addition, exogenous expression of p73 rendered epithelial cells sensitive to apoptosis induced by 5-Aza-CdR or other cytostatic drugs. We therefore conclude that p73 is a relevant target for methylation-dependent efficacy of 5-Aza-CdR in AML cells.

Published

2004

17. Induction of gene expression by 5-Aza-2′-deoxycytidine in acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS) but not epithelial cells by DNA-methylation-dependent and -independent mechanisms

Author

Ingo Tamm, Mandy Wagner, Bernd Dörken, N Sattler, Karin Schmelz, and Michael Lübbert

Subjects

Cancer Research, Decitabine, Apoptosis, chemical and pharmacologic phenomena, Biology, Polymerase Chain Reaction, hemic and lymphatic diseases, mental disorders, Gene expression, medicine, Humans, neoplasms, DNA Primers, Regulation of gene expression, Base Sequence, Myeloid leukemia, Epithelial Cells, Hematology, Methylation, DNA Methylation, medicine.disease, Gene Expression Regulation, Neoplastic, Leukemia, Oncology, CpG site, Leukemia, Myeloid, Myelodysplastic Syndromes, Acute Disease, DNA methylation, Azacitidine, Cancer research, Cell Division, medicine.drug

Abstract

The methylation inhibitor 5-Aza-2'-deoxycytidine (5-Aza-CdR, decitabine) has therapeutic efficacy in acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS). Using microarray analysis, we investigated global changes in gene expression after 5-Aza-CdR treatment in AML. In the AML cell line OCI-AML2, Aza-CdR induced the expression of 81 out of 22 000 genes; 96 genes were downregulated (> or =2-fold change in expression). RT-PCR analysis of 10 randomly selected genes confirmed the changes of expression in AML cells. Similar results were obtained with primary AML and MDS cells after treatment with 5-Aza-CdR ex vivo and in vivo, respectively. In contrast, significantly fewer changes in gene expression and cytotoxicity were detected in normal peripheral blood mononuclear and bone marrow cells or transformed epithelial cells treated with 5-Aza-CdR. Interestingly, only 50.6% of the induced genes contain putative CpG islands in the 5' region. To further investigate the significance of promoter methylation in the induced genes, we analyzed the actual methylation status of randomly selected 5-Aza-CdR-inducible genes. We detected hypermethylation exclusively in the 5' region of the myeloperoxidase (MPO) gene. DNA methylation inversely correlated with MPO expression in newly diagnosed untreated AML patients (P< or =0.004). In contrast, all other analyzed 5-Aza-CdR-inducible genes revealed no CpG methylation in the promoter region, suggesting a methylation-independent effect of 5-Aza-CdR.

Published

2004

18. Activation of caspase-8 in drug-induced apoptosis of B-lymphoid cells is independent of CD95/Fas receptor-ligand interaction and occurs downstream of caspase-3

Author

Peter T. Daniel, Rudi Beyaert, Frank Essmann, Klaus Schulze-Osthoff, Bernd Dörken, Thomas Wieder, Karin Schmelz, and Aram Prokop

Subjects

Fas Ligand Protein, Lymphoma, B-Cell, Paclitaxel, Fas-Associated Death Domain Protein, Immunoblotting, Immunology, Antineoplastic Agents, Apoptosis, Caspase 3, Transfection, Caspase 8, Biochemistry, Fas ligand, Bone Marrow, Tumor Cells, Cultured, Humans, fas Receptor, FADD, Child, Caspase, Adaptor Proteins, Signal Transducing, Epirubicin, Death domain, Antibiotics, Antineoplastic, Membrane Glycoproteins, biology, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Fas receptor, Caspase 9, Cell biology, Caspases, biology.protein, Cancer research, Carrier Proteins

Abstract

The activation of caspase-8, a crucial upstream mediator of death receptor signaling, was investigated in epirubicin- and Taxol-induced apoptosis of B-lymphoma cells. This study was performed because the CD95/Fas receptor-ligand interaction, recruitment of the Fas-associated death domain (FADD) adaptor protein, and subsequent activation of procaspase-8 have been implicated in the execution of drug-induced apoptosis in other cell types. Indeed, active caspase-8 was readily detected after treatment of mature and immature B-lymphoid cells with epirubicin or Taxol. However, neither constitutive nor drug-induced expression of the CD95/Fas ligand was detectable in B-lymphoma cells. Furthermore, overexpression of a dominant-negative FADD mutant (FADDdn) did not block caspase-8 processing and subsequent DNA fragmentation, indicating that drug-induced caspase-8 activation was mediated by a CD95/Fas-independent mechanism. Instead, caspase-8 cleavage was slightly preceded by activation of caspase-3, suggesting that drug-induced caspase-8 activation in B-lymphoma cells is a downstream event mediated by other caspases. This assumption was confirmed in 2 experimental systems—zDEVD-fmk, a cell-permeable inhibitor of caspase-3–like activity, blocked drug-induced caspase-8 cleavage, and depletion of caspase-3 from cell extracts impaired caspase-8 cleavage after in vitro activation with dATP and cytochrome c. Thus, these data indicate that drug-induced caspase-8 activation in B-lymphoma cells is independent of death receptor signaling and is mediated by postmitochondrial caspase-3 activation.

Published

2001

19. A novel NO-responding regulator controls the reduction of nitric oxide in Ralstonia eutropha

Author

Bärbel Friedrich, Rainer Cramm, Anne Pohlmann, and Karin Schmelz

Subjects

Transcription, Genetic, Molecular Sequence Data, Denitrification pathway, Mutant, Regulator, Sigma Factor, Biology, Nitric Oxide, Microbiology, Nitric oxide, chemistry.chemical_compound, Bacterial Proteins, Transcription (biology), Genes, Regulator, Amino Acid Sequence, Molecular Biology, Gene, Regulator gene, DNA-Directed RNA Polymerases, Gene Expression Regulation, Bacterial, Physical Chromosome Mapping, DNA-Binding Proteins, chemistry, Biochemistry, rpoN, Cupriavidus necator, Oxidoreductases, Oxidation-Reduction, RNA Polymerase Sigma 54

Abstract

Ralstonia eutropha H16 mediates the reduction of nitric oxide (NO) to nitrous oxide (N2O) with two isofunctional single component membrane-bound NO reductases (NorB1 and NorB2). This reaction is integrated into the denitrification pathway that involves the successive reduction of nitrate to dinitrogen. The norB1 gene is co-transcribed with norA1 from a sigma54 (RpoN)-dependent promoter, located upstream of norA1. With the aid of norA1'-lacZ transcriptional fusions and the generation of regulatory mutants, it was shown that norB1 gene transcription requires a functional rpoN gene and the regulator NorR, a novel member of the NtrC family of response regulators. The regulator gene maps adjacent to norAB, is divergently transcribed and present in two copies on the megaplasmid pHG1 (norR1) and the chromosome (norR2). Transcription activation by NorR responds to the availability of NO. A nitrite reductase-deficient mutant that is incapable of producing NO endogenously, showed a 70% decrease of norA1 expression. Addition of the NO-donating agent sodium nitroprusside caused induction of norA1'-lacZ transcription. Truncation of the N-terminal receiver domain of NorR1 interrupted the NO signal transduction and led to a constitutive expression of norA1'-lacZ. The results indicate that NorR controls the reductive conversion of NO in R. eutropha. This reaction is not strictly co-ordinated on the regulatory level with the other nitrogen oxide-reducing steps of the denitrification chain that are independent of NorR.

Published

2000

20. XIAP expression is post-transcriptionally upregulated in childhood ALL and is associated with glucocorticoid response in T-cell ALL

Author

Patrick, Hundsdoerfer, Isabell, Dietrich, Karin, Schmelz, Cornelia, Eckert, and Günter, Henze

Subjects

Adult, Male, Gene Expression Regulation, Leukemic, Drug Resistance, Bone Marrow Cells, Bone Marrow Examination, X-Linked Inhibitor of Apoptosis Protein, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Monocytes, Up-Regulation, Treatment Outcome, Pharmacogenetics, Antineoplastic Combined Chemotherapy Protocols, Humans, Leukemia-Lymphoma, Adult T-Cell, Female, RNA, Messenger, Child, Glucocorticoids

Abstract

Resistance to glucocorticoid induced apoptosis is one of the major risk factors for relapse and poor outcome in childhood acute lymphoblastic leukemia (ALL). Overexpression of X-linked inhibitor of apoptosis protein (XIAP) has been shown to be associated with chemotherapy resistance in several malignancies.XIAP protein and mRNA expression were determined in leukemic blasts of 51 childhood ALL patients and normal bone marrow mononuclear cells. XIAP expression was correlated with glucocorticoid response and outcome.XIAP protein but not mRNA expression was found to be highly increased in childhood ALL compared to control bone marrow mononuclear cells (MNC) (median: 3.5 vs. 0.14 ng/10(5) MNC, P0.0001) indicating a post-transcriptional regulation of XIAP expression. In patients with T-cell ALL, poor prednisone response was associated with increased XIAP expression (median: 2.8 in good vs. 5.8 in poor responders; P = 0.005). Similarly, T-cell ALL patients suffering adverse events showed higher initial XIAP levels than patients in continuous complete remission (CCR) (median: 2.7 in patients in CCR vs. 5.6 in patients suffering adverse events; P = 0.007). XIAP inhibition using the low-molecular-weight SMAC mimetic LBW242 resulted in a significant increase of prednisone-induced apoptosis in vitro.In childhood ALL compared to control bone marrow, the expression of the apoptosis inhibitor XIAP is highly increased by post-transcriptional regulation. The association with poor in vivo glucocorticoid response and outcome in T-cell ALL suggests XIAP inhibition as a promising novel approach for the treatment of resistant ALL.

Published

2010

21. Transcriptional regulation of human survivin by early growth response (Egr)-1 transcription factor

Author

Mandy, Wagner, Karin, Schmelz, Bernd, Dörken, and Ingo, Tamm

Subjects

Chromatin Immunoprecipitation, Binding Sites, Base Sequence, Transcription, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Survivin, Molecular Sequence Data, Apoptosis, Electrophoretic Mobility Shift Assay, DNA, Cell Line, Inhibitor of Apoptosis Proteins, Neoplasm Proteins, TNF-Related Apoptosis-Inducing Ligand, Gene Expression Regulation, Cell Line, Tumor, Humans, RNA, Messenger, Promoter Regions, Genetic, Microtubule-Associated Proteins, Early Growth Response Protein 1

Abstract

Survivin, a member of the inhibitor of apoptosis protein family, is involved in both, inhibition of apoptosis and regulation of cell division. Because of the tumor-specific expression of survivin, the reduction of its expression is an important therapeutic option in the treatment of malignant diseases. Thus, we analyzed the transcriptional regulation of survivin in order to establish survivin as a target gene for new therapeutic approaches. Here, we describe a novel regulatory region within the survivin promoter. After treatment with phorbol 12-myristate-13-acetate, the early growth response (Egr)-1 transcription factor binds to the sequence 5'GAGGGGGCG 3' within the human survivin promoter in vitro and in entire cells. In reporter-gene assays and overexpression experiments, survivin is downregulated following exogenous expression of wildtype Egr-1. Using p53 wildtype and mutated cell lines, we show that Egr-1 negatively regulates survivin expression and sensitizes cell lines to TRAIL-induced apoptosis.

Published

2007

22. Endogenous hSNM1B/Apollo interacts with TRF2 and stimulates ATM in response to ionizing radiation

Author

Julia Kallenbach, Karin Schmelz, Paul S. Bradshaw, Marco Anders, Patrick Concannon, Stefanie Heinrich, M. Stephen Meyn, Ilja Demuth, Martin Digweed, and Anika Lindner

Subjects

Tumor suppressor gene, DNA repair, Blotting, Western, Fluorescent Antibody Technique, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, Biology, Protein Serine-Threonine Kinases, Biochemistry, DNA-binding protein, Article, Cell Line, Radiation, Ionizing, Humans, Telomeric Repeat Binding Protein 2, Nuclear protein, Phosphorylation, RNA, Small Interfering, Molecular Biology, Tumor Suppressor Proteins, Autophosphorylation, Nuclear Proteins, Cell Biology, Molecular biology, Telomere, Cell biology, DNA-Binding Proteins, DNA Repair Enzymes, Exodeoxyribonucleases, Protein Binding

Abstract

Human SNM1B/Apollo is involved in the cellular response to DNA-damage, however, its precise role is unknown. Recent reports have implicated hSNM1B in the protection of telomeres. We have found hSNM1B to interact with TRF2, a protein which functions in telomere protection and in an early response to ionizing radiation. Here we show that endogenous hSNM1B forms foci which colocalize at telomeres with TRF1 and TRF2. However, we observed that additional hSNM1B foci could be induced upon exposure to ionizing radiation (IR). In live-cell-imaging experiments, hSNM1B localized to photo-induced double-strand breaks (DSBs) within 10 s post-induction. Further supporting a role for hSNM1B in the early stages of the cellular response to DSBs, we observed that autophosphorylation of ATM, as well as the phosphorylation of ATM target proteins in response to IR, was attenuated in cells depleted of hSNM1B. These observations suggest an important role for hSNM1B in the response to IR damage, a role that may be, in part, upstream of the central player in maintenance of genome integrity, ATM.

Published

2007

23. Extreme variation in apoptosis capacity amongst lymphoid cells of Nijmegen breakage syndrome patients

Author

Krystyna H. Chrzanowska, Ilja Demuth, Karin Schmelz, Nadine Burghardt, Nadja Thierfelder, Martin Digweed, Eva Seemanova, and Karl Sperling

Subjects

Adult, Male, Histology, Adolescent, DNA damage, Apoptosis, Cell Cycle Proteins, Biology, Pathology and Forensic Medicine, Bleomycin, Cell Line, Tumor, medicine, Humans, Radiosensitivity, Phosphorylation, Child, Nijmegen Breakage Syndrome, Immunodeficiency, B-Lymphocytes, Genetic disorder, Nuclear Proteins, Cell Biology, General Medicine, medicine.disease, Nibrin, Lymphoma, Immunology, Female, Tumor Suppressor Protein p53, Nijmegen breakage syndrome, DNA Damage

Abstract

The human genetic disorder, Nijmegen breakage syndrome (NBS), is characterised by radiosensitivity, immunodeficiency and an increased risk for cancer, particularly lymphoma. The NBS1 gene codes for a protein, nibrin, involved in the processing/repair of DNA double strand breaks and in cell cycle checkpoints. The majority of patients (>90%) are homozygous for a founder mutation. Despite this genetic homogeneity, the syndrome shows considerable clinical variability, for example, in age at development of a malignancy. We hypothesised that one reason for such variation might be individual differences in the clearance of heavily damaged precancerous cells by apoptosis. To test this hypothesis we have examined a set of 30 lymphoblastoid B-cell lines from NBS patients for their capacity to enter into apoptosis after a DNA-damaging treatment. There was a substantial 40-fold variation in apoptosis between cell lines from different patients. NBS patient cell lines could be grouped into a large, apoptosis-deficient group and a smaller group with essentially normal apoptotic response to DNA damage. In both groups, cell lines were proficient in TP53 phosphorylation and stabilisation after the same DNA-damaging treatment. Thus the observed variation in apoptosis capacity is not due to failure to activate TP53. Despite the large variation in apoptosis, no statistically significant correlation between apoptotic capacity of patient cell lines and clinical course of the disease was apparent.

Published

2007

24. Decitabine activates specific caspases downstream of p73 in myeloid leukemia

Author

Karin Schmelz, Ingo Tamm, and Mandy Wagner

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Antimetabolites, Antineoplastic, Myeloid, Decitabine, Apoptosis, Cell Line, Tumor, medicine, Humans, Promoter Regions, Genetic, neoplasms, Caspase, biology, Caspase 3, Tumor Suppressor Proteins, Myeloid leukemia, Nuclear Proteins, Tumor Protein p73, Hematology, General Medicine, Cell cycle, DNA Methylation, medicine.disease, DNA-Binding Proteins, Enzyme Activation, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, DNA methylation, Cancer research, biology.protein, Azacitidine, medicine.drug

Abstract

The demethylating effect of 5-aza-2′ deoxycytidine (decitabine, DAC) has been well characterized. The molecular events downstream of methylation inhibition are less well known. Here, DAC was shown to induce apoptosis in acute myeloid leukemia (AML) cells (p53 mutant and wild type) but not in epithelial or normal peripheral blood mononuclear cells. Apoptosis was characterized by activation of the mitochondrial but not the receptor death pathway, as demonstrated by the release of cytochrome c and loss of mitochondrial membrane potential. Western blotting and enzyme assays showed that caspase-3, but not caspase-6 or caspase-8, were activated. Decitabine induced expression of the cell cycle inhibitor p21, arresting AML cell lines in G1 of the cell cycle. Expression of p21 was induced irrespective of the methylation status of its promoter, mediated instead via reexpression of the tumor suppressor p73, an upstream regulator of p21. The promoter of p73 was hypermethylated in AML cell lines in vitro and in primary AML cells ex vivo but not in DAC-resistant epithelial cells. In conclusion, DAC acts on leukemic myeloid cells via caspase activation, which may be dependent on demethylation of the hypermethylated p73 promoter and consequent reexpression of p73.

Published

2005

25. XIAP expression correlates with monocytic differentiation in adult de novo AML: impact on prognosis

Author

Frank Scholz, Torsten Haferlach, Doreen Oltersdorf, Leonid Karawajew, Wolf-Dieter Ludwig, Claudia Schoch, Karin Schmelz, Stephan Richter, Christian Wuchter, and Ingo Tamm

Subjects

Adult, Male, Myeloid, Survivin, X-Linked Inhibitor of Apoptosis Protein, Biology, Inhibitor of apoptosis, Monocytes, Immunophenotyping, Inhibitor of Apoptosis Proteins, Predictive Value of Tests, Risk Factors, medicine, Humans, Aged, Image Cytometry, Caspase 3, Myeloid leukemia, Proteins, Cell Differentiation, Hematology, Middle Aged, medicine.disease, Flow Cytometry, Prognosis, Antigens, Differentiation, Survival Analysis, XIAP, Neoplasm Proteins, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Proto-Oncogene Proteins c-bcl-2, Caspases, Immunology, Cancer research, Female, Myelopoiesis, Microtubule-Associated Proteins

Abstract

Antiapoptotic proteins like the inhibitor of apoptosis proteins (IAPs) are molecular markers potentially useful for the characterization of acute myeloid leukemia (AML). We screened 92 adults with de novo AML for the protein expression of various IAPs, Bcl-2 family members and the proform of Caspase-3 using quantitative immunoblot and flow cytometry. XIAP expression correlated with myelomonocytic French-American-British (FAB) subtypes M4/M5 (P < 0.05) and expression of monocytic markers (CD 14, CD 36; P < 0.05; CD 4, HLA-DR; P < 0.01) in AML blasts. In addition, XIAP was overexpressed in normal monocytes but undetectable in granulocytes. In AML, XIAP expression was significantly lower in patients with favorable than intermediate or poor cytogenetics (n = 74; P < 0.05). In total, 62 of the examined patients were treated according to the German AML Cooperative Group (AMLCG) 92 protocol. These patients were analyzed for prognostic significance of apoptosis-related proteins. Patients expressing low levels of XIAP enjoyed better overall survival than patients expressing high amounts of XIAP (mean, 9 (n = 41) versus 19 months (n = 21); P < 0.05). Other IAPs, most importantly Survivin, were of no prognostic value. We conclude that XIAP but not other IAP family members is associated with monocytic differentiation in normal and malignant myelopoiesis, and may be of prognostic significance for overall survival in adult de novo AML.

Published

2004

26. Tumor necrosis factor alpha sensitizes malignant cells to chemotherapeutic drugs via the mitochondrial apoptosis pathway independently of caspase-8 and NF-kappaB

Author

Peter-T Daniel, Klaus Schulze-Osthoff, Frank Essmann, Antje Müller, Thomas Wieder, Bernd Dörken, Christoph-C Geilen, Karin Schmelz, and Ingo Tamm

Subjects

Adult, Cancer Research, Ceramide, medicine.medical_specialty, medicine.medical_treatment, bcl-X Protein, Antineoplastic Agents, Apoptosis, Biology, Caspase 8, Ceramides, Membrane Potentials, chemistry.chemical_compound, Internal medicine, Cell Line, Tumor, Genetics, medicine, Humans, FADD, Molecular Biology, Sensitization, Epirubicin, Etoposide, Cell Death, Tumor Necrosis Factor-alpha, NF-kappa B, Intracellular Membranes, Blotting, Northern, Hodgkin Disease, Mitochondria, Sphingomyelins, medicine.anatomical_structure, Cytokine, Endocrinology, chemistry, Mitochondrial permeability transition pore, Proto-Oncogene Proteins c-bcl-2, Drug Resistance, Neoplasm, Leukemia, Myeloid, Caspases, biology.protein, Cancer research, Tumor necrosis factor alpha

Abstract

The Hodgkin cell line HD-MyZ is resistant to apoptosis induced by tumor necrosis factor alpha (TNFalpha). In the present work, we show that pretreatment with TNFalpha sensitized the cells to apoptosis induced by antineoplastic agents and ceramide. TNFalpha pretreatment resulted in enhanced cleavage and activity of caspase-3 upon addition of etoposide, epirubicin or ceramide. No caspase-8 activation was detectable, although caspase-8 could be activated in cell-free extracts. Inhibition of caspase-8 by z-IETD-fmk did not block the sensitizing effect of TNFalpha. Furthermore, exogenous ceramide, a mediator of TNFalpha signaling, could not substitute for TNFalpha in sensitization to drug-induced apoptosis. In contrast, we observed mitochondrial changes following cotreatment of cells with TNFalpha and drugs. Mitochondrial permeability transition, cytochrome c release and subsequent processing of caspase-9 preceded the onset of apoptosis, and were enhanced by TNFalpha pretreatment. Interestingly, although transcription factor NF-kappaB protected HD-MyZ cells from drug-induced apoptosis, TNFalpha-mediated sensitization was independent of NF-kappaB, since overexpressing a dominant-negative IkappaB mutant did not alter the TNFalpha effect. Sensitization for drug-induced apoptosis by TNFalpha was abrogated by Bcl-x(L). Thus, the sensitizing effect of TNFalpha is mediated by the mitochondrial pathway and involves processing of caspase-2, -3 and -9, but appears to be independent of caspase-8 processing, Bid cleavage and NF-kappaB signaling. Therefore, sensitization by TNFalpha is mediated at least in part through different pathways, as reported for TRAIL. There, sensitization occurs through a FADD/caspase-8-dependent mechanism. Regarding TNFalpha, the sensitizing effect was also observed in myeloid leukemia cells. Therefore, TNFalpha or alternate molecules activating its pathways might be useful as sensitizers for chemotherapy in hematological malignancies.

Published

2004

27. Survivin Is Negatively Regulated by Early Growth Response (Egr)-1 Transcription Factor in Acute Myeloid Leukemia

Author

Mandy Wagner, Ingo Tamm, Karin Schmelz, and Bernd Dörken

Subjects

Expression vector, Immunology, Cell Biology, Hematology, Transfection, Biology, Inhibitor of apoptosis, Biochemistry, Molecular biology, body regions, Apoptosis, Cell culture, Survivin, Cancer research, neoplasms, Chromatin immunoprecipitation, Transcription factor, hormones, hormone substitutes, and hormone antagonists

Abstract

Survivin, a member of the inhibitor of apoptosis protein family, is involved in both, inhibition of apoptosis and regulation of cell division. It is expressed in embryonic and fetal tissues as well as in the majority of human leukemias, but is undetectable in normal differentiated adult tissue in vivo. The molecular mechanisms involved in the cancer-specific re-expression of survivin are unclear. In this study, we describe a novel mechanism for over-expression of survivin in AML. Using electrophoretic mobility shift assays (EMSA), we show that the early growth response (Egr)-1 transcription factor binds to the sequence 5′ GAGGGGGCG 3′ within the human survivin promoter after induction by phorbol 12-myristate-13-acetate (PMA) in vitro. Furthermore, chromatin immunoprecipitation (ChIP) analysis confirmed the specific binding of Egr-1 to the proximal survivin promoter in PMA treated entire leukemia cells. To further analyze the functionality of the Egr-1 site within the survivin promoter in entire cells, transient transfections of p53 wildtype and mutated cell lines with wildtype Egr-1 expression vector were performed. In these overexpression experiments, mRNA and protein levels of survivin but not of control protein were downregulated after exogenous expression of wildtype Egr-1. Using reporter-gene assays, basal survivin promoter activity was decreased significantly by wildtype Egr-1 transfection, whereas mutant Egr-1 did not change activity of the survivin promoter, implying that Egr-1 specifically blocks survivin expression at the transcriptional level. In addition, Egr-1 over-expression sensitized cells to TRAIL-induced apoptosis. To investigate the expression pattern of Egr-1 in different AML cell lines and control samples from healthy donors, we analyzed the expression of Egr-1 by RT-PCR. Fitting with the above shown data, Egr-1 was expressed at significantly lower levels in AML cell lines expressing high survivin levels than in healthy control samples with low survivin levels. Taken together, we show that the transcription factor Egr-1 binds to the human survivin promoter in vitro and in entire cells, downregulates survivin expression independently of p53 and sensitizes cells to TRAIL-induced apoptosis. Since Survivin is often overexpressed in AML, downregulating Survivin expression by activating Egr-1 may be an interesting therapeutic option.

Published

2006

28. Decitabine: Where Is the Target?

Author

Karin Schmelz, Michael Lübbert, Philipp D. LeCoutre, Ingo Tamm, Nicole Sattler, Bernd Dörken, and Mandy Wagner

Subjects

Immunology, Myeloid leukemia, Decitabine, Promoter, Cell Biology, Hematology, Methylation, Biology, Biochemistry, Molecular biology, medicine.anatomical_structure, CpG site, hemic and lymphatic diseases, Gene expression, DNA methylation, medicine, Bone marrow, medicine.drug

Abstract

The methylation inhibitor 5-Aza-2′-deoxycytidine (decitabine) has therapeutic efficacy in acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS). Using microarray analysis, we investigated global changes in gene expression after decitabine treatment in AML. In the AML cell line OCI-AML2, decitabine induced the expression of 81 out of 22 000 genes; 96 genes were downregulated (X2-fold change in expression). RT-PCR analysis of 10 randomly selected genes confirmed the changes of expression in AML cells. Similar results were obtained with primary AML and MDS cells after treatment with decitabine ex vivo and in vivo, respectively. In contrast, significantly fewer changes in gene expression and cytotoxicity were detected in normal peripheral blood mononuclear and bone marrow cells or transformed epithelial cells treated with decitabine. Interestingly, only 50.6% of the induced genes contain putative CpG islands in the 5′ region. To further investigate the significance of promoter methylation in the induced genes, we analyzed the actual methylation status of randomly selected decitabine-inducible genes. We detected hypermethylation exclusively in the 5′ region of the myeloperoxidase (MPO) gene. DNA methylation inversely correlated with MPO expression in newly diagnosed untreated AML patients (P

Published

2005