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1. Attenuation of soft-tissue sarcomas resistance to the cytotoxic action of TNF-α by restoring p53 function.

Author

Jane Muret, Meriem Hasmim, Izabela Stasik, Abdelali Jalil, Aude Mallavialle, Arash Nanbakhsh, Ludovic Lacroix, Katy Billot, Véronique Baud, Jérome Thiery, Philippe Vielh, Philippe Terrier, Joelle Wiels, Lyubomir Vassilev, Axel Lecesne, Sylvie Bonvalot, and Salem Chouaib

Subjects
Medicine, Science
Abstract

BackgroundIsolated limb perfusion with TNF-α and melphalan is used with remarkable efficiency to treat unresectable limb sarcomas. Here we tested the ability of TNF-α to directly induce apoptosis of sarcoma cells. In addition, we investigated the impact of p53 in the regulation of such effect.Methodology/principal findingsWe first analysed the ability of TNF-α to induce apoptosis in freshly isolated tumour cells. For this purpose, sarcoma tumours (n = 8) treated ex vivo with TNF-α were processed for TUNEL staining. It revealed substantial endothelial cell apoptosis and levels of tumour cell apoptosis that varied from low to high. In order to investigate the role of p53 in TNF-α-induced cell death, human sarcoma cell lines (n = 9) with different TP53 and MDM2 status were studied for their sensitivity to TNF-α. TP53(Wt) cell lines were sensitive to TNF-α unless MDM2 was over-expressed. However, TP53(Mut) and TP53(Null) cell lines were resistant. TP53 suppression in TP53(Wt) cell lines abrogated TNF-α sensitivity and TP53 overexpression in TP53(Null) cell lines restored it. The use of small molecules that restore p53 activity, such as CP-31398 or Nutlin-3a, in association with TNF-α, potentiated the cell death of respectively TP53(Mut) and TP53(Wt)/MDM2(Ampl). In particular, CP-31398 was able to induce p53 as well as some of its apoptotic target genes in TP53(Mut) cells. In TP53(Wt)/MDM2(Ampl) cells, Nutlin-3a effects were associated with a decrease of TNF-α-induced NF-κB-DNA binding and correlated with a differential regulation of pro- and anti-apoptotic genes such as TP53BP2, GADD45, TGF-β1 and FAIM.Conclusion/significanceMore effective therapeutic approaches are critically needed for the treatment of unresectable limb sarcomas. Our results show that restoring p53 activity in sarcoma cells correlated with increased sensitivity to TNF-α, suggesting that this strategy may be an important determinant of TNF-α-based sarcomas treatment.

Published
2012
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4. Supplementary Figure 3 from FLIP: A Targetable Mediator of Resistance to Radiation in Non–Small Cell Lung Cancer

Author

Daniel B. Longley, Kevin M. Prise, Karl T. Butterworth, Gerard G. Hanna, Timothy Harrison, Patrick G. Johnston, Caitriona Holohan, Nyree Crawford, Catherine Higgins, Joanna Majkut, Catherine Fenning, Izabela Stasik, Luke Humphreys, Conor A. Bradley, Zsuzsanna Nemeth, and Kylie A. McLaughlin

Abstract

IR-induced changes in cell surface expression of death receptors

Published
2023

6. Supplementary Figure 4 from FLIP: A Targetable Mediator of Resistance to Radiation in Non–Small Cell Lung Cancer

Author

Daniel B. Longley, Kevin M. Prise, Karl T. Butterworth, Gerard G. Hanna, Timothy Harrison, Patrick G. Johnston, Caitriona Holohan, Nyree Crawford, Catherine Higgins, Joanna Majkut, Catherine Fenning, Izabela Stasik, Luke Humphreys, Conor A. Bradley, Zsuzsanna Nemeth, and Kylie A. McLaughlin

Abstract

Combination of SAHA with IR in H460 and A549 cells using different treatment schedules

Published
2023

7. Exploring a Link Between Alzheimer’s and Glioma by Investigating SORL1 Network

Author

Kristy Montalbo, Emyr Bakker, Izabela Stasik, and Christopher Smith

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

AIMS Use bioinformatics methods to identify and validate associated proteins and genes in the SORL1 network. Generate a bank of patient derived cells in association with the Royal Preston Hospital BTNW tissue bank. Explore identified targets from the bioinformatics in patient derived cells. METHOD Proteins and genes associated with SORL1 and SORLA were identified on GeneCards. Connectivity mapping of known and predicted interactions linked to SORL1 was explored in STRING. For clinical validation differential expression was investigated by comparing genomic data from GTEX and TCGA, available at Xenabrowser. For survival analysis Kaplan-Meier curves were generated on cBioPortal. The five most differently expressed novel targets are taken forward for laboratory experiments using western blots for protein quantification and immunocytochemistry to identify and visualise target proteins. RESULTS A total of 73 genes (30 from GeneCards and 43 from STRING) were obtained. 63 genes from the generated SORL1-related network were shown to be differentially expressed whilst 40 were significantly different between low-surviving patients and high-surviving patients. The top five associated proteins are CKAP4, CTNND1, FN1, HSPA12A and SORCS3. CKAP4, CTNND1 and FN1 are highly expressed in both glioma and glioblastoma, but low expressed in healthy tissue. HSPA12A is low expressed in cancerous brain tissue and highly expressed in healthy samples. SORCS3 is differentially expressed in healthy samples and glioma, but significantly low expressed glioblastoma. CONCLUSION This project provides insight into SORL1 molecular relationships and function in tissue, cultured cells and serum from a patient cohort including demographics, disease progression and site.

Published
2022

8. Computer-aided Design of Novel CDK5 Inhibitors; Towards New Treatments of Glioblastoma

Author

Zahra Khan, Izabela Stasik, and Joseph Hayes

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

AIMS Design and statistically optimize an in silico screening protocol; apply the screening protocol to a compound database; in vitro validation of selected inhibitors (isolated CDK5 enzyme binding assay). METHOD Two large compound databases, ZINC15 and Analyticon Discovery, were used to screen for potential CDK5 ATP-binding site inhibitors. They were first filtered using a generated pharmacophore model and then virtually screened using Glide SP docking with a solved CDK5-p25 structure (PDB: 3O0G). The selected candidates were validated using enzyme binding assays to determine their inhibitory activity on CDK5, as well as against a panel of kinases. RESULTS Over 17,000 compounds were screened during molecular docking studies and of these, ~11,600 compounds returned which are predicted to bind to CDK5. The top 10% of docked compounds were analysed and 30 candidates were selected for single concentration screening at 50 µM concentrations. The 9 most potent compounds were selected for IC50 determinations and revealed 6 compounds with IC50 CONCLUSION Low micromolar potent compounds have been identified through in silico screening and validated in using in vitro binding assays. One flavonoid compound in particular, cirsiliol (IC50 = 5.90 µM), displayed best selectivity towards CDK5, a challenge in kinase inhibitor design. The identified compounds will now pass to cellular studies to determine their effect on Glioblastoma cell lines.

Published
2022

9. Brain Tumour Lessons From Alzheimer’s Disease: Beta-Amyloid and SorLA Expression in Glioblastoma

Author

Lydia Jones, Vicky Jones, Lisa Shaw, Izabela Stasik, and Christopher Smith

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

AIMS Exploring how two proteins strongly associated with Alzheimer’s disease are expressed in glioma. Amyloid beta (Aβ) is a peptide cleaved from amyloid precursor protein (APP) that is shuttled around the cell by sorting-related receptor with A-type repeats (SorLA). Low expression of SorLA has been linked to increased risk of Alzheimer’s disease as APP processing shifts towards production of the plaque-forming Aβ42 rather than the more benign Aβ40. METHOD Expression of Aβ40, Aβ42 and SorLA was determined in immortalised cell lines (grade 4 glioblastoma U87MG, grade 2 astrocytoma 1321N1, foetal astrocytes SVGp12), glioblastoma patient-derived cells (PD301, PD304) and normal human astrocytes through western blotting or immunocytochemistry. RESULTS SorLA was present in all cells. Relative optical density was more than 60-fold higher for U87MG glioblastoma cells and approximately 10-fold higher for 1321N1 astrocytoma cells than SVGp12 cells. Similarly, SorLA had a significantly higher expression (p CONCLUSION These data suggest that SorLA is retained in glioblastoma and remains functional to drive APP processing away from Aβ42 production. Future work will determine how high SorLA expression contributes to the increased motility and invasiveness seen in glioblastoma cells by transfecting siRNA to knock down SorLA.

Published
2022

10. FLIP: A Targetable Mediator of Resistance to Radiation in Non-Small Cell Lung Cancer

Author

Zsuzsanna Németh, Izabela Stasik, Catherine Fenning, Kevin M. Prise, Conor A Bradley, Kylie A. McLaughlin, Gerard G Hanna, Joanna Majkut, Catherine A. Higgins, Caitriona Holohan, Nyree Crawford, Luke M Humphreys, Patrick G. Johnston, Karl T. Butterworth, Tim Harrison, and Daniel B. Longley

Subjects
0301 basic medicine, Cancer Research, Programmed cell death, Lung Neoplasms, CASP8 and FADD-Like Apoptosis Regulating Protein, Antineoplastic Agents, Apoptosis, Radiation Tolerance, 03 medical and health sciences, chemistry.chemical_compound, SDG 3 - Good Health and Well-being, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Humans, FADD, RNA, Small Interfering, Vorinostat, biology, Entinostat, B131, A100, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Histone Deacetylase Inhibitors, 030104 developmental biology, Oncology, chemistry, Flip, Cancer cell, biology.protein, RNA Interference, Signal transduction, Signal Transduction, medicine.drug
Abstract

Resistance to radiotherapy due to insufficient cancer cell death is a significant cause of treatment failure in non–small cell lung cancer (NSCLC). The endogenous caspase-8 inhibitor FLIP is a critical regulator of cell death that is frequently overexpressed in NSCLC and is an established inhibitor of apoptotic cell death induced via the extrinsic death receptor pathway. Apoptosis induced by ionizing radiation (IR) has been considered to be mediated predominantly via the intrinsic apoptotic pathway; however, we found that IR-induced apoptosis was significantly attenuated in NSCLC cells when caspase-8 was depleted using RNA interference (RNAi), suggesting involvement of the extrinsic apoptosis pathway. Moreover, overexpression of wild-type FLIP, but not a mutant form that cannot bind the critical death receptor adaptor protein FADD, also attenuated IR-induced apoptosis, confirming the importance of the extrinsic apoptotic pathway as a determinant of response to IR in NSCLC. Importantly, when FLIP protein levels were downregulated by RNAi, IR-induced cell death was significantly enhanced. The clinically relevant histone deacetylase (HDAC) inhibitors vorinostat and entinostat were subsequently found to sensitize a subset of NSCLC cell lines to IR in a manner that was dependent on their ability to suppress FLIP expression and promote activation of caspase-8. Entinostat also enhanced the antitumor activity of IR in vivo. Therefore, FLIP downregulation induced by HDAC inhibitors is a potential clinical strategy to radiosensitize NSCLC and thereby improve response to radiotherapy. Overall, this study provides the first evidence that pharmacological inhibition of FLIP may improve response of NCSLC to IR. Mol Cancer Ther; 15(10); 2432–41. ©2016 AACR.

Published
2016

11. Identification of an acetylation-dependant Ku70/FLIP complex that regulates FLIP expression and HDAC inhibitor-induced apoptosis

Author

David Haigh, Miriam Sgobba, Kirsty McLaughlin, Rosemary O'Connor, Emma M. Kerr, Cathy Fenning, Joel S. Riley, P.G. Johnston, Izabela Stasik, Daniel B. Longley, Joanna Majkut, Keara Redmond, Caitriona Holohan, Sharron Dolan, Patrick A. Kiely, M. Crudden, Kirsty M. McLaughlin, and S. Van Schaeybroeck

Subjects
CASP8 and FADD-Like Apoptosis Regulating Protein, Down-Regulation, Apoptosis, Biology, Histone Deacetylase 6, Hydroxamic Acids, Transfection, Caspase 8, Histone Deacetylases, Mice, Ubiquitin, medicine, Animals, Humans, Amino Acid Sequence, RNA, Small Interfering, Ku Autoantigen, Molecular Biology, Vorinostat, Original Paper, Mice, Inbred BALB C, Acetylation, Antigens, Nuclear, Cell Biology, HDAC6, HCT116 Cells, DNA-Binding Proteins, Histone Deacetylase Inhibitors, Proteasome, Flip, Cancer research, biology.protein, Female, Histone deacetylase, HT29 Cells, Protein Processing, Post-Translational, medicine.drug
Abstract

FLIP is a potential anti-cancer therapeutic target that inhibits apoptosis by blocking caspase 8 activation by death receptors. We report a novel interaction between FLIP and the DNA repair protein Ku70 that regulates FLIP protein stability by inhibiting its polyubiquitination. Furthermore, we found that the histone deacetylase (HDAC) inhibitor Vorinostat (SAHA) enhances the acetylation of Ku70, thereby disrupting the FLIP/Ku70 complex and triggering FLIP polyubiquitination and degradation by the proteasome. Using in vitro and in vivo colorectal cancer models, we further demonstrated that SAHA-induced apoptosis is dependant on FLIP downregulation and caspase 8 activation. In addition, an HDAC6-specific inhibitor Tubacin recapitulated the effects of SAHA, suggesting that HDAC6 is a key regulator of Ku70 acetylation and FLIP protein stability. Thus, HDAC inhibitors with anti-HDAC6 activity act as efficient post-transcriptional suppressors of FLIP expression and may, therefore, effectively act as 'FLIP inhibitors'.

Published
2012

12. Differential affinity of FLIP and procaspase 8 for FADD’s DED binding surfaces regulates DISC assembly

Author

Daniel B. Longley, M. Sgobba, Keara Redmond, Joel S. Riley, Joanna Majkut, Caitriona Holohan, Dean A. Fennell, Shozeb Haider, David Haigh, Patrick G. Johnston, S. Van Schaeybroeck, Andrew Logan, Izabela Stasik, Nyree Crawford, Emma M. Kerr, and Catherine A. Higgins

Subjects
Immunoprecipitation, FLIP, Fas-Associated Death Domain Protein, C130, Blotting, Western, CASP8 and FADD-Like Apoptosis Regulating Protein, General Physics and Astronomy, Plasma protein binding, Caspase 8, General Biochemistry, Genetics and Molecular Biology, Article, Humans, FADD, DR5, Receptor, Multidisciplinary, biology, C760, apoptosis, General Chemistry, DISC, HCT116 Cells, C700, Cell biology, Blot, Flip, biology.protein, Chromatography, Gel, Death effector domain, Protein Binding
Abstract

Death receptor activation triggers recruitment of FADD, which via its death effector domain (DED) engages the DEDs of procaspase 8 and its inhibitor FLIP to form death-inducing signalling complexes (DISCs). The DEDs of FADD, FLIP and procaspase 8 interact with one another using two binding surfaces defined by α1/α4 and α2/α5 helices, respectively. Here we report that FLIP has preferential affinity for the α1/α4 surface of FADD, whereas procaspase 8 has preferential affinity for FADD's α2/α5 surface. These relative affinities contribute to FLIP being recruited to the DISC at comparable levels to procaspase 8 despite lower cellular expression. Additional studies, including assessment of DISC stoichiometry and functional assays, suggest that following death receptor recruitment, the FADD DED preferentially engages FLIP using its α1/α4 surface and procaspase 8 using its α2/α5 surface; these tripartite intermediates then interact via the α1/α4 surface of FLIP DED1 and the α2/α5 surface of procaspase 8 DED2.

Published
2014

13. Prognostic and therapeutic relevance of FLIP and procaspase-8 overexpression in non-small cell lung cancer

Author

Joel S. Riley, Ryan Hutchinson, Nyree Crawford, Manuel Salto-Tellez, Caitriona Holohan, Kenneth J. O'Byrne, Darragh G. McArt, Patrick G. Johnston, Ian M. Paul, Elaine W. Kay, Daniel B. Longley, Kathy Gately, Robert Cummins, Dean A. Fennell, Peter W. Hamilton, S. Van Schaeybroeck, and Izabela Stasik

Subjects
Cancer Research, C131, Cell Survival, FLIP, Blotting, Western, Immunology, Cell, CASP8 and FADD-Like Apoptosis Regulating Protein, TRAIL, In Vitro Techniques, Biology, Caspase 8, Q1, caspase-8, Cellular and Molecular Neuroscience, chemistry.chemical_compound, SDG 3 - Good Health and Well-being, HDAC inhibitor, Carcinoma, Non-Small-Cell Lung, medicine, Humans, Lung cancer, non-small cell lung cancer, Retrospective Studies, Cisplatin, Entinostat, B131, B132, A100, Cell Biology, Flow Cytometry, medicine.disease, Molecular biology, respiratory tract diseases, medicine.anatomical_structure, chemistry, Flip, Cell culture, Apoptosis, Cancer research, Original Article, medicine.drug
Abstract

Non-small cell lung carcinoma remains by far the leading cause of cancer-related deaths worldwide. Overexpression of FLIP, which blocks the extrinsic apoptotic pathway by inhibiting caspase-8 activation, has been identified in various cancers. We investigated FLIP and procaspase-8 expression in NSCLC and the effect of HDAC inhibitors on FLIP expression, activation of caspase-8 and drug resistance in NSCLC and normal lung cell line models. Immunohistochemical analysis of cytoplasmic and nuclear FLIP and procaspase-8 protein expression was carried out using a novel digital pathology approach. Both FLIP and procaspase-8 were found to be significantly overexpressed in tumours, and importantly, high cytoplasmic expression of FLIP significantly correlated with shorter overall survival. Treatment with HDAC inhibitors targeting HDAC1-3 downregulated FLIP expression predominantly via post-transcriptional mechanisms, and this resulted in death receptor- and caspase-8-dependent apoptosis in NSCLC cells, but not normal lung cells. In addition, HDAC inhibitors synergized with TRAIL and cisplatin in NSCLC cells in a FLIP- and caspase-8-dependent manner. Thus, FLIP and procaspase-8 are overexpressed in NSCLC, and high cytoplasmic FLIP expression is indicative of poor prognosis. Targeting high FLIP expression using HDAC1-3 selective inhibitors such as entinostat to exploit high procaspase-8 expression in NSCLC has promising therapeutic potential, particularly when used in combination with TRAIL receptor-targeted agents.

Published
2013

14. Acquired differential regulation of caspase-8 in cisplatin-resistant non-small-cell lung cancer

Author

N. McTavish, B. Wilson, Daniel B. Longley, Sara Busacca, Dean A. Fennell, Francis McCoy, Ian M. Paul, Martin P. Barr, Izabela Stasik, Nyree Crawford, Alex Chacko, and Kenneth J. O'Byrne

Subjects
Cancer Research, Lung Neoplasms, C131, Immunology, Apoptosis, B200, Biology, Caspase 8, Gene Expression Regulation, Enzymologic, caspase-8, Cellular and Molecular Neuroscience, SDG 3 - Good Health and Well-being, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Humans, Receptor, Lung cancer, Death domain, Cisplatin, B131, BAK, A100, Cell Biology, Fas receptor, medicine.disease, Cell biology, Gene Expression Regulation, Neoplastic, non-small-cell lung cancer, Drug Resistance, Neoplasm, BAX, Cancer research, Original Article, cisplatin resistance, Acid sphingomyelinase, Protein Processing, Post-Translational, medicine.drug
Abstract

Failure to efficiently induce apoptosis contributes to cisplatin resistance in non-small-cell lung cancer (NSCLC). Although BCL-2-associated X protein (BAX) and BCL-2 antagonist killer (BAK) are critical regulators of the mitochondrial apoptosis pathway, their requirement has not been robustly established in relation to cisplatin. Here, we show that cisplatin can efficiently bypass mitochondrial apoptosis block caused by loss of BAX and BAK, via activation of the extrinsic death receptor pathway in some model cell lines. Apoptosis resistance following cisplatin can only be observed when both extrinsic and intrinsic pathways are blocked, consistent with redundancy between mitochondrial and death receptor pathways in cisplatin-induced apoptosis. In H460 NSCLC cells, caspase-8 cleavage was shown to be induced by cisplatin and is dependent on death receptor 4, death receptor 5, Fas-associated protein with death domain, acid sphingomyelinase and ceramide synthesis. In contrast, cisplatin-resistant cells fail to activate caspase-8 via this pathway despite conserving sensitivity to death ligand-driven activation. Accordingly, caspase-8 activation block acquired during cisplatin resistance, can be bypassed by death receptor agonism.

Published
2012

15. Attenuation of Soft-Tissue Sarcomas Resistance to the Cytotoxic Action of TNF-α by Restoring p53 Function

Author

Izabela Stasik, Jerome Thiery, A. Lecesne, Philippe Vielh, Jane Muret, Véronique Baud, Ludovic Lacroix, Sylvie Bonvalot, Katy Billot, Arash Nanbakhsh, Joelle Wiels, Philippe Terrier, Abdelali Jalil, Salem Chouaib, Lyubomir T. Vassilev, Meriem Hasmim, and Aude Mallavialle

Subjects
Melphalan, C131, Cancer Treatment, Gene Expression, B200, Apoptosis, Biochemistry, Molecular Cell Biology, Bone and Soft Tissue Sarcomas, Cytotoxic T cell, Multidisciplinary, medicine.diagnostic_test, Cell Death, B131, Soft tissue, Sarcoma, Signaling in Selected Disciplines, Flow Cytometry, Oncology, Medicine, Tumor necrosis factor alpha, Oncology Agents, medicine.drug, Research Article, Signal Transduction, Programmed cell death, Science, Blotting, Western, Biology, Real-Time Polymerase Chain Reaction, Flow cytometry, Cell Line, Tumor, Chemical Biology, medicine, In Situ Nick-End Labeling, Humans, neoplasms, Oncogenic Signaling, Tumor Necrosis Factor-alpha, Cancers and Neoplasms, A100, A300, medicine.disease, Genes, p53, Small Molecules, Mutation, Cancer research
Abstract

BACKGROUND:\ud Isolated limb perfusion with TNF-α and melphalan is used with remarkable efficiency to treat unresectable limb sarcomas. Here we tested the ability of TNF-α to directly induce apoptosis of sarcoma cells. In addition, we investigated the impact of p53 in the regulation of such effect.\ud \ud METHODOLOGY/PRINCIPAL FINDINGS:\ud We first analysed the ability of TNF-α to induce apoptosis in freshly isolated tumour cells. For this purpose, sarcoma tumours (n = 8) treated ex vivo with TNF-α were processed for TUNEL staining. It revealed substantial endothelial cell apoptosis and levels of tumour cell apoptosis that varied from low to high. In order to investigate the role of p53 in TNF-α-induced cell death, human sarcoma cell lines (n = 9) with different TP53 and MDM2 status were studied for their sensitivity to TNF-α. TP53(Wt) cell lines were sensitive to TNF-α unless MDM2 was over-expressed. However, TP53(Mut) and TP53(Null) cell lines were resistant. TP53 suppression in TP53(Wt) cell lines abrogated TNF-α sensitivity and TP53 overexpression in TP53(Null) cell lines restored it. The use of small molecules that restore p53 activity, such as CP-31398 or Nutlin-3a, in association with TNF-α, potentiated the cell death of respectively TP53(Mut) and TP53(Wt)/MDM2(Ampl). In particular, CP-31398 was able to induce p53 as well as some of its apoptotic target genes in TP53(Mut) cells. In TP53(Wt)/MDM2(Ampl) cells, Nutlin-3a effects were associated with a decrease of TNF-α-induced NF-κB-DNA binding and correlated with a differential regulation of pro- and anti-apoptotic genes such as TP53BP2, GADD45, TGF-β1 and FAIM.\ud \ud CONCLUSION/SIGNIFICANCE:\ud More effective therapeutic approaches are critically needed for the treatment of unresectable limb sarcomas. Our results show that restoring p53 activity in sarcoma cells correlated with increased sensitivity to TNF-α, suggesting that this strategy may be an important determinant of TNF-α-based sarcomas treatment.

Published
2012

16. Vorinostat/SAHA-induced apoptosis in malignant mesothelioma is FLIP/caspase 8-dependent and HR23B-independent

Author

Caitriona Holohan, Steven G. Gray, Izabela Stasik, Jane L. Hurwitz, V. Courtney Broaddus, Daniel B. Longley, Sara Busacca, Kenneth J. O'Byrne, Emma M. Kerr, Kelly M. Redmond, Dario Barbone, Dean A. Fennell, Patrick G. Johnston, and Kirsty M. McLaughlin

Subjects
Male, Mesothelioma, Cancer Research, Programmed cell death, Pleural Neoplasms, CASP8 and FADD-Like Apoptosis Regulating Protein, Apoptosis, Caspase 8, Hydroxamic Acids, Cell Line, Tumor, Spheroids, Cellular, medicine, Humans, Clonogenic assay, Vorinostat, Caspase, Cisplatin, biology, Molecular biology, Caspase Inhibitors, DNA-Binding Proteins, Histone Deacetylase Inhibitors, DNA Repair Enzymes, Oncology, Flip, Cancer research, biology.protein, RNA Interference, Apoptosis Regulatory Proteins, medicine.drug
Abstract

Introduction Malignant pleural mesothelioma (MPM) is a rapidly fatal malignancy that is increasing in incidence. The caspase 8 inhibitor FLIP is an anti-apoptotic protein over-expressed in several cancer types including MPM. The histone deacetylase (HDAC) inhibitor Vorinostat (SAHA) is currently being evaluated in relapsed mesothelioma. We examined the roles of FLIP and caspase 8 in regulating SAHA-induced apoptosis in MPM. Methods The mechanism of SAHA-induced apoptosis was assessed in 7 MPM cell lines and in a multicellular spheroid model. SiRNA and overexpression approaches were used, and cell death was assessed by flow cytometry, Western blotting and clonogenic assays. Results RNAi-mediated FLIP silencing resulted in caspase 8-dependent apoptosis in MPM cell line models. SAHA potently down-regulated FLIP protein expression in all 7 MPM cell lines and in a multicellular spheroid model of MPM. In 6/7 MPM cell lines, SAHA treatment resulted in significant levels of apoptosis induction. Moreover, this apoptosis was caspase 8-dependent in all six sensitive cell lines. SAHA-induced apoptosis was also inhibited by stable FLIP overexpression. In contrast, down-regulation of HR23B, a candidate predictive biomarker for HDAC inhibitors, significantly inhibited SAHA-induced apoptosis in only 1/6 SAHA-sensitive MPM cell lines. Analysis of MPM patient samples demonstrated significant inter-patient variations in FLIP and caspase 8 expressions. In addition, SAHA enhanced cisplatin-induced apoptosis in a FLIP-dependent manner. Conclusions These results indicate that FLIP is a major target for SAHA in MPM and identifies FLIP, caspase 8 and associated signalling molecules as candidate biomarkers for SAHA in this disease.

Published
2011

17. Cytokeratin 18 expression pattern correlates with renal cell carcinoma progression: Relationship with Snail

Author

Mohamed Chebil, Izabela Stasik, Sarra Ben Jilani, Asma Gati, Amine Derouiche, Amel Benammar Elgaaied, Nadia Kourda, Intissar Akalay, Anne Caignard, Salem Chouaib, Bruno Azzarone, Yosra Messai, Muhammad Zaeem Noman, and Meriem Hasmim

Subjects
Male, Cancer Research, Pathology, medicine.medical_specialty, Biology, urologic and male genital diseases, Cytokeratin, Renal cell carcinoma, Cell Line, Tumor, medicine, Carcinoma, Humans, Carcinoma, Renal Cell, Keratin-18, Gene Expression Profiling, B130, Cancer, Cell cycle, medicine.disease, Immunohistochemistry, Kidney Neoplasms, Fibronectins, Gene Expression Regulation, Neoplastic, Phenotype, Real-time polymerase chain reaction, Oncology, Tumor progression, Disease Progression, Female, Collagen, Snail Family Transcription Factors, Kidney cancer, Transcription Factors
Abstract

Renal cell carcinoma (RCC) is the most common type of kidney cancer and recent developments in the molecular biology of RCC have identified multiple pathways associated with the development of this cancer. This study aimed at analyzing the expression pattern of cytokeratin 18 (CK18) in RCC patients and its prognostic relevance. We quantified CK18 mRNA expression and protein using real-time reverse transcription quantitative polymerase chain reaction (RT-QPCR) and immunohistochemistry, respectively, in paired tumor and non-tumor samples from 42 patients. Our data indicate that CK18 mRNA and proteins levels increased with advanced stage and grade of the disease. Using primary (RCC5) and metastatic renal cell carcinoma (RCC5 met) cell lines, we demonstrated that CK18 expression was 5-fold higher in the metastatic as compared to the primary RCC cell line and correlated with a migratory phenotype characterized by a distinct elongated morphology as revealed by Phalloidin staining. In addition, RCC5 met cells displayed an increased capacity to attach to fibronectin and collagen which was lost following CK18 knock-down. Our data also indicate that the expression of CK18 was associated with increased Snail expression which correlated positively with advanced disease in RCC patients. The present findings suggest that CK18 may play an important role in the progression of RCC and it may be used as a new predictor for RCC.

Published
2010

18. The mitochondrial localization of RelB and NFATx in immature T cells

Author

Ewa Ziolo, Andrzej Rapak, Izabela Stasik, and Leon Strządała

Subjects
Lymphoma, T-Lymphocytes, Short Communication, T cell, FK506, Cell, Thymic lymphoma, Mice, Transgenic, Thymus Gland, RelB, Mitochondrion, CREB, Biochemistry, Tacrolimus, Cell Line, Mice, Transcription factors, medicine, Animals, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Transcription factor, NFATx, Thymocytes, Ionophores, NFATC Transcription Factors, biology, Ionomycin, RELB, Transcription Factor RelB, NF-kappa B p50 Subunit, Cell Biology, Mitochondrial translocation, Mitochondria, Cell biology, Thymocyte, medicine.anatomical_structure, Cytoplasm, biology.protein, Immunosuppressive Agents
Abstract

In order to exert their activity, transcription factors must be transported to the nucleus. Certain transcription factors have also been found on mitochondria. Here, the localization of RelB and NFATx in the mitochondrial fractions of normal thymocytes and thymic lymphoma cells is shown for the first time. CREB was only found in the nucleus, while p50 (NFκB) was found in both the nucleus and the cytoplasm, but outside the mitochondria. The translocation of transcription factors to the mitochondria is differentially regulated. Unlike RelB, which is always present in the mitochondrial fraction, NFATx appeared on the mitochondria in cells treated with ionomycin together with an immunosuppressant and inhibitor of calcineurin (FK506). This data reveals that the mitochondrial localization of some transcription factors is precisely controlled by a calcium signal sensitive to FK506 in T cells.

Published
2008

19. OR42 Potential mediation of HLA and cancer associations via non-coding RNAs

Author

Izabela Stasik, Ken I. Mills, and Mehmet Tevfik Dorak

Subjects
Genetics, Immunology, Single-nucleotide polymorphism, Genome-wide association study, General Medicine, Human leukocyte antigen, Biology, Genome, Molecular biology, Genetic variation, Immunology and Allergy, Gene, Chromosome 22, HLA Complex
Abstract

The HLA complex is the most gene dense and polymorphic part of the genome which also contains the strongest trans-eQTLs in the genome. We noted the presence of multiple trans-eQTLs for the DNA repair gene XRCC6 ( P −9 ) across the HLA region from 29.5 MB to 32.5 MB (chromosome 6) despite the absence of any cis-eQTL for XRCC6 in its vicinity in chromosome 22. Other than the HLA-linked ones, there is no trans-eQTL for XRCC6 in the genome. Having observed highly significant (P40) mapped to 26 genes including two uncharacterized and four non-coding RNA (ncRNA) genes (HCG9 & 22, lincRNA243 & 1149) in the HLA region. Many also act as cis-eQTLs for local genes, and most of the strongest ( P ; −8 ) cis-eQTLs map to HLA-region ncRNA genes. Their local target genes include an uncharacterized intergenic region 5′ upstream of HLA-B ( n = 6), the ncRNA gene HCG22 ( n = 4) and HLA-C ( n = 1). Examination of the ImmunoChip results on IHWG cell lines did not suggest a common lineage or linkage to an HLA haplotype for these SNPs. Screening of GWAS catalog and dbGAP for associations of the 42 trans-eQTLs with cancer risk revealed existing associations with lung (rs3117582, rs2395185), breast (rs3130544) and liver (rs9275572) cancer, Hodgkin (rs2395185) and non-Hodgkin (rs2647012; rs6457327) lymphoma, and another SNP (rs2596503) has a reported association with glioblastoma. The examination of the Microarray Innovations in Leukemia (MILE) data revealed highly significant inverse correlations between HCG22 and XRCC6 expression levels both in normal bone marrow ( P = 0.0001, r = -0.43, n = 74) and leukemia samples ( P r = −0.27, n = 2022). HCG22 levels also showed an equally strong inverse correlation with TP53 expression. It appears that HLA region genetic variation correlates with expression of HCG22, which in turn inversely correlates with XRCC6 and TP53 levels. The overall observations suggest a non-immunological mechanism for the involvement of HLA region genetic variation in inherited cancer susceptibility, and implicate an ncRNA-mediated mechanism for trans-eQTL effect on XRCC6.

Published
2015

20. SAHA overcomes FLIP-mediated inhibition of SMAC mimetic-induced apoptosis in mesothelioma

Author

Nyree Crawford, David Waugh, Daniel B. Longley, George Ward, Izabela Stasik, Gianni Chessari, Patrick G. Johnston, Dean A. Fennell, Joanna Majkut, Caitriona Holohan, and Mike McGrath

Subjects
SMAC mimetics, Mesothelioma, Cancer Research, C131, CASP8 and FADD-Like Apoptosis Regulating Protein, Poly (ADP-Ribose) Polymerase-1, Hydroxamic Acids, Inhibitor of Apoptosis Proteins, HDAC inhibitors, B290, Caspase 8, Vorinostat, Caspase 3, B131, Histone deacetylase inhibitor, Drug Synergism, mesothelioma, Receptor-Interacting Protein Serine-Threonine Kinases, Original Article, Poly(ADP-ribose) Polymerases, medicine.drug, Programmed cell death, FLIP, medicine.drug_class, Pleural Neoplasms, Immunology, Down-Regulation, Antineoplastic Agents, Biology, Cellular and Molecular Neuroscience, SDG 3 - Good Health and Well-being, Cell Line, Tumor, medicine, Humans, Tumor microenvironment, Molecular Mimicry, A100, Cell Biology, SAHA/Vorinostat, Enzyme Activation, Histone Deacetylase Inhibitors, Drug Resistance, Neoplasm, Apoptosis, Flip, Cancer research, Cisplatin, Drug Screening Assays, Antitumor
Abstract

Malignant pleural mesothelioma (MPM) is a highly pro-inflammatory malignancy that is rapidly fatal and increasing in incidence. Cytokine signaling within the pro-inflammatory tumor microenvironment makes a critical contribution to the development of MPM and its resistance to conventional chemotherapy approaches. SMAC mimetic compounds (SMCs) are a promising class of anticancer drug that are dependent on tumor necrosis factor alpha (TNFa) signaling for their activity. As circulating TNFa expression is significantly elevated in MPM patients, we examined the sensitivity of MPM cell line models to SMCs. Surprisingly, all MPM cell lines assessed were highly resistant to SMCs either alone or when incubated in the presence of clinically relevant levels of TNFa. Further analyses revealed that MPM cells were sensitized to SMC-induced apoptosis by siRNA-mediated downregulation of the caspase 8 inhibitor FLIP, an antiapoptotic protein overexpressed in several cancer types including MPM. We have previously reported that FLIP expression is potently downregulated in MPM cells in response to the histone deacetylase inhibitor (HDACi) Vorinostat (SAHA). In this study, we demonstrate that SAHA sensitizes MPM cells to SMCs in a manner dependent on its ability to downregulate FLIP. Although treatment with SMC in the presence of TNFa promoted interaction between caspase 8 and the necrosis-promoting RIPK1, the cell death induced by combined treatment with SAHA and SMC was apoptotic and mediated by caspase 8. These results indicate that FLIP is a major inhibitor of SMC-mediated apoptosis in MPM, but that this inhibition can be overcome by the HDACi SAHA.

Published
2013

22. 842 FLIP as a Critical Target for Vorinostat in Mesothelioma

Author

Jane L. Hurwitz, Dario Barbone, Daniel B. Longley, V.C. Broaddus, Dean A. Fennell, Steven G. Gray, Kenneth J. O'Byrne, and Izabela Stasik

Subjects
Cancer Research, Oncology, Flip, business.industry, Cancer research, medicine, Mesothelioma, medicine.disease, business, Vorinostat, medicine.drug
Published
2012

23. Abstract 1041: Restoration of p53 function in soft tissue sarcomas correlates with increased sensitivity to TNFα

Author

A. Lecesne, Sylvie Bonvalot, Philippe Terrier, Izabela Stasik, Jane Muret, Salem Chouaib, and Abdelali Jalil

Subjects
Cancer Research, Pathology, medicine.medical_specialty, Soft tissue sarcoma, Nutlin, Biology, medicine.disease, chemistry.chemical_compound, Oncology, chemistry, Apoptosis, Cell culture, medicine, Cancer research, Cytotoxic T cell, Tumor necrosis factor alpha, Sarcoma, Ex vivo
Abstract

Background: Sarcomas are rare, poorly understood cancers, highly aggressive and refractory to standard therapies. In these tumors mutations of p53 or Mdm2 amplification are frequently found. Isolated limb perfusion (ILP) with TNFα and melphalan is an innovative approach to treat unresectable soft tissue sarcomas (STS) of extremities. TNF is known to increase endothelium permeability for melphalan, and to disrupt tumoral vessels. However, the direct apoptotic effect of TNF on sarcoma cells remains controversial. Several reports indicate an association of sensitivity to TNF with p53 activity in in vitro models. In the present study we attempted to test the ability of TNF to induce apoptosis of sarcoma cells and investigated the role of p53 in the regulation of this effect. Methods: Ex vivo study was performed on sarcoma tumor pieces from patients. Tumor slices were treated with TNF and cytotoxic effect was assessed with TUNEL method. In vitro studies were carried on human soft tissue sarcoma cell lines with different p53 status and Mdm2 expression, representing 5 histological types. Cytotoxic effect of TNF was assessed with DiOC6/PI test. Activation of p53 was verified by the detection of expression of proteins encoded by p53 target genes. Expression of TNF receptor was examined by flow cytometry. Results: In tumor slices treated ex vivo with TNF we observed apoptosis of not only endothelial, but also sarcoma cells. In vitro studies revealed that cell lines with active p53 were sensitive to TNF (80% and 40% of apoptosis), while 6 cell lines were resistant: 2 with wt p53 and Mdm2 amplification (2-4% of apoptosis), 2 with p53 mutation and 2 with p53 deletion (5-15% of apoptosis). TNFR I was expressed by all the cell lines. We next tested sensitivity to TNF after restoration of p53 activity. For this purpose we used either of two compounds: Nutlin-3a, an inhibitor of Mdm2, or CP-31398, a molecule restoring wild-type conformation to mutant TP53. In cell lines with Mdm2 amplification treatment with Nutlin alone resulted in decreased cell viability, while in combined treatment induced strong apoptosis synergistically with TNF. Similarly, treatment of cell lines expressing mutated p53 with CP-31398 led to a significant enhancement of sensitivity to TNF. Conclusions: The results of our ex vivo and in vitro studies suggest, that during ILP, TNF may directly kill sarcoma cells and its cytotoxic activity is correlated with the functionality of p53. Restoration of p53 activity may be advantageous not only in therapies based on DNA disruption, but also based on the use of TNFα. Note: This abstract was not presented at the AACR 101st Annual Meeting 2010 because the presenter was unable to attend. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 101st Annual Meeting of the American Association for Cancer Research; 2010 Apr 17-21; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2010;70(8 Suppl):Abstract nr 1041.

Published
2010

24. Ionomycin-induced apoptosis of thymocytes is independent of Nur77 NBRE or NurRE binding, but is accompanied by Nur77 mitochondrial targeting

Author

Andrzej Rapak, Wojciech Kałas, Ewa Ziolo, Leon Strzadala, and Izabela Stasik

Subjects
Receptors, Steroid, Nerve growth factor IB, Receptors, Cytoplasmic and Nuclear, Endogeny, Apoptosis, Thymus Gland, Biology, Mitochondrion, Response Elements, Tacrolimus, Clonal deletion, Mice, Transactivation, chemistry.chemical_compound, DNA-binding, Nur77, Nuclear Receptor Subfamily 4, Group A, Member 2, Nuclear Receptor Subfamily 4, Group A, Member 1, Animals, Molecular Biology, Cells, Cultured, Thymocytes, Ionophores, Ionomycin, Cytochrome c, Cytochromes c, Cell Biology, Molecular biology, Mitochondrial translocation, Mitochondria, Cell biology, DNA-Binding Proteins, Mice, Inbred C57BL, chemistry, biology.protein, Immunosuppressive Agents, Protein Binding, Transcription Factors
Abstract

The induction of thymocyte apoptosis through the Nur77-mediated intrinsic pathway can be of physiological importance in the clonal deletion of autoreactive thymocytes during negative selection in the thymus and/or in thymocytes undergoing oncogenic transformation. Ionomycin treatment induces endogenous Nur77 expression as well as apoptosis and cytochrome c release in thymocytes. Here it is shown for the first time that in normal thymocytes undergoing apoptosis, ionomycin induces translocation of endogenous Nur77 not only to the nucleus, but also to mitochondria. Immunosuppressant FK506 inhibits Nur77 NBRE and NurRE binding activity but has no effect on thymocytes apoptosis, the subcellular localization of Nur77, or cytochrome c release. This indicates that thymocytes can undergo apoptosis through the intrinsic Nur77-mediated mitochondrial pathway and that the transactivation activity of Nur77 monomers or dimers is not necessary for thymocyte apoptosis.

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