Your search keyword '"Stahel, Rolf A."' showing total 95 results

1. Clinical Case Presentation and Discussion During ESO-ESMO Masterclass: a 10-Year Interactive Educational Experience.

Author

Pavlidis, Nicholas, Peccatori, Fedro A, Aapro, Matti, Cervantes, Andreas, Stahel, Rolf, Eniu, Alex, Cavalli, Franco, and Costa, Alberto

Abstract

In this article, we report on the clinical case presentations that have been delivered during the ESO or ESO-ESMO Masterclasses in Clinical Oncology in the last 10 years. Masterclasses have been held in three different geographical continents including Europe, Middle East, and Latin America, in which participants had to submit a clinical case and present it either in front of a tumor board (multidisciplinary-like sessions) or in small groups. Clinical case presentation is a unique part of the educational program preparing young oncologists to present and discuss their own patients with distinguished experts. In each Masterclass, between 40 and 55 clinical cases-depending on the number of participants-are presented. All presentations are assessed and evaluated by faculty members as well as by the rest of the participants. [ABSTRACT FROM AUTHOR]

Published

2021

2. ESO-ESMO Masterclass in Clinical Oncology: Analysis and Evaluation of the Learning Self-Assessment Test.

Author

Pavlidis, Nicholas, Peccatori, Fedro, Aapro, Matti, Eniu, Alexandru, Stahel, Rolf, Cervantes, Andres, Cavalli, Franco, and Costa, Alberto

Abstract

Masterclass in Clinical Oncology (MCO) represents the "key educational event" of European School of Oncology's (ESO) teaching program. MCO in collaboration with European Society for Medical Oncology (ESMO) is a multidisciplinary and clinical oriented educational event offered mainly to young oncologists worldwide. It provides full immersion in oncology with clinical case presentations and a Learning Self-Assessment Test (LSAT).LSAT is consisting of 45 multiple choice questions on an electronic platform referring to the material taught during the MCO. Three questions related to their topics are requested in advance from each faculty member. The major intentions of LSAT are the following: (a) the learning reflection of the massive information given during 4-5 days of intensive teaching and (b) to offer the opportunity to the participants to prepare themselves for their National Boards or for ESMO examination.In this article, we are analyzing and evaluating the results of LSAT from the ESO-ESMO Central European MCOs. We used the information of Central European MCOs for analysis due to the homogeneity of the available data. We assessed the level of participants' knowledge in relation to their oncology specialty or to their country of origin and the level of the quality of faculty teaching. [ABSTRACT FROM AUTHOR]

Published

2021

3. Progression-Free and Overall Survival for Concurrent Nivolumab With Standard Concurrent Chemoradiotherapy in Locally Advanced Stage IIIA-B NSCLC: Results From the European Thoracic Oncology Platform NICOLAS Phase II Trial (European Thoracic Oncology Platform 6-14).

Author

Peters, Solange, Felip, Enriqueta, Dafni, Urania, Tufman, Amanda, Guckenberger, Matthias, Álvarez, Ruth, Nadal, Ernest, Becker, Annemarie, Vees, Hansjörg, Pless, Miklos, Martinez-Marti, Alex, Lambrecht, Maarten, Andratschke, Nicolaus, Tsourti, Zoi, Piguet, Anne-Christine, Roschitzki-Voser, Heidi, Gasca-Ruchti, Adrian, Vansteenkiste, Johan, Stahel, Rolf A., and De Ruysscher, Dirk

Published

2021

4. The Impact on Outcome by Adding Bevacizumab to Standard Induction Chemotherapy Prior to Mesothelioma Surgery: A Retrospective Single Center Analysis.

Author

Lauk, Olivia, Bruestle, Karina, Neuer, Thomas, Battilana, Bianca, Nguyen, Thi Dan Linh, Frauenfelder, Thomas, Stahel, Rolf, Weder, Walter, Curioni-Fontecedro, Alessandra, and Opitz, Isabelle

Subjects

BEVACIZUMAB, ENDOTHELIAL growth factors, BLOOD products, MESOTHELIOMA, PROPENSITY score matching

Abstract

Objectives: Adding bevacizumab, an anti-Vascular Endothelial Growth Factor (VEGF), to platinum-based chemotherapy/pemetrexed in 1st line treatment of advanced malignant pleural mesothelioma (MPM), significantly improved overall survival. However, increased high grade bleeding after operation was reported in patients with colorectal cancer who previously received bevacizumab. In the present analysis, we assessed for the first time the impact of adding bevacizumab to induction chemotherapy prior to surgery for mesothelioma patients. Methods: Two hundred twenty-seven MPM patients, intended to be treated with induction chemotherapy followed by surgery at the University Hospital of Zurich between 2002 and December 2018, were included in the present analysis. After propensity score matching for gender, histology and age (1:3 ratio), data from 88 patients were analyzed. Sixty-six patients underwent induction chemotherapy (with cis-/carboplatin and pemetrexed: control group) alone and 22 patients underwent induction chemotherapy with the addition of bevacizumab (bevacizumab group) prior macroscopic complete resection (MCR). Perioperative and long-term outcome variables were analyzed. Results: Patients undergoing combination treatment with bevacizumab had a significantly better response than with chemotherapy alone as assessed by modified RECIST (p=0.046). Intraoperative complications in the bevacizumab group (one patient), or in the control group (three patients) were not related to intraoperative bleeding. Postoperative transfusion of blood products occurred in a larger amount in the control group than in the bevacizumab group (p=0.047). Overall survival was not statistically different between both groups. Conclusion: These initial data demonstrate that MCR can be performed safely after triple induction chemotherapy with bevacizumab without increased intra- and postoperative bleeding complications. Response rates were significantly improved by the addition of bevacizumab. [ABSTRACT FROM AUTHOR]

Published

2020

5. Evolution and Clinical Impact of EGFR Mutations in Circulating Free DNA in the BELIEF Trial.

Author

Molina-Vila, Miguel-Angel, Stahel, Rolf A., Dafni, Urania, Jordana-Ariza, Núria, Balada-Bel, Ariadna, Garzón-Ibáñez, Mónica, García-Peláez, Beatriz, Mayo-de-las-Casas, Clara, Felip, Enriqueta, Curioni Fontecedro, Alessandra, Gautschi, Oliver, Peters, Solange, Massutí, Bartomeu, Palmero, Ramon, Ponce Aix, Santiago, Carcereny, Enric, Früh, Martin, Pless, Miklos, Popat, Sanjay, and Cuffe, Sinead

Published

2020

6. Underweight and weight loss are predictors of poor outcome in patients with brain metastasis.

Author

Lareida, Anna, Terziev, Robert, Grossenbacher, Bettina, Andratschke, Nicolaus, Roth, Patrick, Rohrmann, Sabine, Stahel, Rolf, Guckenberger, Matthias, Le Rhun, Emilie, Weller, Michael, and Wolpert, Fabian

Abstract

Purpose: Overweight may be associated with favorable outcome whereas tumor cachexia may be associated with worse outcome in patients with metastatic cancer. Here we evaluate the association of abnormal body mass index and weight change with outcome in patients with brain metastasis. Methods: Patients with a diagnosis of brain metastasis treated at the University Hospital Zurich (n = 703) were assessed for associations of body mass index, weight change, comorbidities and survival. Results: Compared with patients with normal body mass index of 18.5–24.9 kg/m2 and a median overall survival of 9 months (95% confidence interval 7.5–10.5), overall survival was inferior in patients with body mass index < 18.5 kg/m2 (overall survival 6 months, 95% confidence interval 1.6–10.3, p = 0.04), but superior in patients with body mass index > 25 kg/m2 (overall survival 13 months, 95% confidence interval 11.0–15.0; p = 0.033). We report a median relative weight loss of 5% within the first 6 months of diagnosis of brain metastasis (95% confidence interval 3.3–6.5), and reduction exceeding the median was associated with an unfavorable outcome (weight loss < 5% 22.0 months, 95% confidence interval 19.2–24.8; weight loss > 5% 14.0 months, 95% confidence interval 11.9–16.). Conclusion: High body mass index is associated with better, and underweight with worse outcome in patients with brain metastasis. Conversely, weight loss above median may predict poor outcome. Future studies need to address whether vigorous treatment of tumor cachexia, e.g. by specific nutrition management, might improve outcome of patients with brain metastasis. In contrast, regimens associated with weight loss such as ketogenic diet may be detrimental. [ABSTRACT FROM AUTHOR]

Published

2019

7. Stereotactic Body Radiation Therapy (SBRT) as Salvage Therapy for Oligorecurrent Pleural Mesothelioma After Multi-Modality Therapy.

Author

Schröder, Christina, Opitz, Isabelle, Guckenberger, Matthias, Stahel, Rolf, Weder, Walter, Förster, Robert, Andratschke, Nicolaus, and Lauk, Olivia

Subjects

SALVAGE therapy, RADIOTHERAPY, PROGRESSION-free survival, MESOTHELIOMA, STEREOTACTIC radiotherapy

Abstract

Introduction: Therapy options for patients with oligoprogressive malignant pleural mesothelioma (MPM) are limited. Stereotactic Body Radiotherapy (SBRT) may be a promising therapeutic option, as it delivers a localized ablative dose of radiation and therefore balances efficacy and treatment related toxicities. The intent of this retrospective analysis was to evaluate the feasibility of SBRT for limited pleural recurrences. Methods and Materials: This retrospective single-institution study is based on the 21 consecutive patients treated with hypofractionated radiotherapy for oligoprogressive MPM. Clinical and radiological data was collected at regular follow-up visits including toxicity, local control and survival. Results: At primary diagnosis, 57% of the patients presented with stage III disease. Initial treatment of MPM consisted of induction chemotherapy (n = 12) prior to a macroscopic complete resection (n = 18). Three patients received additional intracavitary chemotherapy and another three patients were treated with chemotherapy alone without another treatment at the time of first diagnosis. A total of 50 lesions in recurrent MPM were treated with SBRT. The median number of radiotherapy fractions was 5 (range 3–20) with a median dose per fraction of 5 Gy (range 2.5–12.5 Gy). The median total treatment dose was 30 Gy (20–50 Gy) with a median prescription isodose line (IDL) of 65% (65–100%). Median follow-up of all patients from diagnosis was 28 months (range 7–152 months). Analyzing all lesions separately, the 12-months-local control from SBRT was 73.5%. The median progression free survival (PFS) after SBRT was 6 months (range 0–21 months) and the median OS from first first SBRT was 29 months (range 0–61 months). Only one patients experienced above Grade 3 toxicities. Conclusion: This analysis demonstrates the feasibility of a SBRT approach for oligorecurrent MPM. SBRT was well-tolerated even after multiple repetitions and local control was high with a promising median OS. [ABSTRACT FROM AUTHOR]

Published

2019

8. Impact of delayed and prolonged fixation on the evaluation of immunohistochemical staining on lung carcinoma resection specimen.

Author

van Seijen, Maartje, Brcic, Luka, Gonzales, Atilio Navarro, Sansano, Irene, Bendek, Matyas, Brcic, Iva, Lissenberg-Witte, Birgit, Korkmaz, H. Ibrahim, Geiger, Thomas, Kammler, Rosita, Stahel, Rolf, Thunnissen, Erik, and ETOP

Abstract

Pre-analytical factors, such as fixation time, influence morphology of diagnostic and predictive immunohistochemical staining, which are increasingly used in the evaluation of lung cancer. Our aim was to investigate if variations in fixation time influence the outcome of immunohistochemical staining in lung cancer. From lung resections, specimen with tumor size bigger than 4 cm, 10 samples were obtained: 2 were put through the standard fixation protocol, 5 through the delayed, and 3 through the prolonged fixation protocol. After paraffin embedding, tissue microarrays (TMAs) were made. They were stained with 20 antibodies and scored for quality and intensity of staining. Samples with delay in fixation showed loss of TMA cores on glass slides and deterioration of tissue quality leading to reduction in the expression of CK 7, Keratin MNF116, CAM 5.2, CK 5/6, TTF-1, C-MET, Napsin A, D2-40, and PD-L1. Prolonged fixation had no influence on the performance of immunohistochemical stains. Delay of fixation negatively affects the expression of different immunohistochemical markers, influencing diagnostic (cytokeratins) and predictive (PD-L1) testing. These results emphasize the need for adequate fixation of resection specimen. [ABSTRACT FROM AUTHOR]

Published

2019

9. Afatinib in NSCLC With HER2 Mutations: Results of the Prospective, Open-Label Phase II NICHE Trial of European Thoracic Oncology Platform (ETOP).

Author

Dziadziuszko, Rafal, Smit, Egbert F., Dafni, Urania, Wolf, Juergen, Wasąg, Bartosz, Biernat, Wojciech, Finn, Stephen P., Kammler, Roswitha, Tsourti, Zoi, Rabaglio, Manuela, Ruepp, Barbara, Roschitzki-Voser, Heidi, Stahel, Rolf A., Felip, Enriqueta, and Peters, Solange

Published

2019

10. miR-625-3p and lncRNA GAS5 in Liquid Biopsies for Predicting the Outcome of Malignant Pleural Mesothelioma Patients Treated with Neo-Adjuvant Chemotherapy and Surgery.

Author

Kresoja-Rakic, Jelena, Szpechcinski, Adam, Kirschner, Michaela B., Ronner, Manuel, Minatel, Brenda, Martinez, Victor D., Lam, Wan L., Weder, Walter, Stahel, Rolf, Früh, Martin, Cerciello, Ferdinando, and Felley-Bosco, Emanuela

Subjects

MESOTHELIOMA, CANCER chemotherapy, ADJUVANT treatment of cancer, NON-coding RNA, IRINOTECAN, THERAPEUTICS

Abstract

Combining neo-adjuvant chemotherapy and surgery is part of multimodality treatment of malignant pleural mesothelioma (MPM), but not all patients benefit from this approach. In this exploratory analysis, we investigated the prognostic value of circulating miR-625-3p and lncRNA GAS5 after neo-adjuvant chemotherapy. 36 MPM patients from the SAKK 17/04 trial (NCT00334594), whose blood was available before and after chemotherapy were investigated. RNA was isolated from plasma and reverse transcribed into cDNA. miR-16-5p and β-actin were used as a reference gene for miR-625-3p and GAS5, respectively. After exclusion of samples due to hemolysis or RNA degradation, paired plasma samples from 32 patients before and after chemotherapy were further analyzed. Quantification of miR-625-3p levels in all 64 samples revealed a bimodal distribution and cloning and sequencing of miR-625-3p qPCR product revealed the presence of miR-625-3p isomiRs. Relative change of the circulating miR-625-3p and GAS5 levels after chemotherapy showed that increased circulating miR-625-3p and decreased GAS5 was significantly associated with disease progression (Fisher’s test, p = 0.0393). In addition, decreased levels of circulating GAS5 were significantly associated with shorter overall and progression-free survival. Our exploratory analysis revealed a potential value of circulating non-coding RNA for selection of patients likely to benefit from surgery after platinum-based adjuvant chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

11. Multimodal Treatment in Operable Stage III NSCLC: A Pooled Analysis on Long-Term Results of Three SAKK trials (SAKK 16/96, 16/00, and 16/01).

Author

Früh, Martin, Betticher, Daniel C., Stupp, Roger, Xyrafas, Alexandros, Peters, Solange, Ris, Hans Beat, Mirimanoff, Rene Olivier, Ochsenbein, Adrian F., Schmid, Ralph, Matzinger, Oscar, Stahel, Rolf A., Weder, Walter, Guckenberger, Matthias, Rothschild, Sacha I., Lardinois, Didier, Mach, Nicholas, Mark, Michael, Gautschi, Oliver, Thierstein, Sandra, and Biaggi Rudolf, Christine

Published

2019

12. Live-Cell Mesothelioma Biobank to Explore Mechanisms of Tumor Progression.

Author

Oehl, Kathrin, Kresoja-Rakic, Jelena, Opitz, Isabelle, Vrugt, Bart, Weder, Walter, Stahel, Rolf, Wild, Peter, and Felley-Bosco, Emanuela

Subjects

MESOTHELIOMA, BIOBANKS, CANCER invasiveness

Abstract

Experimental models closely representing in vivo conditions allow investigating mechanisms of resistance. Our aims were to establish a live-cell biobank of malignant pleural mesothelioma (MPM) samples and to obtain proof of principle that primary culture chemoresistant models, mimicking tumor progression observed in patients, can be obtained in vitro, providing a useful tool to investigate underlying mechanisms. Primary mesothelioma cultures were established from 235 samples between 2007 and 2014. Of two MPM patients, primary cultures obtained at different time points: at initial diagnosis, after neoadjuvant treatment at surgery and/or after tumor recurrence, were deeply investigated. Cells and corresponding tumor tissue were characterized by mesothelial protein and gene expression analysis. In addition, primary cultures from chemo naive patients were exposed to increasing doses of cisplatin/pemetrexed during three months and compared with non-treated cells in a cytotoxicity assay, and by selected profiling of senescence markers. In vitro chemoresistance in the primary mesothelioma cell cultures was associated with increased Thy1 (CD90) expression. Thy1 expression in MPM samples was significantly associated with poor overall survival in the TCGA MPM cohort. Our results illustrate that the establishment of a large live-cell MPM biobank contributes to a better understanding of therapy resistance observed in vivo, which eventually may lead to a more logical approach for developing new treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2018

13. A Novel BRCA1-Associated Protein-1 Isoform Affects Response of Mesothelioma Cells to Drugs Impairing BRCA1-Mediated DNA Repair.

Author

Parrotta, Rossella, Okonska, Agata, Ronner, Manuel, Weder, Walter, Stahel, Rolf, Penengo, Lorenza, and Felley-Bosco, Emanuela

Published

2017

14. Posttranscriptional Regulation Controls Calretinin Expression in Malignant Pleural Mesothelioma.

Author

Kresoja-Rakic, Jelena, Sulemani, Merve, Kirschner, Michaela B., Ronner, Manuel, Reid, Glen, Kao, Steven, Schwaller, Beat, Weder, Walter, Stahel, Rolf A., and Felley-Bosco, Emanuela

Subjects

MESOTHELIOMA, CALRETININ, PLEURA cancer, CALCIUM-binding proteins, LUCIFERASES, GENE transfection

Abstract

Calretinin (CALB2) is a diagnostic and prognostic marker in malignant pleural mesothelioma (MPM). We previously reported that calretinin expression is regulated at the mRNA level. The presence of a medium-sized (573 nucleotide) 30 untranslated region (3'UTR) predicted to contain binding sites for miR-30a/b/c/d/e and miR-9 as well as an adenine/uridine-rich element (ARE) in all three transcripts arising from the CALB2 gene, suggests that calretinin expression is regulated via posttranscriptional mechanisms. Our aim was to investigate the role of the CALB2-3'UTR in the posttranscriptional regulation of calretinin expression in MPM. CALB2-3'UTR was inserted downstream of the luciferase reporter gene using pmiRGLO vector and reporter expression was determined after transfection into MPM cells. Targeted mutagenesis was used to generate variants harboring mutated miR-30 family and ARE binding sites. Electrophoretic mobility shift assay was used to test for the presence of ARE binding proteins. CALB2-3'UTR significantly decreased luciferase activity in MPM cells. Analysis of mutation in the ARE site revealed a further destabilization of the reporter and human antigen R (HuR) binding to the ARE sequence was detected. The mutation of two miR-30 binding sites abolished CALB2-3'UTR destabilization effect; a transient delivery of miR-30e-5p mimics or anti-miR into MPM cells resulted in a significant decrease/increase of the luciferase reporter expression and calretinin protein, respectively. Moreover, overexpression of CALB2-3'UTR quenched the effect of miR-30e-5p mimics on calretinin protein levels, possibly by sequestering the mimics, thereby suggesting a competitive endogenous RNA network. Finally, by data mining we observed that expression of miR-30e-5p was negatively correlated with the calretinin expression in a cohort of MPM patient samples. Our data show the role of (1) adenine-uridine (AU)-binding proteins in calretinin stabilization and (2) miR-30e-5p in the posttranscriptional negative regulation of calretinin expression via interaction with its 3'UTR. Furthermore, our study demonstrates a possible physiological role of calretinin's alternatively spliced transcripts. [ABSTRACT FROM AUTHOR]

Published

2017

15. Bevacizumab Plus Pemetrexed Versus Pemetrexed Alone as Maintenance Therapy for Patients With Advanced Nonsquamous Non-Small-cell Lung Cancer: Update From the Swiss Group for Clinical Cancer Research (SAKK) 19/09 Trial.

Author

Gautschi, Oliver, Rothschild, Sacha I., Qiyu Li, Matter-Walstra, Klazien, Zippelius, Alfred, Betticher, Daniel C., Früh, Martin, Stahel, Rolf A., Cathomas, Richard, Rauch, Daniel, Pless, Miklos, Peters, Solange, Froesch, Patrizia, Zander, Thilo, Schneider, Martina, Biaggi, Christine, Mach, Nicolas, Ochsenbein, Adrian F., Li, Qiyu, and Swiss Group for Clinical Cancer Research

Published

2017

16. Propensity matched comparison of extrapleural pneumonectomy and pleurectomy/decortication for mesothelioma patients.

Author

Kostron, Arthur, Friess, Martina, Inci, Ilhan, Hillinger, Sven, Schneiter, Didier, Gelpke, Hans, Stahel, Rolf, Seifert, Burkhardt, Weder, Walter, and Opitz, Isabelle

Published

2017

17. Randomized Phase III Trial of Erlotinib versus Docetaxel in Patients with Advanced Squamous Cell Non-Small Cell Lung Cancer Failing First-Line Platinum-Based Doublet Chemotherapy Stratified by VeriStrat Good versus VeriStrat Poor. The European Thoracic Oncology Platform (ETOP) EMPHASIS-lung Trial.

Author

Peters, Solange, Stahel, Rolf A., Dafni, Urania, Ponce Aix, Santiago, Massutí, Bartomeu, Gautschi, Oliver, Coate, Linda, López Martín, Ana, van Heemst, Robbert, Berghmans, Thierry, Meldgaard, Peter, Cobo Dols, Manuel, Garde Noguera, Javier, Curioni-Fontecedro, Alessandra, Rauch, Daniel, Mark, Michael T., Cuffe, Sinead, Biesma, Bonne, van Henten, Arjen M.J., and Juan Vidal, Óscar

Published

2017

18. Low Merlin expression and high Survivin labeling index are indicators for poor prognosis in patients with malignant pleural mesothelioma.

Author

Meerang, Mayura, Bérard, Karima, Friess, Martina, Bitanihirwe, Byron K.Y., Soltermann, Alex, Vrugt, Bart, Felley-Bosco, Emanuela, Bueno, Raphael, Richards, William G., Seifert, Burkhardt, Stahel, Rolf, Weder, Walter, and Opitz, Isabelle

Published

2016

19. Relapse pattern and second-line treatment following multimodality treatment for malignant pleural mesothelioma.

Author

Kostron, Arthur, Friess, Martina, Crameri, Ornella, Inci, Ilhan, Schneiter, Didier, Hillinger, Sven, Stahel, Rolf, Weder, Walter, and Opitz, Isabelle

Subjects

MESOTHELIOMA, CANCER relapse, PNEUMONECTOMY, CANCER chemotherapy, CANCER radiotherapy, ONCOLOGIC surgery, THERAPEUTICS

Abstract

OBJECTIVES: To analyse the relapse pattern and influence of second-line treatment after recurrence of malignant pleural mesothelioma (MPM) in patients who had previously undergone multimodality treatment. METHODS: Between September 1999 and December 2013, 136 patients underwent macroscopic complete resection (MCR) by extrapleural pneumonectomy after induction chemotherapy for MPM. We analysed 106 patients who presented with recurrent disease until October 2014. Data were retrieved from our mesothelioma database, with additional information regarding precise localization gathered by reviewing the imaging and medical records. RESULTS: The overall recurrence rate was 78% (106/136 patients). The median freedom from recurrence was 9 months after surgery [95% confidence interval (95% CI) 7-10]. Local recurrence only was observed in 33 patients (31%), distant metastases only in 27 patients (26%) and simultaneous distant and local recurrence in 46 patients (43%). Local recurrence was observed significantly less frequently in patients having received adjuvant radiotherapy (19 vs 47%, P = 0.003), but there was no significant impact on overall survival (OS) [radiation: 22 months (95% CI 19-24); no-radiation: 23 months (95% CI 18-27), P = 0.6]. The median OS was 22 months (95% CI 21-24), median postrecurrence survival (PRS) was 7 months (95% CI 5-9) and patients with local recurrence only survived significantly longer (12 months, 95% CI 8-16) compared with patients with distant recurrence only (5 months, 95% CI 2-8) or distant plus local relapse (6 months, 95% CI 3-9; P = 0.04). A total of 78 patients received a second-line therapy after tumour recurrence: chemotherapy (n = 48), local radiotherapy (n = 9), surgery (n = 10) or a combination thereof (n = 11). Patients undergoing second-line treatment survived significantly longer compared with patients not receiving therapy (P < 0.0005). The median PRS after surgery was significantly longer than that of patients receiving chemo-, radio- or chemo-radiotherapy (P = 0.04). CONCLUSIONS: Local recurrence of MPM remains the most frequent type of relapse even after multimodality treatment including MCR. In the present cohort, active treatment seems beneficial to the patient since surgical excision of local tumour relapse has good long-term outcome in selected patients. Thus, second-line treatment may prolong PRS; however, these results need to be confirmed in a prospective manner. [ABSTRACT FROM AUTHOR]

Published

2016

20. A New Prognostic Score Supporting Treatment Allocation for Multimodality Therapy for Malignant Pleural Mesothelioma: A Review of 12 Years' Experience.

Author

Opitz, Isabelle, Friess, Martina, Kestenholz, Peter, Schneiter, Didier, Frauenfelder, Thomas, Thi Dan Linh Nguyen-Kim, Seifert, Burkhardt, Hoda, Mir Alireza, Klepetko, Walter, Stahel, Rolf A., Weder, Walter, and Nguyen-Kim, Thi Dan Linh

Published

2015

21. Expression of the Stem Cell Factor Nestin in Malignant Pleural Mesothelioma Is Associated with Poor Prognosis.

Author

Thies, Svenja, Friess, Martina, Frischknecht, Lukas, Korol, Dimitri, Felley-Bosco, Emanuela, Stahel, Rolf, Vrugt, Bart, Weder, Walter, Opitz, Isabelle, and Soltermann, Alex

Subjects

STEM cell factor, MESOTHELIOMA, MESENCHYMAL stem cells, BIPHASIC insulin, CANCER chemotherapy, PEMETREXED, PROGNOSIS

Abstract

Background: The epithelioid and sarcomatoid histologic variants of malignant pleural mesothelioma (MPM) can be considered as E- and M-parts of the epithelial-mesenchymal transition (EMT) axis; the biphasic being an intermediate. EMT is associated with an increase of stem cell (SC) traits. We correlated the neural crest SC marker nestin and the EMT marker periostin with histology, type of neo-adjuvant chemotherapy (CT) and overall survival (OS) of MPM patients. Patients and Methods: Tumor tissues of a historic cohort 1 (320 patients) and an intended induction chemotherapy followed by extrapleural pneumonectomy (EPP) cohort 2 (145 patients) were immunohistochemically H-scored (intensity of immunoreactivity multiplied by frequency of stained cells). Paired chemo-naïve biopsies and -treated surgical specimens were available for 105/145 patients. CT included platinum/gemcitabine (Pla/Gem) or platinum/pemetrexed (Pla/Pem). Results: Expression of any cytosolic nestin progressively increased from epithelioid to biphasic to sarcomatoid MPM in cohort 1, whereas the diagnostic markers calretinin and podoplanin decreased. In cohort 2, Pla/Pem CT increased the expression level of nestin in comparison to Pla/Gem, whereas the opposite was found for periostin. In Pla/Pem treated patients, nestin was higher in biphasic MPM compared to epithelioid. In addition to non-epithelioid histology, any expression of nestin in chemo-naïve biopsies (median overall survival: 22 vs. 17 months) and chemo-treated surgical specimens (18 vs. 12 months) as well as high periostin in biopsies (23 vs. 15 months) were associated with poor prognosis. In the multivariate survival analysis, any nestin expression in chemo-naïve biopsies proved to be an independent prognosticator against histology. In both pre- and post-CT situations, the combination of nestin or periostin expression with non-epithelioid histology was particularly/ dismal (all p-values <0.05). Conclusions: The SC marker nestin and the EMT marker periostin allow for further prognostic stratification among histologic variants of MPM. Their expression level is influenced by neo-adjuvant chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2015

22. Bevacizumab, Pemetrexed, and Cisplatin, or Bevacizumab and Erlotinib for Patients With Advanced Non-Small-Cell Lung Cancer Stratified by Epidermal Growth Factor Receptor Mutation: Phase II Trial SAKK19/09.

Author

Gautschi, Oliver, Mach, Nicholas, Rothschild, Sacha I, Li, Qiyu, Stahel, Rolf A, Zippelius, Alfred, Cathomas, Richard, Früh, Martin, Betticher, Daniel C, Peters, Solange, Rauch, Daniel, Feilchenfeldt, Jonas, Bubendorf, Lukas, Savic, Spasenija, Jaggi, Rolf, Leibundgut, Elisabeth Oppliger, Largiadèr, Carlo, Brutsche, Martin, Pilop, Christiane, and Stalder, Lukas

Published

2015

23. Bevacizumab, Pemetrexed, and Cisplatin, or Bevacizumab and Erlotinib for Patients With Advanced Non--Small-Cell Lung Cancer Stratified by Epidermal Growth Factor Receptor Mutation: Phase II Trial SAKK19/09.

Author

Gautschi, Oliver, Mach, Nicholas, Rothschild, Sacha I., Qiyu Li, Stahel, Rolf A., Zippelius, Alfred, Cathomas, Richard, Früh, Martin, Betticher, Daniel C., Peters, Solange, Rauch, Daniel, Feilchenfeldt, Jonas, Bubendorf, Lukas, Savic, Spasenija, Jaggi, Rolf, Leibundgut, Elisabeth Oppliger, Largiadèr, Carlo, Brutsche, Martin, Pilop, Christiane, and Stalder, Lukas

Published

2015

24. Use of Computed Tomography and Positron Emission Tomography/Computed Tomography for Staging of Local Extent in Patients With Malignant Pleural Mesothelioma.

Author

Frauenfelder, Thomas, Kestenholz, Peter, Hunziker, Roger, Linh Nguyen, Thi Dan, Fries, Martina, Veit-Haibach, Patrick, Husmann, Lars, Stahel, Rolf, Weder, Walter, and Opitz, Isabelle

Published

2015

25. Chemotherapy of Malignant Pleural Mesothelioma Induces Both Senescence and Apoptosis.

Author

Felley-Bosco, Emanuela and Stahel, Rolf A.

Published

2013

26. Lung Cancer.

Author

Zimmermann, Stefan, Fontecedro, Alessandra Curioni, Stahel, Rolf A., and Peters, Solange

Published

2013

27. Whole genome RNAi screens reveal a critical role of REV3 in coping with replication stress.

Author

Kotov, Ilya N., Siebring-van Olst, Ellen, Knobel, Philip A., van der Meulen-Muileman, Ida H., Felley-Bosco, Emanuela, van Beusechem, Victor W., Smit, Egbert F., Stahel, Rolf A., and Marti, Thomas M.

Published

2014

28. Determinants of outcome of solitary fibrous tumors of the pleura: an observational cohort study.

Author

Franzen, Daniel, Diebold, Matthias, Soltermann, Alex, Schneiter, Didier, Kestenholz, Peter, Stahel, Rolf, Weder, Walter, and Kohler, Malcolm

Abstract

Background: Solitary fibrous tumors of the pleura (SFTP) are rare and their long-term outcome is difficult to predict, as there are insufficient data which allow accurate characterization of the malignant variant. Thus the aim of this study was to describe the outcome and possible determinants of malignant behavior of SFTPs. Methods: Data were collected retrospectively from medical records of patients treated at the University Hospital Zurich from 1992 to 2012. Kaplan-Meier and Cox regression analysis were performed to define disease-free survival time (defined as survival without tumor-recurrence or tumor-related death) using the classical histo-morphological criteria (tumor size, localization, pedunculation, tumor necrosis or hemorrhage, mitotic activity and nuclear pleomorphism) and immunohistochemical parameters. Results: 42 patients (20 males) with SFTP (median (IQR) age 62 (56–71) years) could be identified. SFTP were associated with symptoms in 50% of all cases. Complete resection was achieved by video-assisted thoracic surgery or thoracotomy in 20 and 22 patients, respectively. Three SFTP-related deaths (7.1%) and four tumor recurrences (9.5%) were observed. Mean disease-free survival time was 136.2 (±13.1) months, and 2-, 5- and 10-year disease-free survival was 91%, 84%, and 67%, respectively. Mean disease-free survival inversely correlated with the mean tumor diameter, number of mitotic figures and proliferation rate (Ki-67 expression). Other criteria (tumor necrosis, atypical localization, sessile tumor, and pleomorphism) were not statistically significant prognostic parameters. Conclusions: Patients with large SFTP with a high mitotic index and high proliferation rate should be followed-up closely and over a prolonged time period in order to recognize recurrence of the SFTP early and at a treatable stage. Future research on this topic should focus on the prognostic role of immunohistochemistry including Ki-67 expression and molecular parameters. [ABSTRACT FROM AUTHOR]

Published

2014

29. GAS5 long non-coding RNA in malignant pleural mesothelioma.

Author

Renganathan, Arun, Kresoja-Rakic, Jelena, Echeverry, Nohemy, Ziltener, Gabriela, Vrugt, Bart, Opitz, Isabelle, Stahel, Rolf A., and Felley-Bosco, Emanuela

Subjects

MESOTHELIOMA, NON-coding RNA, CELL cycle, CELL lines, GENE expression, IMMUNOHISTOCHEMISTRY

Abstract

Background Malignant pleural mesothelioma (MPM) is an aggressive cancer with short overall survival. Long non-coding RNAs (lncRNA) are a class of RNAs more than 200 nucleotides long that do not code for protein and are part of the 90% of the human genome that is transcribed. Earlier experimental studies in mice showed GAS5 (growth arrest specific transcript 5) gene deletion in asbestos driven mesothelioma. GAS5 encodes for a lncRNA whose function is not well known, but it has been shown to act as glucocorticoid receptor decoy and microRNA "sponge". Our aim was to investigate the possible role of the GAS5 in the growth of MPM. Methods Primary MPM cultures grown in serum-free condition in 3% oxygen or MPM cell lines grown in serum-containing medium were used to investigate the modulation of GAS5 by growth arrest after inhibition of Hedgehog or PI3K/mTOR signalling. Cell cycle length was determined by EdU incorporation assay in doxycycline inducible short hairpinGAS5 clones generated from ZL55SPT cells. Gene expression was quantified by quantitative PCR. To investigate the GAS5 promoter, a 0.77 kb sequence was inserted into a pGL3 reporter vector and luciferase activity was determined after transfection into MPM cells. Localization of GAS5 lncRNA was identified by in situ hybridization. To characterize cells expressing GAS5, expression of podoplanin and Ki-67 was assessed by immunohistochemistry. Results GAS5 expression was lower in MPM cell lines compared to normal mesothelial cells. GAS5 was upregulated upon growth arrest induced by inhibition of Hedgehog and PI3K/mTOR signalling in in vitro MPM models. The increase in GAS5 lncRNA was accompanied by increased promoter activity. Silencing of GAS5 increased the expression of glucocorticoid responsive genes glucocorticoid inducible leucine-zipper and serum/glucocorticoid-regulated kinase-1 and shortened the length of the cell cycle. Drug induced growth arrest was associated with GAS5 accumulation in the nuclei. GAS5 was abundant in tumoral quiescent cells and it was correlated to podoplanin expression. Conclusions The observations that GAS5 levels modify cell proliferation in vitro, and that GAS5 expression in MPM tissue is associated with cell quiescence and podoplanin expression support a role of GAS5 in MPM biology. [ABSTRACT FROM AUTHOR]

Published

2014

30. PI3K/mTOR signaling in mesothelioma patients treated with induction chemotherapy followed by extrapleural pneumonectomy.

Author

Bitanihirwe, Byron K Y, Meerang, Mayura, Friess, Martina, Soltermann, Alex, Frischknecht, Lukas, Thies, Svenja, Felley-Bosco, Emanuela, Tsao, Ming-Sound, Allo, Ghassan, de Perrot, Marc, Seifert, Burkhardt, Moch, Holger, Stahel, Rolf, Weder, Walter, and Opitz, Isabelle

Published

2014

31. Identification of a seven glycopeptide signature for malignant pleural mesothelioma in human serum by selected reaction monitoring.

Author

Cerciello, Ferdinando, Choi, Meena, Nicastri, Annalisa, Bausch-Fluck, Damaris, Ziegler, Annemarie, Vitek, Olga, Felley-Bosco, Emanuela, Stahel, Rolf, Aebersold, Ruedi, and Wollscheid, Bernd

Subjects

GLYCOPEPTIDES, MESOTHELIOMA, TUMOR markers, BLOOD serum analysis, PROTEOMICS, ENZYME-linked immunosorbent assay, CONFERENCES & conventions, THERAPEUTICS

Abstract

Background Serum biomarkers can improve diagnosis and treatment of malignant pleural mesothelioma (MPM). However, the evaluation of potential new serum biomarker candidates is hampered by a lack of assay technologies for their clinical evaluation. Here we followed a hypothesis-driven targeted proteomics strategy for the identification and clinical evaluation of MPM candidate biomarkers in serum of patient cohorts. Results Based on the hypothesis that cell surface exposed glycoproteins are prone to be released from tumor-cells to the circulatory system, we screened the surfaceome of model cell lines for potential MPM candidate biomarkers. Selected Reaction Monitoring (SRM) assay technology allowed for the direct evaluation of the newly identified candidates in serum. Our evaluation of 51 candidate biomarkers in the context of a training and an independent validation set revealed a reproducible glycopeptide signature of MPM in serum which complemented the MPM biomarker mesothelin. Conclusions Our study shows that SRM assay technology enables the direct clinical evaluation of protein-derived candidate biomarker panels for which clinically reliable ELISA's currently do not exist. [ABSTRACT FROM AUTHOR]

Published

2013

32. Treatment of malignant pleural mesothelioma by fibroblast activation protein-specific re-directed T cells.

Author

Schuberth, Petra C., Hagedorn, Christian, Jensen, Shawn M., Gulati, Pratiksha, van den Broek, Maries, Mischo, Axel, Soltermann, Alex, Jüngel, Astrid, Belaunzaran, Osiris Marroquin, Stahel, Rolf, Renner, Christoph, and Petrausch, Ulf

Subjects

MESOTHELIOMA, T cells, FIBROBLASTS, IMMUNODEFICIENCY, LABORATORY mice, PHYSIOLOGICAL effects of cytokines, PHYSIOLOGY

Abstract

Introduction: Malignant pleural mesothelioma (MPM) is an incurable malignant disease, which results from chronic exposition to asbestos in at least 70% of the cases. Fibroblast activation protein (FAP) is predominantly expressed on the surface of reactive tumor-associated fibroblasts as well as on particular cancer types. Because of its expression on the cell surface, FAP is an attractive target for adoptive T cell therapy. T cells can be re-directed by retroviral transfer of chimeric antigen receptors (CAR) against tumor-associated antigens (TAA) and therefore represent a therapeutic strategy of adoptive immunotherapy. Methods: To evaluate FAP expression immunohistochemistry was performed in tumor tissue from MPM patients. CD8+ human T cells were retrovirally transduced with an anti-FAP-F19-ΔCD28/CD3ζ-CAR. T cell function was evaluated in vitro by cytokine release and cytotoxicity assays. In vivo function was tested with an intraperitoneal xenograft tumor model in immunodeficient mice. Results: FAP was found to be expressed in all subtypes of MPM. Additionally, FAP expression was evaluated in healthy adult tissue samples and was only detected in specific areas in the pancreas, the placenta and very weakly for cervix and uterus. Expression of the anti-FAP-F19-ΔCD28/CD3ζ-CAR in CD8+ T cells resulted in antigen-specific IFNγ release. Additionally, FAP-specific re-directed T cells lysed FAP positive mesothelioma cells and inflammatory fibroblasts in an antigen-specific manner in vitro. Furthermore, FAP-specific re-directed T cells inhibited the growth of FAP positive human tumor cells in the peritoneal cavity of mice and significantly prolonged survival of mice. Conclusion: FAP re-directed CD8+ T cells showed antigen-specific functionality in vitro and in vivo. Furthermore, FAP expression was verified in all MPM histotypes. Therefore, our data support performing a phase I clinical trial in which MPM patients are treated with adoptively transferred FAP-specific re-directed T cells. [ABSTRACT FROM AUTHOR]

Published

2013

33. Testing for anaplastic lymphoma kinase rearrangement to target crizotinib therapy: oncology, pathology and health economic perspectives.

Author

Lee, James A., Bubendorf, Lukas, Stahel, Rolf, and Peters, Solange

Published

2013

34. Differential Effects of Lovastatin on Cisplatin Responses in Normal Human Mesothelial Cells versus Cancer Cells: Implication for Therapy.

Author

Yandong Shi, Felley-Bosco, Emanuela, Marti, Thomas M., and Stahel, Rolf A.

Subjects

CANCER cells, CELLULAR pathology, BIOCHEMICAL genetics, CISPLATIN, ANTINEOPLASTIC agents, OXIDATIVE stress

Abstract

The cancer killing efficacy of standard chemotherapeutic agents such as cisplatin (CDDP) is limited by their side effects to normal tissues. Therefore, research efforts optimizing the safety and efficacy of those agents are clinically relevant. We did screen for agents that specifically protect normal human mesothelial cells against CDDP without reducing the cancer cell killing efficacy. Lovastatin was identified from the screen. Lovastatin at a pharmacologically relevant concentration strongly arrested the proliferation of normal cells, whereas cancer cells were less affected. CDDP-induced DNA damage response was not activated and normal cells showed enhanced tolerance to CDDP when normal cells were treated with the combination of CDDP and lovastatin. We demonstrate that interfering with protein geranylgeranylation is involved in the lovastatin-mediated CDDP protective effect in normal cells. In contrast to normal cells, in cancer cells lovastatin did not change the CDDP-induced response, and cancer cells were not protected by lovastatin. Furthermore, lovastatin at the pharmacological relevant concentration per se induced DNA damage, oxidative stress and autophagy in cancer cells but not in normal mesothelial cells. Therefore, our data suggest that lovastatin has a potential to improve the therapeutic index of cisplatin-based therapy. [ABSTRACT FROM AUTHOR]

Published

2012

35. Re-directed T cells for the treatment of fibroblast activation protein (FAP)-positive malignant pleural mesothelioma (FAPME-1).

Author

Petrausch, Ulf, Schuberth, Petra C, Hagedorn, Christian, Soltermann, Alex, Tomaszek, Sandra, Stahel, Rolf, Weder, Walter, and Renner, Christoph

Subjects

T cells, FIBROBLASTS, MESOTHELIOMA, ASBESTOS & health, DISEASE incidence, DEVELOPED countries

Abstract

Background: Asbestos is the main cause of MPM in industrialized countries. Even since asbestos is banned in most developed countries, the peak wave of MPM incidence is anticipated for the next years due to the long latency of asbestos induced MPM. MPM patients not eligible for surgical procedures like decortication or pleuropneumectomie have a median survival of 12 months with palliative chemotherapy. Therefore, new therapeutic approaches are of crucial need in this clinical situation. Methods/design: This is a phase I trial for patients with malignant pleural mesothelioma with pleural effusion testing the safety of a fixed single dose of 1x106 adoptively transferred FAP-specific re-directed T cells given directly in the pleural effusion. Lymphocytes will be taken 21 days before transfer from peripheral blood. CD8 positive T cells will be isolated and re-programmed by retroviral transfer of a chimeric antigen receptor recognizing FAP which serves as target structure in MPM. At day 0 of the protocol, re-directed T cells will be injected in the pleural effusion and patients will be monitored for 48h under intermediate care conditions. AE, SAE, SADR and SUSAR will be monitored for 35 days and evaluated by an independent safety board to define any dose limiting toxicity (DLT). No further patient can be treated before the previous patient passed day 14 after T cell transfer. The protocol will be judged as save when no DLT occurred in the first 3 patients, or 1 DLT in 6 patients. Secondary objectives are feasibility and immune monitoring. Discussion: Adoptive T cell transfer is a new and rapidly expanding branch of immunotherapies focusing on cancer treatment. Recently, objective responses could be observed in patients with chronic lymphatic leukemia treated with adoptively transferred CD19-specific re-directed T cells. The choice of the target antigen determines the possible on-target off-tissue toxicity of such approaches. There are reports of severe toxicity in patients who received T cells intravenously due to unexpected expression of the target antigen (on-target) in other tissues than the tumor (off-tissue). To minimize the risk of on-target off-tissue toxicity and to maximize the on-target anti-tumor effect we propose a clinical protocol with loco-regional administration of re-directed T cells. FAP-specific T cells will be directly injected in the pleural effusion of patients with MPM. Trial registration: ClinicalTrials.gov (NCT01722149) [ABSTRACT FROM AUTHOR]

Published

2012

36. Starvation-induced activation of ATM/Chk2/p53 signaling sensitizes cancer cells to cisplatin.

Author

Shi, Yandong, Felley-Bosco, Emanuela, Marti, Thomas M., Orlowski, Katrin, Pruschy, Martin, and Stahel, Rolf A.

Subjects

CANCER cells, CISPLATIN, CELL proliferation, TUMOR growth, DNA damage, SERUM

Abstract

Background: Optimizing the safety and efficacy of standard chemotherapeutic agents such as cisplatin (CDDP) is of clinical relevance. Serum starvation in vitro and short-term food starvation in vivo both stress cells by the sudden depletion of paracrine growth stimulation. Methods: The effects of serum starvation on CDDP toxicity were investigated in normal and cancer cells by assessing proliferation, cell cycle distribution and activation of DNA-damage response and of AMPK, and were compared to effects observed in cells grown in serum-containing medium. The effects of short-term food starvation on CDDP chemotherapy were assessed in xenografts-bearing mice and were compared to effects on tumor growth and/or regression determined in mice with no diet alteration. Results: We observed that serum starvation in vitro sensitizes cancer cells to CDDP while protecting normal cells. In detail, in normal cells, serum starvation resulted in a complete arrest of cellular proliferation, i.e. depletion of BrdU-incorporation during S-phase and accumulation of the cells in the G0/G1-phase of the cell cycle. Further analysis revealed that proliferation arrest in normal cells is due to p53/p21 activation, which is AMPK-dependent and ATM-independent. In cancer cells, serum starvation also decreased the fraction of S-phase cells but to a minor extent. In contrast to normal cells, serum starvation-induced p53 activation in cancer cells is both AMPK- and ATM-dependent. Combination of CDDP with serum starvation in vitro increased the activation of ATM/Chk2/p53 signaling pathway compared to either treatment alone resulting in an enhanced sensitization of cancer cells to CDDP. Finally, short-term food starvation dramatically increased the sensitivity of human tumor xenografts to cisplatin as indicated not only by a significant growth delay, but also by the induction of complete remission in 60% of the animals bearing mesothelioma xenografts, and in 40% of the animals with lung carcinoma xenografts. Conclusion: In normal cells, serum starvation in vitro induces a cell cycle arrest and protects from CDDP induced toxicity. In contrast, proliferation of cancer cells is only moderately reduced by serum starvation whereas CDDP toxicity is enhanced. The combination of CDDP treatment with short term food starvation improved outcome in vivo. Therefore, starvation has the potential to enhance the therapeutic index of cisplatin-based therapy. [ABSTRACT FROM AUTHOR]

Published

2012

37. Pleural mesothelioma side populations have a precursor phenotype.

Author

Frei, Claudia, Opitz, Isabelle, Soltermann, Alex, Fischer, Bruno, Moura, Ubiratan, Rehrauer, Hubert, Weder, Walter, Stahel, Rolf, and Felley-Bosco, Emanuela

Subjects

DRUG resistance in cancer cells, MESOTHELIOMA, ATP-binding cassette transporters, IMMUNOHISTOCHEMISTRY, MESENCHYMAL stem cells, MULTIDRUG resistance, CANCER chemotherapy, CELL populations, PHENOTYPES

Abstract

DyeCycleViolet was used to set up the side population (SP) functional assay aimed at identifying subpopulations of malignant pleural mesothelioma (MPM) tumor cells with chemoresistance phenotype associated with ABCG2 transporter activity. Self-renewal, chemoresistance and tumorigenicity were tested for SP and non-side population (NSP) cells. Tumors were characterized by mesothelin, calretinin, N-cadherin, D2-40 and Wilms tumor 1 (WT1) immunohistochemistry. Surface expression of mesenchymal stem cell markers CD90, CD73 and CD105 was investigated in SP and NSP cells. We identified SP cells with self-renewal properties and increased chemoresistance in MPM cell lines and tumor-derived primary cell cultures. Compared with the non-SP fraction (NSP), the SP fraction led to the development of tumors including cells with mesothelium precursor phenotype characterized by mesenchymal morphology, being WT1 negative but cytoplasmic D2-40 positive and having a tendency of increased tumorigenicity. The same phenotypic shift was observed in patients with relapsing tumors after chemotherapy. Furthermore, the SP cells were enriched in CD105−/low expressing cells, which were small sized and had increased tumorigenicity compared with CD105high cells. Taken together, our results support the hypothesis that MPM CD105−/low, chemoresistant small sized SP cells may constitute the cellular pool out of which recurrence develops. Further characterization of mechanisms of chemoresistance and self-renewal should lead to targets specific for this subpopulation in MPM patients. [ABSTRACT FROM AUTHOR]

Published

2011

38. Automated ERCC1 Immunohistochemistry in Non-small Cell Lung Cancer.

Author

Arbogast, Stefanie, Behnke, Silvia, Opitz, Isabelle, Stahel, Rolf A., Seifert, Burkhardt, Weder, Walter, Moch, Holger, and Soltermann, Alex

Published

2011

39. Pegfilgrastim reduces the length of hospitalization and the time to engraftment in multiple myeloma patients treated with melphalan 200 and auto-SCT compared with filgrastim.

Author

Samaras, Panagiotis, Blickenstorfer, Marcel, Siciliano, Raffaele Daniele, Haile, Sarah R., Buset, Elefteri M., Petrausch, Ulf, Mischo, Axel, Honegger, Hanspeter, Schanz, Urs, Stussi, Georg, Stahel, Rolf A., Knuth, Alexander, Stenner-Liewen, Frank, and Renner, Christoph

Subjects

MULTIPLE myeloma, FILGRASTIM, DRUG therapy, STEM cell transplantation, NEUTROPENIA

Abstract

To reduce the duration of neutropenia after conditioning chemotherapy and autologous peripheral blood stem cell transplantation (APBSCT), granulocyte-colony stimulating factors (G-CSF) are commonly administered. We retrospectively evaluated the impact of pegfilgrastim compared to filgrastim on neutrophil engraftment, hospital stay, and supportive measures in patients with multiple myeloma after conditioning with Melphalan 200 (Mel200) followed by APBSCT. Ninety-two APBSCT after Mel200 treatment were performed in 72 patients between January 2006 and December 2009 at our institution. Patients received either single-dose pegfilgrastim ( n = 46; 50%), or daily filgrastim ( n = 46; 50%) after APBSCT (median duration of filgrastim use, 9 days; range, 3-14 days). Duration of neutropenia grade IV was shorter with pegfilgrastim compared with filgrastim (median, 5 days (range, 3-14 days) versus 6 days (range, 3-9 days), p = 0.0079). The length of hospitalization differed significantly (pegfilgrastim (median, 14.5 days; range, 11-47 days) versus filgrastim (median, 15.5 days; range, 12-64 days), p = 0.024). Pegfilgrastim-treated patients had less red blood cell transfusions (median, 0 transfusions (range, 0-10) versus 0.5 transfusions (range, 0-9), p = 0.00065). Pegfilgrastim was associated with reduced cost of the treatment procedure compared with filgrastim ( p = 0.031). Pegfilgrastim appears to be at least equivalent to filgrastim without additional expenditure in myeloma patients treated with Mel200 and APBSCT. [ABSTRACT FROM AUTHOR]

Published

2011

40. Equivalence of Pegfilgrastim and Filgrastim in Lymphoma Patients Treated with BEAM Followed by Autologous Stem Cell Transplantation.

Author

Samaras, Panagiotis, Buset, Elefteri M., Siciliano, Raffaele Daniele, Haile, Sarah R., Petrausch, Ulf, Mischo, Axel, Honegger, Hanspeter, Pestalozzi, Bernhard C., Schanz, Urs, Stussi, Georg, Stahel, Rolf A., Knuth, Alexander, Renner, Christoph, and Stenner-Liewen, Frank

Subjects

FILGRASTIM, HODGKIN'S disease, STEM cell transplantation, COST analysis, LYMPHOMA treatment, THERAPEUTICS

Abstract

Objective: To evaluate the impact of pegfilgrastim on engraftment, hospital stay and resources in patients with Hodgkin's and non-Hodgkin's lymphoma after conditioning with high-dose BEAM followed by autologous peripheral blood stem cell transplantation (APBSCT) compared with filgrastim. Methods: We reviewed patient charts and our prospective transplantation database for clinical data from the post-transplant period. An integrated cost analysis, including the use of blood products and length of hospital stay, was also performed. Results: Fourteen (26%) patients with Hodgkin's lymphoma and 40 (74%) patients with non-Hodgkin's lymphoma were analyzed. Thirty-four (68%) patients received single-dose pegfilgrastim (6 mg), and 20 (32%) patients received daily filgrastim (5 μg/kg) after APBSCT. No differences were observed regarding duration of neutropenia grade 4 (pegfilgrastim median 7 days/filgrastim median 8 days; p = 0.13), thrombocytopenia grade 4 (7/9.5 days, respectively; p = 0.21), fever (4.5/2 days; p = 0.057), intravenous antibiotic treatment (11/10 days; p = 0.75) or length of hospital stay (16.5/16 days; p = 0.27) between the groups. The use of pegfilgrastim resulted in 12% higher treatment-related costs when compared to filgrastim, without reaching statistical significance (p = 0.38). Conclusion: Pegfilgrastim appears to be equivalent to filgrastim after high-dose BEAM followed by APBSCT in the treatment of lymphoma patients. Copyright © 2010 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2010

41. Consensus for EGFR Mutation Testing in Non-small Cell Lung Cancer.

Author

Pirker, Robert, Herth, Felix J. F., Kerr, Keith M., Filipits, Martin, Taron, Miquel, Gandara, David, Hirsch, Fred R., Grunenwald, Dominique, Popper, Helmut, Smit, Egbert, Dietel, Manfred, Marchetti, Antonio, Manegold, Christian, Schirmacher, Peter, Thomas, Michael, Rosell, Rafael, Cappuzzo, Federico, and Stahel, Rolf

Published

2010

42. The ESMO CME program: How practicing oncologists can maintain their knowledge in the E-era? Certification and recertification opportunities.

Author

Cervantes, Andrés, Vola, Doris, Jezdic, Svetlana, and Stahel, Rolf

Subjects

CONTINUING medical education, CONTINUING education, ONCOLOGY, PROFESSIONAL education, ONCOLOGISTS

Abstract

The main objective of the European Society for Medical Oncology (ESMO) continuing medical education (CME) program is to set standards of clinical competence for practice in oncology and encourage the update of knowledge required for professional excellence over a lifetime of service. To guarantee the maintenance levels of knowledge and skills, as well as the improvement in attitudes to cancer care, ESMO has taken several educational initiatives: the ESMO examination; the ESMO medical oncology re-certification program; organisation and/or accreditation of congresses, partnership and joint conferences, supported and labelled courses/meetings. The ESMO flagship journal, Annals of Oncology is an important educational tool that publishes articles addressing multiple oncology disciplines and provides CME points to those who participate in the on-line CME quiz. Currently, ESMO focuses on fostering new challenging CME opportunities such as E-Learning modules and new development tools with an appealing content of high scientific and educational value for practicing oncologists.Journal of Medical Marketing (2009) 9, 166–169. doi:10.1057/jmm.2009.9 [ABSTRACT FROM AUTHOR]

Published

2009

43. Malignant pleural mesothelioma.

Author

Stahel, Rolf A., Felley-Bosco, Emanuela, Opitz, Isabelle, and Weder, Walter

Abstract

Malignant pleural mesothelioma continues to be a challenge. The diagnosis and treatment of patients with malignant pleural mesothelioma requires a multidisciplinary approach. The diagnosis is best made by thoracoscopic biopsy and the aid of immunohistochemistry. Molecular studies identified inactivation of the neurofibromatosis-2 gene and INK4a/ARF to be key events in tumorigenesis. Based on the results of a Phase III trial, the combination of cisplatin with pemetrexed has become the preferred choice for chemotherapy, although there is suggestive evidence for the activity of other platin combinations based on Phase II studies. The optimal second-line chemotherapy remains to be defined. Surgical interventions ranging from pleurectomy/decortication to extrapleural pneumonectomy are increasingly offered in specialized centers, and the results of multimodality approaches with neoadjuvant or adjuvant chemotherapy and extrapleural pneumonectomy are encouraging. Ongoing investigations are defining the role of postoperative radiotherapy and the clinical activity of tyrosine kinase inhibitors targeting VEGFR2, histone deacetylase inhibitors and proteosome inhibitors. [ABSTRACT FROM AUTHOR]

Published

2009

44. Pemetrexed Plus Cisplatin or Pemetrexed Plus Carboplatin for Chemonaïve Patients with Malignant Pleural Mesothelioma: Results of the International Expanded Access Program.

Author

Santoro, Armando, O’brien, Mary E., Stahel, Rolf A., Nackaerts, Kristiaan, Baas, Paul, Karthaus, Meinolf, Eberhardt, Wilfried, Paz-Ares, Luis, Sundstrom, Stein, Liu, Yushan, Ripoche, Veronique, Blatter, Johannes, Visseren-Grul, Carla M., and Manegold, Christian

Published

2008

45. Human agonistic TRAIL receptor antibodies Mapatumumab andLexatumumab induce apoptosis in malignant mesothelioma and actsynergistically with cisplatin.

Author

Belyanskaya, Larisa L, Marti, Thomas M, Hopkins-Donaldson, Sally, Kurtz, Stefanie, Felley-Bosco, Emanuela, and Stahel, Rolf A

Subjects

APOPTOSIS, ANTINEOPLASTIC agents, CANCER treatment, TUMOR necrosis factors, IMMUNOGLOBULINS, TUMORS, MESOTHELIOMA

Abstract

Background: The incidence of malignant pleural mesothelioma (MPM) is associated with exposure to asbestos, and projections suggest that the yearly number of deaths in Western Europe due to MPM will increase until 2020. Despite progress in chemo- and in multimodality therapy, MPM remains a disease with a poor prognosis. Inducing apoptosis by tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) or agonistic monoclonal antibodies which target TRAIL-receptor 1 (TRAIL-R1) or TRAIL-R2 has been thought to be a promising cancer therapy. Results: We have compared the sensitivity of 13 MPM cell lines or primary cultures to TRAIL and two fully human agonistic monoclonal antibodies directed to TRAIL-R1 (Mapatumumab) and TRAIL-R2 (Lexatumumab) and examined sensitization of the MPM cell lines to cisplatin-induced by the TRAIL-receptor antibodies. We found that sensitivity of MPM cells to TRAIL, Mapatumumab and Lexatumumab varies largely and is independent of TRAIL-receptor expression. TRAIL-R2 contributes more than TRAIL-R1 to death-receptor mediated apoptosis in MPM cells that express both receptors. The combination of cisplatin with Mapatumumab or Lexatumumab synergistically inhibited the cell growth and enhanced apoptotic death. Furthermore, pre-treatment with cisplatin followed by Mapatumumab or Lexatumumab resulted in significant higher cytotoxic effects as compared to the reverse sequence. Combination-induced cell growth inhibition was significantly abrogated by pre-treatment of the cells with the antioxidant N-acetylcysteine. Conclusion: Our results suggest that the sequential administration of cisplatin followed by Mapatumumab or Lexatumumab deserves investigation in the treatment of patients with MPM. [ABSTRACT FROM AUTHOR]

Published

2007

46. A phase II, open-label study of gefitinib (IRESSA) in patients with locally advanced, metastatic, or relapsed renal-cell carcinoma.

Author

Jermann, Monika, Stahel, Rolf A., Salzberg, Marc, Cerny, Thomas, Joerger, Markus, Gillessen, Silke, Morant, Rudolf, Egli, Fritz, Rhyner, Kaspar, Bauer, Jean A., and Pless, Miklos

Subjects

RENAL cell carcinoma, CANCER, RENAL cancer, ANTINEOPLASTIC agents, CANCER chemotherapy, METASTASIS

Abstract

Epidermal growth factor receptor (EGFR) expression has been associated with clinical outcome in some studies of renal-cell carcinoma (RCC). We investigated the efficacy and safety of gefitinib (IRESSA), an EGFR tyrosine kinase inhibitor, in RCC patients. This phase II trial recruited 28 patients with advanced, metastatic, or relapsed RCC. Patients received oral gefitinib 500 mg/day. Objective responses (ORs) were assessed every 2 months according to RECIST. Baseline tumor biopsies were analyzed immunohistochemically for EGFR expression. At trial closure (March 2003), no ORs were seen but 14 patients (53.8%) had stable disease. At extended analysis (August 2004), median time to progression was 110 days (95% confidence interval [CI]: 55, 117); median overall survival was 303 days (95% CI 180, 444). Gefitinib was generally well tolerated. Skin rash and diarrhea were the most common drug-related adverse events (AEs) [54 and 39% of patients, respectively] and the most common drug-related grade 3/4 AEs (both 11%). The majority of tumor biopsies (91%) had ≥70% of tumor cells expressing membrane EGFR. Despite the lack of ORs in this study, disease control was observed in 53.8% of patients. Gefitinib was generally well tolerated and no unexpected drug-related AEs were observed. [ABSTRACT FROM AUTHOR]

Published

2006

47. Cisplatin activates Akt in small cell lung cancer cells and attenuates apoptosis by survivin upregulation.

Author

Belyanskaya, Larisa L., Hopkins-Donaldson, Sally, Kurtz, Stefanie, Simões-Wüst, Ana Paula, Yousefi, Shida, Simon, Hans-Uwe, Stahel, Rolf, and Zangemeister-Wittke, Uwe

Published

2005

48. Management and costs of treating lung cancer patients in a university hospital.

Author

Dedes, Konstantin J., Szucs, Thomas D., Bodis, Stephan, Joerger, Markus, Lowy, Adam, Russi, Erich W., Steinert, Hans C., Weder, Walter, and Stahel, Rolf A.

Subjects

MEDICAL care costs, LUNG cancer, HISTOLOGY, CANCER patients, CANCER treatment, MEDICAL economics, HOSPITAL care, MEDICAL care use, ANTINEOPLASTIC agents, ACADEMIC medical centers, COMPARATIVE studies, HEALTH care teams, HOSPITAL costs, LUNG tumors, RESEARCH methodology, MEDICAL cooperation, RESEARCH, EVALUATION research, RETROSPECTIVE studies, ECONOMICS

Abstract

Background: New diagnostic tools and emerging medications have significantly changed the existing medical treatment options for lung cancer over the last 5 years. However, the increase in healthcare costs in all developed societies has put the more economical treatments on centre stage.Objective: To examine the patterns and costs of lung cancer management at a Swiss University hospital at which there is a focus on interdisciplinary treatment.Patients and Methods: All patients encountered during 1998 at the University Hospital of Zurich (USZ) with any diagnosis of lung cancer were selected for this retrospective study. Medical and sociodemographic data were collected by medical chart review for a period beginning with the first contact and ending with the last follow-up examination up to 30 months afterwards. Costs were calculated by assessing all resources used by each patient, multiplied by a uniform average cost factor. Results are in euros at 1999 prices.Results: The sample included 118 patients (72% male) with a mean age of 64.2 years (SD 9.8, range 34-85 years) and a mean smoking history of 45 pack-years (SD 31.8, range 0-13 pack-years). Eighty-nine percent of all patients showed histology of non-small cell lung cancer (NSCLC), whereas 11% showed small cell lung cancer (SCLC). Of the NSCLC patients, 27% were classified as stage I, 14% as stage II, 19% as stage IIIA, 11% as stage IIIB and 26% as stage IV disease. The overall survival rate after 1 year was 55% and after 2 years was 29%. Gender and health insurance status were not associated with overall survival. The median length of hospitalisation during the first year of treatment was 14 days (range 0-112 days). For the entire patient sample, the mean cost per patient was 19,408 euros (median 14,691 euros, range 1821-80,020 euros), 71% of which was due to the hospitalisation costs. The mean cost per NSCLC patient was 19,212 euros (median 14,511 euros, range 1821-80,020 euros) and for SCLC patients it was 20,992 euros (median 15,367 euros, range 5282-51,840 euros).Conclusion: This is the first study attempting to estimate the hospital cost of treatment for lung cancer patients in Switzerland and central Europe. The major part of the total cost was due to hospitalisation costs. Patients with advanced stages of lung cancer show the highest cost, mainly due to the costs of chemotherapy. We found that the distribution of total cost is asymmetric: a small number of patients with an excessively long hospital stay cause very high costs. [ABSTRACT FROM AUTHOR]

Published

2004

49. HIV-testing and Newly-diagnosed Malignant Lymphomas. The SAKK 96/90 Registration Study.

Author

D'Addario, Giannicola, Dieterle, Alexander, Torhorst, Joachim, Maibach, Rudolf, Stahel, Rolf, Egli, Fritz, Lohri, Andreas, Cavalli, Franco, Fey, Martin, and Ketterer, Nicolas

Subjects

LYMPHOMAS, HIV infections

Abstract

The association of Non-Hodgkin Lymphoma (NHL) and HIV-infection was soon recognized and the Center of Disease Control (CDC) has classified some types of NHL as AIDS-defining illnesses (ADI). Hodgkin's disease (HD) represents the most common type of non ADI malignancy in HIV-infected cases. Commonly, data on malignant lymphoma in this population is collected in known HIV-positive patients or in autopsy-series. This registration study was designed to estimate the incidence of HIVpositivity in patients with newly diagnosed malignant lymphoma. A registration of all patients with newly diagnosed malignant lymphoma and their HIV-status was performed in every center of the Swiss Group for Clinical Cancer research (SAKK) from January 1, 1991 to July 31, 1993. Among 474 eligible patients, HIV-status was evaluated in 400 and 52 were tested positive (13%), 42 (81%) of them males. Three of them were newly detected cases (after lymphoma-diagnosis). Three hundred and forty patients (72%) presented with NHL, 42 (12.4%) of them HIV-positive; 33 out of these had aggressive lymphoma. B-symptoms were significantly more frequent in HIV-positive patients. In the 134 patients with HD, 10 (7.5%) tested HIV-positive, mostly presenting with stage IV disease (7), B-symptoms (9) and extranodal disease (7). In conclusion, 13% out of 400 evaluated patients with newly diagnosed malignant lymphoma tested HIV-positive. The study confirms the predominance of aggressive lymphoma histologies and frequent presentation with B-symptoms in HIV-positive patients with NHL. Male gender, young age (26-35 years) and B-symptoms are prognostic factors for HIV-positivity in NHL. [ABSTRACT FROM AUTHOR]

Published

2003

50. Bcl-2/bcl-xL Bispecific Antisense Treatment Sensitizes Breast Carcinoma Cells to Doxorubicin, Paclitaxel and Cyclophosphamide.

Author

Simões-Wüst, A., Schürpf, Thomas, Hall, Jonathan, Stahel, Rolf, and Zangemeister-Wittke, Uwe

Abstract

Overexpression of the anti-apoptotic proteins bcl-2 and bcl-xL is implicated in breast cancer development, tumor progression and drug resistance. Here we describe the use of the bcl-2/bcl-xL bispecific antisense oligonucleotide 4625 to sensitize breast carcinoma cells to anti-cancer drugs routinely used in breast cancer therapy. MCF7 cells were treated with oligonucleotide 4625, doxorubicin, paclitaxel or cyclophosphamide alone, or with combinations of oligonucleotide and the anti-cancer drugs. As measured in cell viability assays, treatment with the various combinations reduced the number of viable MCF7 cells more effectively than treatment with the single drugs alone. Treatment with a sequence control oligonucleotide did not affect cell viability. All combination treatments induced apoptosis as demonstrated by the appearance of massive nuclear condensation in a high proportion of the cells. To further characterize the interaction between 4625 and doxorubicin, paclitaxel or cyclophosphamide, the median-effect method was used. In MCF7 cells all combinations resulted in potent synergistic effects over a broad range of toxicity with combination indices ranging from 0.8 to 0.1. Similarly, strong synergistic interactions between oligonucleotide 4625 and the anti-cancer drugs were also observed in cultures of the breast carcinoma cell line MDA-MB-231. Our data suggest the use of 4625 as a potent adjuvant in breast cancer chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2002