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Start Over Author "Niegisch, Günter" Publisher elsevier b.v.
23 results on '"Niegisch, Günter"'

1. Enfortumab Vedotin in Metastatic Urothelial Carcinoma: Survival and Safety in a European Multicenter Real-world Patient Cohort

Author

Zschäbitz, Stefanie, Biernath, Nadine, Hilser, Thomas, Höllein, Alexander, Zengerling, Friedemann, Cascucelli, Jozefina, Paffenholz, Pia, Seidl, Daniel, Lutz, Christoph, Schlack, Katrin, Kingreen, Dorothea, Klümper, Niklas, Ivanyi, Philipp, von Amsberg, Gunhild, Heers, Hendrik, Roghmann, Florian, Tauber, Robert L., Cathomas, Richard, Hofer, Luisa, Niegisch, Günter, Klee, Melanie, Ehrenberg, Roland, Hassler, Andreas, Hadaschik, Boris A., Grünwald, Viktor, and Darr, Christopher

Published
2023
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4. Efficacy of Surgery in the Primary Tumor Site for Metastatic Urothelial Cancer: Analysis of an International, Multicenter, Multidisciplinary Database

Author

Moschini, Marco, Xylinas, Evanguelos, Zamboni, Stefania, Mattei, Agostino, Niegisch, Günter, Yu, Evan Y., Bamias, Aristotelis, Agarwal, Neeraj, Sridhar, Srikala S., Sternberg, Cora N., Vaishampayan, Ulka N., Rosenberg, Jonathan E., Bellmunt, Joaquim, Galsky, Matthew D., Montorsi, Francesco, and Necchi, Andrea

Published
2020
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5. Modeling 1-year Relapse-free Survival After Neoadjuvant Chemotherapy and Radical Cystectomy in Patients with Clinical T2–4N0M0 Urothelial Bladder Carcinoma: Endpoints for Phase 2 Trials

Author

Bandini, Marco, Briganti, Alberto, Plimack, Elizabeth R., Niegisch, Günter, Yu, Evan Y., Bamias, Aristotelis, Agarwal, Neeraj, Sridhar, Srikala S., Sternberg, Cora N., Vaishampayan, Ulka, Théodore, Christine, Rosenberg, Jonathan E., Bellmunt, Joaquim, Galsky, Matthew D., Montorsi, Francesco, and Necchi, Andrea

Published
2019
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6. Lack of Effectiveness of Postchemotherapy Lymphadenectomy in Bladder Cancer Patients with Clinical Evidence of Metastatic Pelvic or Retroperitoneal Lymph Nodes Only: A Propensity Score-based Analysis

Author

Necchi, Andrea, Mariani, Luigi, Lo Vullo, Salvatore, Yu, Evan Y., Woods, Michael E., Wong, Yu-Ning, Harshman, Lauren C., Alva, Ajjaj, Sternberg, Cora N., Bamias, Aristotelis, Grivas, Petros, Koshkin, Vadim S., Roghmann, Florian, Dobruch, Jakub, Eigl, Bernie J., Nappi, Lucia, Milowsky, Matthew I., Niegisch, Guenter, Pal, Sumanta K., De Giorgi, Ugo, Recine, Federica, Vaishampayan, Ulka, Berthold, Dominik D., Bowles, Daniel W., Baniel, Jack, Theodore, Christine, Ladoire, Sylvain, Srinivas, Sandy, Agarwal, Neeraj, Crabb, Simon, Sridhar, Srikala, Golshayan, Ali-Reza, Ohlmann, Carsten, Xylinas, Evanguelos, Powles, Thomas, Rosenberg, Johnathan E., Bellmunt, Joaquim, van Rhijn, Bas, Galsky, Matthew D., and Hendricksen, Kees

Published
2019
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9. Changes in histone deacetylase (HDAC) expression patterns and activity of HDAC inhibitors in urothelial cancers.

Author

Niegisch, Günter, Knievel, Judith, Koch, Annemarie, Hader, Christiane, Fischer, Ute, Albers, Peter, and Schulz, Wolfgang A.

Subjects
*GENE expression, *TRANSITIONAL cell carcinoma, *ISOENZYMES, *CELL lines, *HISTONE deacetylase inhibitors, *DRUG efficacy, *MESSENGER RNA, *THERAPEUTICS
Abstract

Abstract: Objective: To determine histone deacetylase (HDAC) isoenzyme expression patterns in urothelial cancer tissues and cell lines and investigate their potential to predict the efficacy of the HDAC inhibitor vorinostat. Materials and methods: Expression of HDAC mRNAs was determined by quantitative RT-PCR in 18 urothelial cancer cell lines (UCC), normal uroepithelial controls (NUC), 24 urothelial cancer tissues, and 12 benign controls. Results were compared with published microarray data. Effects of pan-HDAC inhibitor vorinostat and on UCCs were determined by viability and apoptosis assays, cell cycle analysis, and measurements of p21CIP1, thymidylate synthase (TS), and EZH2. In addition, protein expression levels of HDACs were investigated in UCCs. Results: Prominent changes in UCCs were HDAC2 and/or HDAC8 up-regulation in 11 of 18 cell lines and decreased expression of HDAC4, HDAC5, and/or HDAC7 mRNA in 15 of 18 cell lines. In cancer tissues, HDAC8 was likewise significantly up-regulated (P = 0.002), whereas HDAC2 up-regulation was detected only in a subset of tumors (9/24, P = 0.085). Overexpression of HDAC2 and HDAC8 mRNA did not correspond with the protein level. Vorinostat induced G2/M arrest, an increase in the sub-G1 fraction, up-regulation of p21, and down-regulation of TS in all UCC. Effects on EZH2 and PARP cleavage as well as activation of caspase 3/7 differed between cell lines. Associations between the overall sensitivity to the pan-HDACi vorinostat and overexpression of HDAC2 and HDAC8 mRNA were not observed. Conclusions: In urothelial cancer, up-regulation of HDAC2 and HDAC8 and down-regulation of HDAC4, HDAC5, and HDAC7 mRNA are common findings. The treatment effect of the pan-HDAC inhibitor vorinostat was variable in UCCs and up-regulation of HDAC2 and HDAC8 was not predictive for treatment response. Whether selective targeting of HDAC2, HDAC8, or other HDACs deregulated in urothelial cancer (e.g., HDAC4, HDAC5, and HDAC7) result in a more consistent treatment response needs further investigation. [Copyright &y& Elsevier]

Published
2013
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10. Tailored immunotherapy approach with nivolumab with or without ipilimumab in patients with advanced transitional cell carcinoma after platinum-based chemotherapy (TITAN-TCC): a multicentre, single-arm, phase 2 trial.

Author

Grimm, Marc-Oliver, Grün, Christine Barbara, Niegisch, Günter, Pichler, Martin, Roghmann, Florian, Schmitz-Dräger, Bernd, Baretton, Gustavo, Schmitz, Marc, Bolenz, Christian, Foller, Susan, Leucht, Katharina, Schumacher, Ulrike, Schostak, Martin, Meran, Johannes, Loidl, Wolfgang, and Zengerling, Friedemann

Subjects
*TRANSITIONAL cell carcinoma, *NIVOLUMAB, *IPILIMUMAB, *BLADDER cancer, *KIDNEY pelvis, *IMMUNOTHERAPY
Abstract

Nivolumab is used after platinum-based chemotherapy in patients with metastatic urothelial carcinoma. Studies suggest improved outcomes for dual checkpoint inhibition with high ipilimumab doses. We aimed to examine the safety and activity of nivolumab induction and high-dose ipilimumab as an immunotherapeutic boost as a second-line treatment for patients with metastatic urothelial carcinoma. TITAN-TCC is a multicentre, single-arm, phase 2 trial done at 19 hospitals and cancer centres in Germany and Austria. Adults aged 18 years or older with histologically confirmed metastatic or surgically unresectable urothelial cancer of the bladder, urethra, ureter, or renal pelvis were eligible. Patients had to have progression during or after first-line platinum-based chemotherapy and up to one more second-line or third-line treatment, a Karnofsky Performance Score of 70 or higher, and measurable disease as per Response Evaluation Criteria in Solid Tumors version 1.1. After four doses of intravenous nivolumab 240 mg induction monotherapy every 2 weeks, patients with a partial or complete response at week 8 continued maintenance nivolumab, whereas those with stable or progressive disease (non-responders) at week 8 received a boost of two or four doses of intravenous nivolumab 1 mg/kg plus ipilimumab 3 mg/kg every 3 weeks. Patients who subsequently had progressive disease during nivolumab maintenance also received a boost, using this schedule. The primary endpoint was the confirmed investigator-assessed objective response rate in the intention-to-treat population and had to exceed 20% for the null hypothesis to be rejected (based on the objective response rate with nivolumab monotherapy in the CheckMate-275 phase 2 trial). This study is registered with ClinicalTrials.gov , NCT03219775 , and is ongoing. Between April 8, 2019, and Feb 15, 2021, 83 patients with metastatic urothelial carcinoma were enrolled and all received nivolumab induction treatment (intention-to-treat population). The median age of enrolled patients was 68 years (IQR 61–76), and 57 (69%) were male and 26 (31%) were female. 50 (60%) patients received at least one boost dose. A confirmed investigator-assessed objective response was recorded in 27 (33%) of 83 patients in the intention-to-treat population, including six (7%) patients who had a complete response. This objective response rate was significantly higher than the prespecified threshold of 20% or less (33% [90% CI 24–42]; p=0·0049). The most common grade 3–4 treatment-related adverse events were immune-mediated enterocolitis (nine [11%] patients) and diarrhoea (five [6%] patients). Two (2%) treatment-related deaths were reported, both due to immune-mediated enterocolitis. Treatment with nivolumab and nivolumab plus ipilimumab boosts in early non-responders and patients who progress late significantly improved objective response rate after previous platinum-based chemotherapy compared with the rate reported with nivolumab in the CheckMate-275 trial. Our study provides evidence for the added value of high-dose ipilimumab 3 mg/kg and suggests a potential role for the combination as a rescue strategy in platinum-pretreated patients with metastatic urothelial carcinoma. Bristol Myers Squibb. [ABSTRACT FROM AUTHOR]

Published
2023
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11. Prognostic Factors in Second-Line Treatment of Urothelial Cancers With Gemcitabine and Paclitaxel (German Association of Urological Oncology Trial AB20/99)

Author

Niegisch, Günter, Fimmers, Rolf, Siener, Roswitha, Park, Su-In, and Albers, Peter

Subjects
*TRANSITIONAL cell carcinoma, *CANCER chemotherapy, *CANCER prognosis, *PACLITAXEL, *CLINICAL trials, *COHORT analysis, *MEDICAL statistics, *THERAPEUTICS
Abstract

Abstract: Background: In the treatment of urothelial cancer, identification of patients who are likely to benefit from further therapy after cisplatin failure is crucial for reasonable treatment decisions. Objective: Validate the prognostic factor model (PFM) for survival developed by Bellmunt et al. in a different patient cohort with a different chemotherapy regimen. Design, setting, and participants: Baseline parameters of 102 patients treated within a randomized phase 3 trial of second-line gemcitabine and paclitaxel (GP) comparing short-term to prolonged chemotherapy (German Association of Urological Oncology trial AB20/99) were analyzed. Patients were stratified according to the PFM based on a score including performance status, presence of hepatic metastases, and hemoglobin levels. Measurements: The baseline parameters of the GP cohort were compared with those of patients treated in the phase 3 trial of vinflunine versus best supportive care. Univariate and multivariate analyses of baseline parameters with respect to overall survival (OS) and treatment response were performed. OS of patients stratified according to the PFM was compared by log-rank test. Results and limitations: The vinflunine and the GP cohorts differed, as patients after perioperative (neoadjuvant or adjuvant) treatment were included in the latter cohort. According to the PFM, prognostic subgroups with significant difference in OS (11.8 mo [95% confidence interval (CI), 6.3–17.3], 8.1 mo [95% CI, 4.8–11.4], 3.2 mo [95% CI, 0.0–7.9]; p =0.007) were identified. The PFM identified risk groups in patients with failed treatment of metastatic disease (14.1 mo [95% CI, 8.9–19.3], 7.3 mo [95% CI, 0.0–17.8], 3.8 mo [95% CI, 0.0–9.0]; p =0.006) but not in patients treated (neo)adjuvantly. Lymph node–only disease was a strong predictor of treatment response that overruled every other single predictive parameter (0.284, p = 0.0266). Conclusions: The PFM was successfully validated in the GP and should be used to tailor second-line treatment strategy. Patients with lymph node–only disease may benefit from second-line treatment even if anemia or impaired performance status is present. Trial registration: German Cancer Society 01–09 (www.krebsgesellschaft.de). [Copyright &y& Elsevier]

Published
2011
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14. Late toxicities and recurrences in patients with clinical stage I non-seminomatous germ cell tumours after 1 cycle of adjuvant bleomycin, etoposide and cisplatin versus primary retroperitoneal lymph node dissection – A 13-year follow-up analysis of a phase III trial cohort

Author

Hiester, Andreas, Fingerhut, Anna, Niegisch, Günter, Siener, Roswitha, Krege, Susanne, Schmelz, Hans-Ulrich, Dieckmann, Klaus-Peter, Heidenreich, Axel, Kwasny, Peter, Pechoel, Maik, Lehmann, Jan, Kliesch, Sabine, Köhrmann, Kai-Uwe, Fimmers, Rolf, Loy, Volker, Wittekind, Christian, Hartmann, Michael, and Albers, Peter

Subjects
*GERMINOMA, *ETOPOSIDE, *PATIENT aftercare, *CONFIDENCE intervals, *DRUG tolerance, *CANCER relapse, *TUMOR classification, *CANCER patients, *TESTIS tumors, *CISPLATIN, *QUESTIONNAIRES, *DESCRIPTIVE statistics, *SURVIVAL analysis (Biometry), *SECONDARY primary cancer, *COMBINED modality therapy, *BLEOMYCIN, *DRUG toxicity, *SURGICAL excision, *LYMPH node surgery, *LONGITUDINAL method
Abstract

One cycle of adjuvant chemotherapy with bleomycin, etoposide and cisplatin (BEP) has shown superiority in recurrence-free survival over retroperitoneal lymph node dissection (RPLND) in patients with clinical stage (CS) I non-seminomatous germ cell tumours (NSGCTs) of the testis in the setting of a phase III trial. We report the recurrences and late toxicities of this study after 13 years of follow-up. Questionnaires from 382 patients with CS I NSGCT treated with 1 cycle of adjuvant BEP (arm A) or RPLND + two cycles of adjuvant BEP in cases of pathological stage II disease (arm B) were evaluated regarding recurrences and late toxicity. Overall, information on recurrence status was available in 337 patients, and 170 questionnaires were evaluable for toxicity (arm A: 95; arm B: 75). With a median follow-up of 13.8 years (0–22), 3 patients (1.6%) in arm A and 16 patients (8.4%) in arm B experienced recurrence. The 15-year PFS in arm A/B was 99% (CI 96–100%)/92% (CI 89–99%) (p = 0.0049). The 15-year OS in arm A/B was 93% (CI 87–97%)/93% (CI 86–97%) (p = 0.83). Eight patients (4.2%) in arm A and four patients (2.1%) in arm B showed metachronous secondary testicular cancer (p = 0.26). Five patients (2.6%) in arm A and four patients (2.1%) in arm B developed other malignancies. Toxicities were not significantly different apart from retrograde ejaculation, which occurred more frequently after RPLND (10% versus 24%, p = 0.01). With long-term observation, one cycle of BEP remains superior to RPLND in preventing recurrence and was tolerated without any clinically relevant long-term toxicities. • >13-year follow-up recurrences in CS I NSGCT more frequent with RPLND than after BEP x1. • No excess mortality due to secondary malignancies could be detected. • Late toxicities do not differ between 1 x BEP and RPLND. [ABSTRACT FROM AUTHOR]

Published
2021
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16. BTA stat®, NMP22® BladderChek®, UBC® Rapid Test, and CancerCheck® UBC® rapid VISUAL as urinary marker for bladder cancer: Final results of a German multicenter study.

Author

Ecke, Thorsten H., Meisl, Christina J., Schlomm, Thorsten, Rabien, Anja, Labonté, Flora, Rong, Dezhi, Hofbauer, Sebastian, Friedersdorff, Frank, Sommerfeldt, Lilli, Gagel, Nella, Gössl, Andreas, Barski, Dimitri, Otto, Thomas, Grunewald, Camilla M., Niegisch, Günter, Hennig, Martin J.P., Kramer, Mario W., Koch, Stefan, Roggisch, Jenny, and Hallmann, Steffen

Subjects
*BLADDER cancer, *NON-muscle invasive bladder cancer, *BLADDER, *URINALYSIS, *TUMOR markers, *RAPID diagnostic tests
Abstract

• First multicenter study comparing urine-based rapid tests for bladder cancer. • Highest sensitivities for HGNMI bladder cancer for BTA stat® and UBC® Rapid Test. • Cytology should mostly be used in specialized centers. • Use of urinary-based rapid tests in management of bladder cancer should be discussed. BTA stat®, NMP22® BladderChek®, UBC® Rapid Test, and CancerCheck® UBC® rapid VISUAL are urinary-based rapid tests. This multicenter study is the first study comparing all available rapid tests on a large cohort of bladder cancer patients and healthy controls in one setting. In total 732 urine samples (second morning urine) in a real-world assessment have been analyzed. We evaluated clinical samples from 464 patients with histologically confirmed urothelial tumors of the urinary bladder (17 solitary CIS, 189 low-grade, 187 high-grade nonmuscle invasive, 71 high-grade muscle invasive), 77 patients with No Evidence of Disease (NED), and from 191 healthy controls. Urine samples were analyzed by the BTA stat®, NMP22® BladderChek®, UBC® Rapid Test point-of-care (POC) system using the concile Omega 100 POC reader, and CancerCheck® UBC® rapid VISUAL. Sensitivities and specificities were calculated by contingency analyses. All investigated urinary markers detected more pathological concentrations in urine of bladder cancer patients compared to tumor-free patients. The calculated diagnostic sensitivities for BTA stat®, NMP22® BladderChek®, UBC® Rapid Test, CancerCheck® UBC® rapid VISUAL, and cytology were 62.4%, 13.4%, 58.2%, 28.6%, 36.2% for low-grade, 83.4%, 49.5%, 84.5%, 63.1%, 71.2% for high-grade nonmuscle invasive, and 95.8%, 35.2%, 76.1%, 50.7%, 67.7% for high-grade muscle-invasive bladder cancer. The specificity was 67.9%, 95.5%, 79.4%, 94.4%, and 83.7%, respectively. The area under the curve (AUC) after receiver operating characteristics (ROC) analysis for high-grade non–muscle-invasive tumors was 0.757, 0.725, 0.819, 0.787, and 0.774, respectively. The analysis of more than 700 urine samples offers an objective view on urine-based rapid diagnostics. Elevated pathological concentrations of markers in urine of bladder cancer patients were detected in all investigated tests. The highest sensitivities for high-grade non–muscle-invasive tumors were calculated for BTA stat® and UBC® Rapid Test, whereas NMP22® BladderChek®, and cytology showed the highest specificities. BTA stat® and UBC® Rapid Test have the potential to be used as a clinical valuable urinary protein biomarker for the detection of high-grade non–muscle-invasive bladder cancer patients and could be included in the management of these tumors. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Incremental Utility of Adjuvant Chemotherapy in Muscle-invasive Bladder Cancer: Quantifying the Relapse Risk Associated with Therapeutic Effect.

Author

Pederzoli, Filippo, Bandini, Marco, Briganti, Alberto, Plimack, Elizabeth R., Niegisch, Günter, Yu, Evan Y., Bamias, Aristotelis, Agarwal, Neeraj, Sridhar, Srikala S., Sternberg, Cora N., Vaishampayan, Ulka N., Théodore, Christine, Rosenberg, Jonathan E., Harshman, Lauren C., Bellmunt, Joaquim, Galsky, Matthew D., Gallina, Andrea, Salonia, Andrea, Montorsi, Francesco, and Necchi, Andrea

Subjects
*CANCER relapse, *THERAPEUTIC complications, *ADJUVANT treatment of cancer, *BLADDER cancer, *DISEASE relapse
Abstract

The availability of new potent systemic therapies for urothelial carcinoma may change the way we use standard chemotherapy perioperatively. In particular, identifying which patients with muscle-invasive bladder cancer (MIBC) would benefit from adjuvant chemotherapy (AC) is compelling. From a multicenter database we selected 950 patients with cT2–4N0M0 MIBC treated with radical cystectomy (RC), with or without neoadjuvant chemotherapy (NAC), and AC. We used Kaplan-Meier analyses to test 1-yr recurrence-free survival (RFS) rates according to AC use. Nomogram-derived probabilities of 1-yr recurrence after RC were plotted against actual recurrence rates according to AC use. Overall, we did not see evidence of an AC effect on the 1-yr RFS rate (p = 0.6). Conversely, the 1-yr RFS rate was higher among patients with pT3–4 or pN1 disease who received AC (75% vs 54%; p < 0.001). We were unable to demonstrate a difference between AC and no AC among patients who received prior NAC (1-yr RFS 57% vs 76%; p = 0.057). As the most important finding, AC was associated with incremental RFS benefits only for patients with a nomogram-derived 1-yr recurrence probability of >40%. Patient summary : Maximizing disease control with adjuvant chemotherapy was beneficial for patients with muscle-invasive bladder cancer who had a calculated recurrence risk of >40% and did not impact cancer recurrence in lower-risk disease. Therefore, patient stratification using the nomogram available for predicting recurrence is advisable pending external validation. Adjuvant chemotherapy after neoadjuvant treatment and radical cystectomy for muscle-invasive bladder cancer should be offered only to patients with a high risk of 1-yr recurrence. Time-based endpoints may be more useful to help data interpretation for the next adjuvant and neoadjuvant immunotherapy studies. [ABSTRACT FROM AUTHOR]

Published
2019
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18. Efficacy and safety outcomes of darolutamide in patients with non-metastatic castration-resistant prostate cancer with comorbidities and concomitant medications from the randomised phase 3 ARAMIS trial.

Author

Fizazi, Karim, Shore, Neal D., Smith, Matthew, Ramos, Rodrigo, Jones, Robert, Niegisch, Günter, Vjaters, Egils, Wang, Yuan, Srinivasan, Shankar, Sarapohja, Toni, and Verholen, Frank

Subjects
*DRUG efficacy, *STATISTICS, *ANTIANDROGENS, *DRUG tolerance, *POLYPHARMACY, *TREATMENT effectiveness, *CASTRATION-resistant prostate cancer, *RANDOMIZED controlled trials, *DESCRIPTIVE statistics, *STATISTICAL sampling, *DATA analysis, *DRUG side effects, *TERMINATION of treatment, *PATIENT safety, *COMORBIDITY, *OVERALL survival, *PROPORTIONAL hazards models
Abstract

In patients with non-metastatic castration-resistant prostate cancer (nmCRPC) in the Androgen Receptor Antagonizing Agent for Metastasis-free Survival (ARAMIS) trial, darolutamide significantly improved median metastasis-free survival by nearly 2 years and reduced the risk of death by 31% versus placebo, with a favourable safety/tolerability profile. This post hoc analysis of ARAMIS evaluated efficacy and safety in patients by number of comorbidities and concomitant medications. Patients with nmCRPC were randomised 2:1 to darolutamide (n = 955) or placebo (n = 554) while continuing androgen-deprivation therapy. Overall survival (OS) and treatment-emergent adverse events (TEAEs) were evaluated in subgroups by median numbers of ongoing comorbidities and concomitant medications. HRs were determined from univariate analysis using Cox regression. Median numbers of comorbidities and concomitant medications were 6 and 10, respectively, with 41.6% of patients having >6 comorbidities and 48.8% taking >10 concomitant medications. For patients with ≤ 6 and >6 comorbidities, darolutamide increased OS versus placebo (hazard ratio [HR] 0.65 and 0.73, respectively), and this benefit was consistent for cardiovascular, metabolic, and other comorbidities (HR range: 0.39–0.88). For patients taking ≤ 10 and >10 concomitant medications, increased OS was also observed with darolutamide versus placebo (HR 0.76 and 0.66, respectively), and the benefit was consistent across medication classes (HR range: 0.45–0.80). Incidences of TEAEs and TEAEs leading to treatment discontinuation with darolutamide were similar to placebo across subgroups by numbers of comorbidities and concomitant medications. The OS benefit and safety of darolutamide remained consistent with that observed in the overall ARAMIS population, even in patients with high numbers of comorbidities or concomitant medications. NCT02200614. Darolutamide increased overall survival versus placebo, and incidences of most adverse events were similar between treatments in patients with ≤ 6 or >6 comorbidities and those taking ≤ 10 or >10 concomitant medications. [Display omitted] • Patients with nmCRPC in ARAMIS had a substantial comorbidity burden. • Darolutamide provided consistent survival benefit across comorbidity subgroups. • Darolutamide improved survival independent of the number of concomitant medications. • Safety of darolutamide in these subgroups was consistent with overall population. [ABSTRACT FROM AUTHOR]

Published
2023
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19. Atezolizumab in Platinum-treated Locally Advanced or Metastatic Urothelial Carcinoma: Outcomes by Prior Number of Regimens.

Author

Perez-Gracia, Jose Luis, Loriot, Yohann, Rosenberg, Jonathan E., Powles, Thomas, Necchi, Andrea, Hussain, Syed A., Morales-Barrera, Rafael, Retz, Margitta M., Niegisch, Günter, Durán, Ignacio, Théodore, Christine, Grande, Enrique, Shen, Xiaodong, Wang, Jingjing, Nelson, Betty, Derleth, Christina L., and van der Heijden, Michiel S.

Subjects
*TRANSITIONAL cell carcinoma, *THERAPEUTIC use of monoclonal antibodies, *PLATINUM, *DRUG efficacy, *HEALTH outcome assessment, *THERAPEUTICS, *ATEZOLIZUMAB
Abstract

Background Patients with metastatic urothelial carcinoma (mUC) who progress after platinum-based chemotherapy have had few treatment options and uniformly poor outcomes. Atezolizumab (anti-programmed death-ligand 1) was approved in the USA for cisplatin-ineligible and platinum-treated mUC based on IMvigor210, a phase 2, single-arm, two-cohort study. Objective To evaluate the efficacy and safety of atezolizumab by the number of prior lines of systemic therapy in patients with pretreated mUC. Design, setting, and participants IMvigor210 enrolled 315 patients with mUC with progression during or following platinum-based therapy at 70 international sites between May 2014 and November 2014. Key inclusion criteria included age ≥18 yr, creatinine clearance ≥30 ml/min, and Eastern Cooperative Oncology Group performance status 0–1, with no limit on prior lines of treatment. Intervention Patients in this cohort received atezolizumab 1200 mg intravenously every 3 wk until loss of clinical benefit. Outcome measurements and statistical analysis Centrally assessed Response Evaluation Criteria In Solid Tumors v1.1 objective response rate (ORR), median duration of response, overall survival (OS), and adverse events were evaluated by prior treatment. Potential differences between subgroups were evaluated using log-rank (for OS) and chi-square (for ORR and adverse events frequencies) testing. Results and limitations Three hundred and ten patients were efficacy and safety evaluable (median follow-up, 21 mo). Objective responses and prolonged OS occurred across all prespecified subgroups; median duration of response was not reached in most subgroups. In patients without prior systemic mUC therapy (first-line subgroup), ORR was 25% (95% confidence interval: 14–38), and median OS was 9.6 mo (95% confidence interval: 5.9–15.8). No significant differences in efficacy or toxicity by therapy line were observed. Conclusions Atezolizumab demonstrated comparable efficacy and safety in previously treated patients with mUC across all lines of therapy evaluated. Patient summary We investigated effects of previous treatment in patients with metastatic urothelial carcinoma that progressed after platinum-based therapy. Atezolizumab was active and tolerable no matter how many treatment regimens patients had received. ClinicalTrials.gov, NCT02108652 . [ABSTRACT FROM AUTHOR]

Published
2018
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20. MTDH/AEG-1 contributes to central features of the neoplastic phenotype in bladder cancer.

Author

Nikpour, Mahnaz, Emadi-Baygi, Modjtaba, Fischer, Ute, Niegisch, Günter, Schulz, Wolfgang A., and Nikpour, Parvaneh

Subjects
*GENETIC transformation, *NEOPLASTIC cell transformation, *BLADDER cancer, *CANCER invasiveness, *BREAST cancer, *LIVER cancer, *OVARIAN cancer
Abstract

Abstract: Objectives: Carcinoma of the bladder is the fifth most common cancer whose incidence continues to rise. MTDH/AEG-1 is associated with the initiation and progression of many cancers including breast, hepatocellular, ovarian, and colorectal carcinomas. However, the expression and functional importance of MTDH/AEG-1 in bladder cancer remains unknown. The present study was aimed at exploring the functional role of MTDH/AEG-1 in selected bladder cancer cell lines. Methods and materials: The relative expression of MTDH/AEG-1 was assessed by real-time quantitative reverse transcription-polymerase chain reaction in several human bladder cancer cell lines as well as cancerous and benign bladder tissues. Then, expression of MTDH/AEG-1 in RT112 and 647V bladder cancer cell lines was knocked down by an RNA interference strategy. Cell viability and apoptosis were determined after treatment with specific interfering RNA. Potential effects of MTDG/AEG-1 specific interfering RNA on the cell cycle were investigated by flow cytometry. We also performed anchorage-independent growth and wound-healing assays to study MTDH/AEG-1 function. Results: Down-regulation of MTDH/AEG-1 did not significantly affect the cell cycle distribution but rather reduced cell viability via apoptosis, as evidenced by increased annexin V staining and caspase 3/7 activities as well as mitochondrial potential disruption. Of note, serum starvation did not exacerbate the effects of MTDH/AEG-1 knockdown. Furthermore, MTDH/AEG-1 down-regulation significantly decreased anchorage-independent growth and migration of bladder carcinoma cells. Conclusion: Overexpression of MTDH/AEG-1 contributes to the neoplastic phenotype of bladder cancer cells by promoting survival, clonogenicity, and migration. [Copyright &y& Elsevier]

Published
2014
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21. Corrigendum re: "Atezolizumab in Platinum-treated Locally Advanced or Metastatic Urothelial Carcinoma: Outcomes by Prior Number of Regimens" [Eur Urol 2018;73:462–8].

Author

Perez-Gracia, Jose Luis, Loriot, Yohann, Rosenberg, Jonathan E., Powles, Thomas, Necchi, Andrea, Hussain, Syed A., Morales-Barrera, Rafael, Retz, Margitta M., Niegisch, Günter, Durán, Ignacio, Théodore, Christine, Grande, Enrique, Shen, Xiaodong, Wang, Jingjing, Nelson, Betty, Derleth, Christina L., and van der Heijden, Michiel S.

Subjects
*UROLOGY, *FINGOLIMOD, *ADVISORY boards, *ATEZOLIZUMAB
Published
2019
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22. Targeting urothelial carcinoma cells by combining cisplatin with a specific inhibitor of the autophagy-inducing class III PtdIns3K complex.

Author

Schlütermann, David, Berleth, Niklas, Böhler, Philip, Deitersen, Jana, Stuhldreier, Fabian, Wallot-Hieke, Nora, Wu, Wenxian, Peter, Christoph, Stork, Björn, Skowron, Margaretha A., Hoffmann, Michèle J., and Niegisch, Günter

Subjects
*TRANSITIONAL cell carcinoma, *CISPLATIN, *AUTOPHAGY, *CANCER cells, *CELL survival, *ANTINEOPLASTIC agents, *APOPTOSIS, *BIOCHEMISTRY, *CELL lines, *CELL physiology, *DRUG resistance in cancer cells, *DRUG synergism, *PHENOMENOLOGY, *PHOSPHOTRANSFERASES, *CHEMICAL inhibitors, *PHARMACODYNAMICS, BLADDER tumors
Abstract

Background: Cisplatin-based regimens are routinely employed for the treatment of urothelial carcinoma. However, therapeutic success is hampered by the primary presence of or the development of cisplatin resistance. This chemoresistance is executed by multiple cellular pathways. In recent years, the cellular process of autophagy has been identified as a prosurvival pathway of cancer cells. On the one hand, autophagy enables cancer cells to survive conditions of low oxygen or nutrient supply, frequently found in tumors. On the other hand, autophagy supports chemoresistance of cancer cells. Here, we aimed at investigating the involvement of autophagy for cisplatin resistance in different urothelial carcinoma cell lines.Materials& Methods: We analyzed the expression levels of different autophagy-related proteins in cisplatin-sensitive and cisplatin-resistant urothelial carcinoma cell lines. Furthermore, we performed cell viability assays and caspase activity assays with cells treated with cisplatin, non-specific or specific autophagy inhibitors (chloroquine, 3-methyladenine, SAR405) or combinations thereof.Results: We found that autophagy-related proteins are up-regulated in different cisplatin-resistant urothelial carcinoma cells compared to the sensitive parental cell lines. Furthermore, inhibition of autophagy, in general, or of the autophagy-inducing class III PtdIns3K complex, in particular, sensitized both sensitive and resistant urothelial carcinoma cells to cisplatin-induced cytotoxic effects.Conclusion: We propose that targeting the autophagic machinery might represent a suitable approach to complement or even increase cisplatin efficacy in order to overcome cisplatin resistance in urothelial carcinoma. [ABSTRACT FROM AUTHOR]

Published
2018
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23. Applying the chicken embryo chorioallantoic membrane assay to study treatment approaches in urothelial carcinoma.

Author

Skowron, Margaretha A., Sathe, Anuja, Romano, Andrea, Hoffmann, Michèle J., Schulz, Wolfgang A., Van Koeveringe, Gommert A., Albers, Peter, Nawroth, Roman, and Niegisch, Günter

Subjects
*URINARY organ cancer treatment, *CHICKEN embryos, *XENOGRAFTS, *ANTINEOPLASTIC agents, *CISPLATIN, *ANIMAL experimentation, *GENETIC techniques, *URINARY organs, *TUMOR treatment, *TUMORS
Abstract

Background: Rapid development of novel treatment options demands valid preclinical screening models for urothelial carcinoma (UC). The translational value of high-throughput drug testing using 2-dimensional (2D) cultures is limited while for xenograft models handling efforts and costs often become prohibitive for larger-scale drug testing. Therefore, we investigated to which extent the chicken chorioallantoic membrane (CAM) assay might provide an alternative model to study antineoplastic treatment approaches for UC.Methods: The ability of 8 human UC cell lines (UCCs) to form tumors after implantation on CAMs was investigated. Epithelial-like RT-112 and mesenchymal-like T-24 UCCs in cell culture or as CAM tumors were treated with cisplatin alone or combined with histone deacetylase inhibitors (HDACi) romidepsin and suberanilohydroxamic acid. Tumor weight, size, and bioluminescence activity were monitored; tumor specimens were analyzed by histology and immunohistochemistry. Western blotting and quantitative real time polymerase chain reaction were used to measure protein and mRNA expression.Results: UCCs were reliably implantable on the CAM, but tumor development varied among cell lines. Expression of differentiation markers (E-cadherin, vimentin, CK5, CK18, and CK20) was similar in CAM tumors and 2D cultures. Cellular phenotypes also remained stable after recultivation of CAM tumors in 2D cultures. Bioluminescence images correlated with tumor weight. Cisplatin and HDACi decreased weight and growth of CAM tumors in a dose-dependent manner, but HDACi treatment acted less efficiently as in 2D cultures, especially on its typically associated molecular markers. Synergistic effects of HDACi and subsequent cisplatin treatment on UCCs were neither detected in 2D cultures nor detected in CAM tumors.Conclusion: Our results demonstrate that the CAM assay is a useful tool for studying tumor growth and response to conventional anticancer drugs under 3D conditions, especially cytotoxic drugs as cisplatin. With some limitations, it might serve as a cost- and time-effective preclinical screening assay for novel therapeutic approaches before further assessment in expensive and cumbersome animal models. [ABSTRACT FROM AUTHOR]

Published
2017
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