Your search keyword '"Coens, C. (Corneel)"' showing total 8 results

1. INTELLANCE 2/EORTC 1410 randomized phase II study of Depatux-M alone and with temozolomide vs temozolomide or lomustine in recurrent EGFR amplified glioblastoma

Author

Bent, M.J. (Martin) van den, Eoli, M. (Marica), Sepulveda, J.M. (Juan Manuel), Smits, M. (Marion), Walenkamp, A.M.E. (Annemiek M.), Frenel, J.-S. (Jean-Sebastian), Franceschi, C. (Claudio), Clement, P.M.J. (Paul), Chinot, O., De Vos, F. (Filip), Whenham, N. (Nicolas), Sanghera, P. (Paul), Weller, M. (Michael), Dubbink, H.J. (Erik Jan), French, P.J. (Pim), Looman, J. (Jim), Dey, J. (Jyotirmoy), Krause, S. (Scott), Ansell, P. (Pete), Nuyens, S. (Sarah), Spruyt, M. (Maarten), Brilhante, J. (Joana), Coens, C. (Corneel), Gorlia, T.S. (Thierry), Golfinopoulos, V. (Vassilis), Bent, M.J. (Martin) van den, Eoli, M. (Marica), Sepulveda, J.M. (Juan Manuel), Smits, M. (Marion), Walenkamp, A.M.E. (Annemiek M.), Frenel, J.-S. (Jean-Sebastian), Franceschi, C. (Claudio), Clement, P.M.J. (Paul), Chinot, O., De Vos, F. (Filip), Whenham, N. (Nicolas), Sanghera, P. (Paul), Weller, M. (Michael), Dubbink, H.J. (Erik Jan), French, P.J. (Pim), Looman, J. (Jim), Dey, J. (Jyotirmoy), Krause, S. (Scott), Ansell, P. (Pete), Nuyens, S. (Sarah), Spruyt, M. (Maarten), Brilhante, J. (Joana), Coens, C. (Corneel), Gorlia, T.S. (Thierry), and Golfinopoulos, V. (Vassilis)

Abstract

BACKGROUND: Depatuxizumab mafodotin (Depatux-M) is a tumor-specific antibody-drug conjugate consisting of an antibody (ABT-806) directed against activated epidermal growth factor receptor (EGFR) and the toxin monomethylauristatin-F. We investigated Depatux-M in combination with temozolomide or as a single agent in a randomized controlled phase II trial in recurrent EGFR amplified glioblastoma. METHODS: Eligible were patients with centrally confirmed EGFR amplified glioblastoma at first recurrence after chemo-irradiation with temozolomide. Patients were randomized to either Depatux-M 1.25 mg/kg every 2 weeks intravenously, or this treatment combined with temozolomide 150-200 mg/m2 day 1-5 every 4 weeks, or either lomustine or temozolomide. The primary endpoint of the study was overall survival. RESULTS: Two hundred sixty patients were randomized. In the primary efficacy analysis with 199 events (median follow-up 15.0 mo), the hazard ratio (HR) for the combination arm compared with the control arm was 0.71 (95% CI = 0.50, 1.02; P = 0.062). The efficacy of Depatux-M monotherapy was comparable to that of the control arm (HR = 1.04, 95% CI = 0.73, 1.48; P = 0.83). The most frequent toxicity in Depatux-M treated patients was a reversible corneal epitheliopathy, occurring as grades 3-4 adverse events in 25-30% of patients. In the long-term follow-up analysis with median follow-up of 28.7 months, the HR for the comparison of the combination arm versus the control arm was 0.66 (95% CI = 0.48, 0.93). CONCLUSION: This trial suggests a possible role for the use of Depatux-M in combination with temozolomide in EGFR amplified recurrent glioblastoma, especially in patients relapsing well after the end of first-line adjuvant temozolomide treatment. (NCT02343406).

Published

2020

2. Symptom clusters in newly diagnosed glioma patients: which symptom clusters are independently associated with functioning and global health status?

Author

Coomans, M.B., Dirven, L, Aaronson, N.K. (Neil), Baumert, B.G. (Brigitta), Bent, M.J. (Martin) van den, Bottomley, A. (Andrew), Brandes, A. (Alba), Chinot, O, Coens, C. (Corneel), Gorlia, T.S. (Thierry), Herrlinger, U, Keime-Guibert, F., Malmstrom, A, Martinelli, F, Stupp, R. (Roger), Talacchi, A., Weller, M. (Michael), Wick, W. (Wolfgang), Reijneveld, J.C., Taphoorn, MJ, Coomans, M.B., Dirven, L, Aaronson, N.K. (Neil), Baumert, B.G. (Brigitta), Bent, M.J. (Martin) van den, Bottomley, A. (Andrew), Brandes, A. (Alba), Chinot, O, Coens, C. (Corneel), Gorlia, T.S. (Thierry), Herrlinger, U, Keime-Guibert, F., Malmstrom, A, Martinelli, F, Stupp, R. (Roger), Talacchi, A., Weller, M. (Michael), Wick, W. (Wolfgang), Reijneveld, J.C., and Taphoorn, MJ

Abstract

Background. Symptom management in glioma patients remains challenging, as patients suffer from various concurrently occurring symptoms. This study aimed to identify symptom clusters and examine the association between these symptom clusters and patients’ functioning. Methods. Data of the CODAGLIO project was used, including individual patient data from previously published international randomized controlled trials (RCTs) in glioma patients. Symptom prevalence and level of functioning were assessed with European Organisation for Research and Treatment of Cancer (EORTC) quality of life QLQC30 and QLQ-BN20 self-report questionnaires. Associations between symptoms were examined with Spearman correlation coefficients and partial correlation networks. Hierarchical cluster analyses were performed to identify symptom clusters. Multivariable regression analyses were performed to determine independent associations between the symptom clusters and functioning, adjusted for possible confounders. Results. Included in the analysis were 4307 newly diagnosed glioma patients from 11 RCTs who completed the EORTC questionnaires before randomization. Many patients (44%) suffered from 5–10 symptoms simultaneously. Four symptom clusters were identified: a motor cluster, a fatigue cluster, a pain cluster, and a gastrointestinal/seizures/bladder control cluster. Having symptoms in the motor cluster was associated with decreased (≥10 points difference) physical, role, and

Published

2019

3. EORTC Gynecological Cancer Group on the frontline of practice-changing clinical trials

Author

Casado, A. (Antonio), Penninckx, B. (Björn), Reed, N.S. (Nick ), Burg, M.E.L. (Maria) van der, Berns, P.M.J.J. (Els), Katsaros, D. (Dionyssios), Ferrero, A. (Annamaria), Mota, T. (Tatiana), Jimeno, A. (Antonio), Vermorken, J.B. (Jan), Pecorelli, S. (Sergio), Coens, C. (Corneel), Vergote, I. (Ignace), Casado, A. (Antonio), Penninckx, B. (Björn), Reed, N.S. (Nick ), Burg, M.E.L. (Maria) van der, Berns, P.M.J.J. (Els), Katsaros, D. (Dionyssios), Ferrero, A. (Annamaria), Mota, T. (Tatiana), Jimeno, A. (Antonio), Vermorken, J.B. (Jan), Pecorelli, S. (Sergio), Coens, C. (Corneel), and Vergote, I. (Ignace)

Abstract

After more than 30 years of clinical and translational research, and having contributed to large randomized international clinical trials in gynecologic cancer, the multidisciplinary EORTC Gynecologic Cancer Group (GCG) currently is dealing with one of the greatest challenges in cancer research, which is to discover and establish clinically useful predictive and prognostic factors, to identify subgroups of patients based on genomic patterns and activated pathways and to design clinical trials appropriate for such subgroups. EORTC GCG current and future research has to include the validation of prognostic and predictive markers, the identification of novel therapies that target specific pathways, and a better understanding of the molecular basis for resistance. These studies will require the collection of large numbers of biologic specimens, both at time of diagnosis and at time of recurrence and, whenever possible, during treatment. These objectives can only be reached with transversal cooperation within the EORTC framework (Pathobiology group, Imaging group, etc.), as well as international cooperation. Support from private industry will also be important in the context of a high-standard cooperation among industry and academia. The EORTC with its unique multidisciplinary infrastructure and long experience in cancer research is taking part through the EORTC GCG in international networks focused on gynecological cancer research on a large scale. Intergroup collaboration and international contribution to establish the current and future world-wide standards of care is also a priority for the GCG. The GCG also has a good track record in rare tumors and will continue working on rare diseases along with international partners.

Published

2012

4. Health-related quality of life in non-small-cell lung cancer: An update of a systematic review on methodologic issues in randomized controlled trials

Author

Claassens, L. (Lily), Meerbeeck, J. (Jan) van, Coens, C. (Corneel), Quinten, C. (Chantal), Ghislain, I. (Irina), Sloan, E.K. (Elizabeth), Wang, X.S. (Xin Shelly), Velikova, G. (Galina), Bottomley, A. (Andrew), Claassens, L. (Lily), Meerbeeck, J. (Jan) van, Coens, C. (Corneel), Quinten, C. (Chantal), Ghislain, I. (Irina), Sloan, E.K. (Elizabeth), Wang, X.S. (Xin Shelly), Velikova, G. (Galina), and Bottomley, A. (Andrew)

Abstract

Purpose This study is an update of a systematic review of health-related quality-of-life (HRQOL) methodology reporting in non-small-cell lung cancer (NSCLC) randomized controlled trials (RCTs). The objective was to evaluate HRQOL methodology reporting over the last decade and its benefit for clinical decision making. Methods A MEDLINE systematic literature review was performed. Eligible RCTs implemented patientreported HRQOL assessments and regular oncology treatments for newly diagnosed adult patients with NSCLC. Included studies were published in English from August 2002 to July 2010. Two independent reviewers evaluated all included RCTs. Results Fifty-three RCTs were assessed. Of the 53 RCTs, 81% reported that there was no significant difference in overall survival (OS). However, 50% of RCTs that were unable to find OS differences reported a significant difference in HRQOL scores. The quality of HRQOL reporting has improved; both reporting of clinically significant differences and statistical testing of HRQOL have improved. A European Organisation for Research and Treatment of Cancer HRQOL questionnaire was used in 57% of the studies. However, reporting of HRQOL hypotheses and rationales for choosing HRQOL instruments were significantly less than before 2002 (P < .05). Conclusion The number of NSCLC RCTs incorporating HRQOL assessments has considerably increased. HRQOL continues to demonstrate its importance in RCTs, especially in those studies in which no OS difference is found. Despite the improved quality of HRQOL methodology reporting, certain aspects remain underrepresented. Our findings suggest need for an international standardization of HRQOL reporting similar to the CONSORT guidelines for clinical findings.

Published

2011

5. Neoadjuvant chemotherapy or primary surgery in stage IIIC or IV ovarian cancer

Author

Vergote, I. (Ignace), Tropé, C.G. (Claes ), Amant, F. (Frédéric), Kristensen, G.B. (Gunnar ), Ehlen, T. (Tom), Johnson, N. (Nichola), Verheijen, R.H.M. (René), Burg, M.E.L. (Maria) van der, Lacave, A.J., Panici, P.B. (Pierluigi Benedetti), Kenter, G.G. (Gemma ), Casado, A. (Antonio), Mendiola, C. (Cesar), Coens, C. (Corneel), Verleye, L. (Leen), Stuart, G.C.E. (Gavin ), Pecorelli, S. (Sergio), Reed, N.S. (Nick ), Vergote, I. (Ignace), Tropé, C.G. (Claes ), Amant, F. (Frédéric), Kristensen, G.B. (Gunnar ), Ehlen, T. (Tom), Johnson, N. (Nichola), Verheijen, R.H.M. (René), Burg, M.E.L. (Maria) van der, Lacave, A.J., Panici, P.B. (Pierluigi Benedetti), Kenter, G.G. (Gemma ), Casado, A. (Antonio), Mendiola, C. (Cesar), Coens, C. (Corneel), Verleye, L. (Leen), Stuart, G.C.E. (Gavin ), Pecorelli, S. (Sergio), and Reed, N.S. (Nick )

Abstract

BACKGROUND: Primary debulking surgery before initiation of chemotherapy has been the standard of care for patients with advanced ovarian cancer. METHODS: We randomly assigned patients with stage IIIC or IV epithelial ovarian carcinoma, fallopian-tube carcinoma, or primary peritoneal carcinoma to primary debulking surgery followed by platinum-based chemotherapy or to neoadjuvant platinum-based chemotherapy followed by debulking surgery (so-called interval debulking surgery). RESULTS: Of the 670 patients randomly assigned to a study treatment, 632 (94.3%) were eligible and started the treatment. The majority of these patients had extensive stage IIIC or IV disease at primary debulking surgery (metastatic lesions that were larger than 5 cm in diameter in 74.5% of patients and larger than 10 cm in 61.6%). The largest residual tumor was 1 cm or less in diameter in 41.6% of patients after primary debulking and in 80.6% of patients after interval debulking. Postoperative rates of adverse effects and mortality tended to be higher after primary debulking than after interval debulking. The hazard ratio for death (intention-to-treat analysis) in the group assigned to neoadjuvant chemotherapy followed by interval debulking, as compared with the group assigned to primary debulking surgery followed by chemotherapy, was 0.98 (90% confidence interval [CI], 0.84 to 1.13; P = 0.01 for non-inferiority), and the hazard ratio for progressive disease was 1.01 (90% CI, 0.89 to 1.15). Complete resection of all macroscopic disease (at primary or interval surgery) was the strongest independent variable in predicting overall survival. CONCLUSIONS: Neoadjuvant chemotherapy followed by interval debulking surgery was not inferior to primary debulking surgery followed by chemotherapy as a treatment option for patients with bulky stage IIIC or IV ovarian carcinoma in this study. Complete resection of all macroscopic disease, whether performed as primary treatment or after neoadjuvant chemotherapy

Published

2010

6. Promoter hypermethylation of FANCF and outcome in advanced ovarian cancer

Author

Lim, S.L., Smith, P., Syed, N., Coens, C. (Corneel), Wong, H., Burg, M. (Mirjam) van der, Szlosarek, P., Crook, T. (Tim), Green, J.A., Lim, S.L., Smith, P., Syed, N., Coens, C. (Corneel), Wong, H., Burg, M. (Mirjam) van der, Szlosarek, P., Crook, T. (Tim), and Green, J.A.

Abstract

The Fanconi gene family has a role in DNA repair and inactivation of FANCF has been proposed as a mechanism of sensitisation to platinum chemotherapy. This study sought to confirm this hypothesis in cell lines and a large series of ovarian cancer samples. Promoter methylation was assessed by methylation-sensitive polymerase chain reaction of FANCF in nine ovarian cancer cell lines and 74 ovarian cancer samples taken from patients entered on a trial of cisplatin-based chemotherapy. This study confirmed methylation-dependent silencing of FANCF in one out of nine ovarian cancer cell lines. Methylation of FANCF was demonstrated in 13.2% of 53 evaluable ovarian tumour samples. Progression-free survival gave an HR of 3.63 (95% CI: 1.54-8.54, P=0.0016) in favour of the unmethylated cases. There was no association with overall survival. This study does not support methylation-dependent silencing of FANCF as a mechanism of sensitisation to platinum-based chemotherapy in ovarian cancer.

Published

2008

7. Phase II study of bleomycin, vindesine, mitomycin C and cisplatin (BEMP) in recurrent or disseminated squamous cell carcinoma of the uterine cervix

Author

Luijk, I.F. van, Coens, C. (Corneel), Burg, M.E.L. (Maria) van der, Kobierska, A., Namer, M., Lhomme, C., Zola, P., Zanetta, G., Vermorken, J.B. (Jan), Luijk, I.F. van, Coens, C. (Corneel), Burg, M.E.L. (Maria) van der, Kobierska, A., Namer, M., Lhomme, C., Zola, P., Zanetta, G., and Vermorken, J.B. (Jan)

Abstract

Objective: We carried out a phase II trial with BEMP [bleomycin, vindesine (Eldisine®), mitomycin C and cisplatin] in patients with recurrent and/or metastatic squamous cell carcinoma of the uterine cervix with the specific aim to assess whether BEMP was of particular interest when certain disease sites were involved. Patients and methods: Eligible patients received four cycles of E 3 mg/m2, day 1 + 8; P 50 mg/m2, day 1; B 15 mg/day (continuous infusion), day 2-4 and M 8 mg/m2, day 5 (on alternate cycles), every 3 weeks during an induction phase. Thereafter, those without progression continued with MEP every 4 weeks in a maintenance phase. MEP consisted of E 3 mg/m2, day 1 + 8, M 6 mg/m2(on alternate cycles) and P 50 mg/m2, both on day 1. All drugs were given i.v. Both response evaluation and toxicity grading were assessed according to World Health Organization criteria. Results: Of the 161 eligible patients, 143 were assessable for survival, 148 for toxicity and 131 for response. Overall response rate was 45% [complete (CR) 14.5%, partial response (PR) 30.5%]. Most responsive disease sites were lung, lymph nodes and skin metastases (>60% response, CR rate >25%). Median duration of response was 7.6 months. Survival was significantly better in patients with only distant metastases: 12.9 months versus 8.6 months in those with other disease sites involved (P = 0.002). In a multivariate analysis, patients with a good performance status yielded a better prognosis (P = 0.0017), as did the patients with only metastatic disease compared with those who had pelvic disease also or solely (P = 0.045). There were two toxic deaths and 21% of patients stopped treatment because of excessive toxicity. Conclusions: Patients with a good performance status and only distant metastases seem optimal candidates to receive the BEMP regimen. This benefit should be balanced against the expected serious toxic effects.

Published

2007

8. The prognostic value of health-related quality-of-life data in predicting survival in glioblastoma cancer patients

Author

Mauer, M. (Murielle), Stupp, R. (Roger), Taphoorn, M.J. (Martin), Coens, C. (Corneel), Osoba, D. (David), Marosi, C. (Christine), Wong, R., Witte, O. de, Cairncross, J.G. (Gregory), Efficace, F. (Fabio), Mirimanoff, R.O., Forsyth, P., Bent, M.J. (Martin) van den, Weller, M. (Michael), Bottomley, A. (Andrew), Mauer, M. (Murielle), Stupp, R. (Roger), Taphoorn, M.J. (Martin), Coens, C. (Corneel), Osoba, D. (David), Marosi, C. (Christine), Wong, R., Witte, O. de, Cairncross, J.G. (Gregory), Efficace, F. (Fabio), Mirimanoff, R.O., Forsyth, P., Bent, M.J. (Martin) van den, Weller, M. (Michael), and Bottomley, A. (Andrew)

Abstract

This is one of the few studies that have explored the value of baseline symptoms and health-related quality of life (HRQOL) in predicting survival in brain cancer patients. Baseline HRQOL scores (from the EORTC QLQ-C30 and the Brain Cancer Module (BN 20)) were examined in 490 newly diagnosed glioblastoma cancer patients for the relationship with overall survival by using Cox proportional hazards regression models. Refined techniques as the bootstrap re-sampling procedure and the computation of C-indexes and R2- coefficients were used to try and validate the model. Classical analysis controlled for major clinical prognostic factors selected cognitive functioning (P=0.0001), global health status (P=0.0055) and social functioning (P<0.0001) as statistically significant prognostic factors of survival. However, several issues question the validity of these findings. C-indexes and R2-coefficients, which are measures of the predictive ability of the models, did not exhibit major improvements when adding selected or all HRQOL scores to clinical factors. While classical techniques lead to positive results, more refined analyses suggest that baseline HRQOL scores add relatively little to clinical factors to predict survival. These results may have implications for future use of HRQOL as a prognostic factor in cancer patients.

Published

2007