Ovarian Neoplasms Clinical Trial
Official title:
Phase II Randomized Trial of the Polo-like Kinase 1 Inhibitor BI 6727 Monotherapy Versus Investigator´s Choice Chemotherapy in Ovarian Cancer Patients Resistant or Refractory to Platinum-based Cytotoxic Therapy
This is an international, randomized phase II trial. The aim is to assess the efficacy and
the safety of BI 6727 Versus investigator's best choice single agent cytotoxic in recurrent
third and fourth lines platinum resistant/refractory ovarian cancer.
100 patients will be randomised at the study entry to receive either BI 6727 (Arm A: 50
patients) or non-platinum single agent cytotoxic (Arm B: 50 patients) Treatment will be
continued until disease progression or unacceptable toxicity. Primary endpoint: disease
control rate at week 24 according to Response Evaluation Criteria In Solid Tumours version
1.1.
Secondary endpoints: efficacy (progression free survival, overall survival, biological
tumour response, biological progression free survival assessed by serum CA 125 according to
Gynecologic Cancer Intergroup criteria, safety according to the NCI CTCAE v.3, disease
symptoms control assessed by the EORTC QLQ-C30, QLQ-OV28 and individual symptoms
questionnaires, pharmacokinetics of BI 6727.
Others endpoints: biomarkers and pharmacogenetics analysis (optional)
| Status | Completed |
| Enrollment | 110 |
| Est. completion date | June 2014 |
| Est. primary completion date | June 2014 |
| Accepts healthy volunteers | No |
| Gender | Female |
| Age group | 18 Years and older |
| Eligibility |
Inclusion criteria: 1. Confirmed recurrent epithelial ovarian carcinoma, peritoneal carcinoma or fallopian tube carcinoma. 2. Platinum resistant or platinum refractory disease. 3. Eastern Collaborative Oncology Group performance status < = 2. 4. Life expectancy > = 3 months. 5. At least one measurable lesion (Response Evaluation Criteria In Solid Tumours version 1.1). 6. Adequate hepatic, renal and bone marrow functions. 7. signed written informed consent prior to admission to the study. Exclusion criteria: 1. Contre-indications for cytotoxic treatment according to the Summary of Product Characteristics (Arm B). 2. Clinical evidence of active brain metastasis or leptomeningeal involvement. 3. Other malignancy currently requiring active therapy. 4. QTc prolongation according to Fridericia formula deemed clinically relevant by the investigator (e.g., congenital long QT syndrome, QTc according to Fridericia formula > 470 ms). 5. Hypersensitivity to one of the trial drugs or the excipients. 6. Serious illness or concomitant non- oncological disease. 7. Systemic anticancer therapy within 4 weeks before the start of the study. 8. Evidence of ileus sor sub ileus. |
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| Belgium | 1230.18.32003 Boehringer Ingelheim Investigational Site | Brussel | |
| Belgium | 1230.18.32004 Boehringer Ingelheim Investigational Site | Edegem | |
| Belgium | 1230.18.32002 Boehringer Ingelheim Investigational Site | Gent | |
| Belgium | 1230.18.32001 Boehringer Ingelheim Investigational Site | Leuven | |
| France | 1230.18.3321A Boehringer Ingelheim Investigational Site | Angers Cedex 9 | |
| France | 1230.18.3307A Boehringer Ingelheim Investigational Site | Bordeaux cedex | |
| France | 1230.18.3301A Boehringer Ingelheim Investigational Site | Caen | |
| France | 1230.18.3322A Boehringer Ingelheim Investigational Site | Lille Cedex | |
| France | 1230.18.3313A Boehringer Ingelheim Investigational Site | Lyon | |
| France | 1230.18.3312A Boehringer Ingelheim Investigational Site | Nantes cedex 02 | |
| France | 1230.18.3308A Boehringer Ingelheim Investigational Site | Nice cedex | |
| France | 1230.18.3302A Boehringer Ingelheim Investigational Site | Paris | |
| France | 1230.18.3314A Boehringer Ingelheim Investigational Site | Paris Cedex 20 | |
| France | 1230.18.3309A Boehringer Ingelheim Investigational Site | Pierre-Bénite cedex | |
| France | 1230.18.3305A Boehringer Ingelheim Investigational Site | Reims cedex | |
| France | 1230.18.3320A Boehringer Ingelheim Investigational Site | Saint-Brieuc cedex | |
| France | 1230.18.3311A Boehringer Ingelheim Investigational Site | Strasbourg | |
| France | 1230.18.3310A Boehringer Ingelheim Investigational Site | Toulouse Cedex 9 | |
| France | 1230.18.3315A Boehringer Ingelheim Investigational Site | Vandoeuvre les Nancy cedex | |
| Slovakia | 1230.18.42101 Boehringer Ingelheim Investigational Site | Bratislava | |
| Slovakia | 1230.18.42103 Boehringer Ingelheim Investigational Site | Poprad | |
| Spain | 1230.18.34006 Boehringer Ingelheim Investigational Site | Badalona | |
| Spain | 1230.18.34001 Boehringer Ingelheim Investigational Site | Barcelona | |
| Spain | 1230.18.34005 Boehringer Ingelheim Investigational Site | Barcelona | |
| Spain | 1230.18.34007 Boehringer Ingelheim Investigational Site | Girona | |
| Spain | 1230.18.34004 Boehringer Ingelheim Investigational Site | L'Hospitalet de Llobregat | |
| Spain | 1230.18.34002 Boehringer Ingelheim Investigational Site | Madrid | |
| Spain | 1230.18.34003 Boehringer Ingelheim Investigational Site | Madrid | |
| Sweden | 1230.18.46005 Boehringer Ingelheim Investigational Site | Linköping | |
| Sweden | 1230.18.46001 Boehringer Ingelheim Investigational Site | Stockholm | |
| Sweden | 1230.18.46003 Boehringer Ingelheim Investigational Site | Uppsala |
| Lead Sponsor | Collaborator |
|---|---|
| Boehringer Ingelheim |
Belgium, France, Slovakia, Spain, Sweden,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Disease Control Rate (DCR) at Week 24 According to Response Evaluation Criteria In Solid Tumours (RECIST) Version 1.1 | DCR was defined as the proportion of patients who had an overall response of complete response (CR), partial response (PR), or stable disease (SD). | Week 24 | No |
| Secondary | Progression Free Survival (PFS) | Progression-free survival of a patient was based on the investigator's assessment; it was defined as the number of days from the date of randomisation until the date of either disease progression or death from any cause, whichever occurred first. Definition of disease progression according to RECIST version 1.1; Patients with measurable tumour lesions at baseline, Target-lesions: at least a 20% increase in the sum of diameters of target lesions, the sum of diameters must also demonstrate an absolute increase of at least 5 mm,taking as reference the smallest sum on study, or appearance of 1 or more new lesions. Non-target lesions: unequivocal progression of existing non-target lesions or appearance of 1 or more new lesions Patients with non-measurable tumour lesions at baseline, Non-target lesions: requires unequivocal progression of existing non-target lesions or appearance of 1 or more new lesions |
From randomization until disease progression, death or study discontinuation; Up to 213 weeks | No |
| Secondary | Overall Survival (OS) | OS is defined as time from randomisation to death irrespective of the cause of the death. | From randomization until death or study discontinuation; Up to 213 weeks | No |
| Secondary | Best Overall Response | Best overall response (BOR) is defined as the best response recorded at any time from the date of randomisation until the end of treatment. Missing categories signify that no tumour imaging has been performed post baseline, and therefore the response status could not be assessed. |
time from the date of randomisation until study completion/discontinuation; Up to 213 weeks | No |
| Secondary | Biological Tumour Response Based on Serum Cancer Antigen 125 (CA-125) According to the Gynaecologic Cancer Intergroup (GCIG) Criteria | Patients were to have a pre-treatment CA-125 of at least twice the upper limit of normal to be considered for CA-125 response. Patients were not evaluable by CA-125 if they had received mouse antibodies or if they had undergone medical and/or surgical interference with their peritoneum or pleura during the previous 28 days. In eligible patients, a CA-125 response was defined as the moment the CA- 25 was reduced by 50%, with this being confirmed with a consecutive CA-125 assessment not earlier than 28 days after the previous one. Biological response rate based on serum CA-125 levels was assessed according to the guidelines by the Gynaecologic Cancer Intergroup. Monitoring of blood levels of the tumour marker CA-125 was performed at screening and every 6 weeks thereafter. |
At screening and every 6 weeks thereafter (Up to 213 weeks) | No |
| Secondary | Biological Progression-free Survival Based on Serum Cancer Antigen 125 (CA-125) According to the Gynaecologic Cancer Intergroup (GCIG) Criteria | Biological PFS including assessment of CA-125 levels was defined as the time from randomisation until the first occurrence of progressive disease according to CA-125, progressive disease according to radiological evidence, or death. Also according to the below criterias, In patients with radiological measurable disease, disease progression during study treatment could not be declared on the basis of CA-125 alone. Patients with elevated CA-125 pre-treatment and normalization of CA-125 had to show evidence of CA-125 = to two times the upper normal limit on two occasions at least one week apart or Patients with elevated CA-125 pre-treatment, which never normalized, had to show evidence of CA-125 = to two times the nadir value on two occasions at least one week apart or Patients with CA-125 in the normal range pre-treatment had to show evidence of CA-125 = to two times the upper normal limit on two occasions at least one week apart. |
At screening and every 6 weeks thereafter (Up to 213 weeks ) | No |
| Secondary | Time to Deterioration in Global Health Status/Quality of Life (QOL) | Time to deterioration in global health status/Quality of life (QOL) and symptom control assessed by the European Organisation for Research and Treatment of Cancer (EORTC) QLQ-C30, QLQ-OV28, and individual symptom questionnaires. The time to deterioration was defined as the time from randomisation to a score increased (i.e. worsened) by at least 10 points from baseline (0-100 point scale). If score is missing, and patient died within 28 days after scheduled time for completion, the patient was considered deteriorated. In this case, time to deterioration is time to death. |
Every 6 weeks (Up to 213 weeks ) | No |
| Secondary | Time to Deterioration in Fatigue/Quality of Life (QOL) | Time to deterioration in fatigue/Quality of life (QOL) and symptom control assessed by the European Organisation for Research and Treatment of Cancer (EORTC) QLQ-C30, QLQ-OV28, and individual symptom questionnaires. The time to deterioration was defined as the time from randomisation to a score increased (i.e. worsened) by at least 10 points from baseline (0-100 point scale). If score is missing, and patient died within 28 days after scheduled time for completion, the patient was considered deteriorated. In this case, time to deterioration is time to death. |
Every 6 weeks (Up to 213 weeks ) | No |
| Secondary | Time to Deterioration in Pain/ Quality of Life (QOL) | Time to deterioration in pain/ Quality of life (QOL) and symptom control assessed by the European Organisation for Research and Treatment of Cancer (EORTC) QLQ-C30, QLQ-OV28, and individual symptom questionnaires. The time to deterioration was defined as the time from randomisation to a score increased (i.e. worsened) by at least 10 points from baseline (0-100 point scale). If score is missing, and patient died within 28 days after scheduled time for completion, the patient was considered deteriorated. In this case, time to deterioration is time to death. |
Every 6 weeks (Up to 213 weeks ) | No |
| Secondary | Time to Deterioration in Abdominal Bloating/ Quality of Life (QOL) | Time to deterioration in abdominal bloating/ Quality of life (QOL) and symptom control assessed by the European Organisation for Research and Treatment of Cancer (EORTC) QLQ-C30, QLQ-OV28, and individual symptom questionnaires. The time to deterioration was defined as the time from randomisation to a score increased (i.e. worsened) by at least 10 points from baseline (0-100 point scale). If score is missing, and patient died within 28 days after scheduled time for completion, the patient was considered deteriorated. In this case, time to deterioration is time to death. |
Every 6 weeks (Up to 213 weeks ) | No |
| Secondary | Time to Deterioration in the Three Most Troublesome Disease Specific Symptoms/ Quality of Life (QOL) | Three most troublesome disease specific symptoms, defined by the patient at baseline. Patients that have defined more than 3 most troublesome symptoms have not been taken into account in the analysis. Quality of life (QOL) and symptom control assessed by the European Organisation for Research and Treatment of Cancer (EORTC) QLQ-C30, QLQ-OV28, and individual symptom questionnaires. The time to deterioration was defined as the time from randomisation to a score increased (i.e. worsened) by at least 10 points from baseline (0-100 point scale). If score is missing, and patient died within 28 days after scheduled time for completion, the patient was considered deteriorated. In this case, time to deterioration is time to death. |
Every 6 weeks (Up to 213 weeks) | No |
| Secondary | Incidence and Intensity of Adverse Events According to the United States National Cancer Institute (US NCI) Common Terminology Criteria for Adverse Events (CTCAE) Version 3.0 | Incidence and intensity of adverse events according to the United States National Cancer Institute (US NCI) Common Terminology Criteria for Adverse Events (CTCAE) version 3.0 | From first treatment administration to 21 days after the last drug administration (Up to 1403 days) | No |
| Secondary | Clinically Relevant Changes in Laboratory and ECG Data | Clinically relevant changes in laboratory and ECG data | From first treatment administration to 21 days after the last drug administration (Up to 1403 days) | No |
| Secondary | AUC (0-24); Area Under the Concentration-time Curve in Plasma Over the Time Interval From 0 to 24 Hours for BI 6727 BS | AUC (0-24); area under the concentration-time curve in plasma over the time interval from 0 to 24 hours for BI 6727 BS | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | AUC (0-24); Area Under the Concentration-time Curve in Plasma Over the Time Interval From 0 to 24 Hours for CD 10899 BS | AUC (0-24); area under the concentration-time curve in plasma over the time interval from 0 to 24 hours for CD 10899 BS (metabolite of Volasertib BI 6727) | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | AUC (0-inf); Area Under the Concentration-time Curve in Plasma Over the Time Interval From 0 Extrapolated to Infinity for BI 6727 BS | AUC (0-inf); area under the concentration-time curve in plasma over the time interval from 0 extrapolated to infinity for BI 6727 BS | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | AUC (0-inf); Area Under the Concentration-time Curve in Plasma Over the Time Interval From 0 Extrapolated to Infinity for CD 10899 BS | AUC (0-inf); area under the concentration-time curve in plasma over the time interval from 0 extrapolated to infinity for CD 10899 BS (metabolite of Volasertib BI 6727) | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Cmax; Maximum Measured Concentration of BI 6727 BS in Plasma | Cmax; maximum measured concentration of BI 6727 BS in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Cmax; Maximum Measured Concentration of CD 10899 BS in Plasma | Cmax; maximum measured concentration of CD 10899 BS (metabolite of Volasertib BI 6727) in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Tmax; Time From Dosing to Maximum Measured Concentration of BI 6727 BS in Plasma | tmax; time from dosing to maximum measured concentration of BI 6727 BS in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Tmax; Time From Dosing to Maximum Measured Concentration of CD 10899 BS in Plasma | tmax; time from dosing to maximum measured concentration of CD 10899 BS (metabolite of Volasertib BI 6727) in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | t1/2; Terminal Half-life of BI 6727 BS in Plasma | t1/2; Terminal half-life of BI 6727 BS in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | t1/2; Terminal Half-life of CD 10899 BS in Plasma | t1/2; Terminal half-life of CD 10899 BS in plasma | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | MRT; Mean Residence Time of BI 6727 BS in the Body | MRT; Mean residence time of BI 6727 BS in the body | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | CL; Total Clearance of BI 6727 BS in Plasma After Intravenous Administration | CL; total clearance of BI 6727 BS in plasma after intravenous administration | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Vss;Apparent Volume of Distribution at Steady State Following Intravenous Administration for BI 6727 BS | Vss;apparent volume of distribution at steady state following intravenous administration for BI 6727 BS | -0.083 hours (h), 2h, 4h, 6h, 24h, 168h and 336 h after first drug administration | No |
| Secondary | Biomarkers and Pharmacogenetics Analysis (Optional) | This endpoint has not been statistically analysed in the study report | 6 months | No |
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