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Oxaliplatin and Cetuximab in First-line Treatment of Metastatic Colorectal Cancer (mCRC) (OPUS)

This study has been completed.
Sponsor:
Information provided by (Responsible Party):
Merck KGaA
ClinicalTrials.gov Identifier:
NCT00125034
First received: July 28, 2005
Last updated: August 23, 2011
Last verified: August 2011
History of Changes
Results First Received: August 23, 2011  
Study Type: Interventional
Study Design: Allocation: Randomized;   Endpoint Classification: Efficacy Study;   Intervention Model: Parallel Assignment;   Masking: Open Label;   Primary Purpose: Treatment
Conditions: Neoplasm Metastasis
Colorectal Cancer
Interventions: Biological: Cetuximab
Drug: Oxaliplatin

  Participant Flow
  Hide Participant Flow

Recruitment Details
Key information relevant to the recruitment process for the overall study, such as dates of the recruitment period and locations
First & last subject randomized: 27 Jul 2005 & 8 Mar 2006, respectively. Primary outcome and disease control rate cut-off dates 4 Aug 2006, others: 1 Mar 2007; except overall survival, KRAS overall survival and KRAS progression-free survival outcomes, metastatic surgery outcome and adverse events: 30 Nov 2008.

Pre-Assignment Details
Significant events and approaches for the overall study following participant enrollment, but prior to group assignment
629 subjects were prescreened, of whom 344 subjects were randomised. 338 subjects (Safety Population) received treatment. One subject was erroneously randomized, and was excluded from the ITT population (337 subjects).

Reporting Groups
  Description
Cetuximab Plus FOLFOX-4 Cetuximab plus 5-Fluorouracil(5-FU)/Folinic acid (FA) and oxaliplatin. Cetuximab will always be administered first, followed by oxaliplatin at least 1 hour later. Following completion of the oxaliplatin infusion or simultaneously with oxaliplatin FA will be administered (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day intravenously (IV) over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.
FOLFOX-4 Alone 5-FU/FA and oxaliplatin. Oxaliplatin will always be administered first or simultaneously with FA (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day IV over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.

Participant Flow:   Overall Study
    Cetuximab Plus FOLFOX-4     FOLFOX-4 Alone  
STARTED     170 [1]   168 [2]
COMPLETED     170     168  
NOT COMPLETED     0     0  
[1] Randomized & treated. 1 subject was not randomized correctly and was excluded in the ITT population.
[2] Randomized & treated



  Baseline Characteristics
  Hide Baseline Characteristics

Reporting Groups
  Description
Cetuximab Plus FOLFOX-4 Cetuximab plus 5-Fluorouracil(5-FU)/Folinic acid (FA) and oxaliplatin. Cetuximab will always be administered first, followed by oxaliplatin at least 1 hour later. Following completion of the oxaliplatin infusion or simultaneously with oxaliplatin FA will be administered (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day intravenously (IV) over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.
FOLFOX-4 Alone 5-FU/FA and oxaliplatin. Oxaliplatin will always be administered first or simultaneously with FA (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day IV over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.
Total Total of all reporting groups

Baseline Measures
    Cetuximab Plus FOLFOX-4     FOLFOX-4 Alone     Total  
Number of Participants  
[units: participants]
 		  169     168     337  
Age  
[units: participants]
 		     
<=18 years     0     0     0  
Between 18 and 65 years     96     109     205  
>=65 years     73     59     132  
Age  
[units: years]
Median ( Full Range ) 		  62.0  
  ( 24 to 82 )   		  60.0  
  ( 30 to 82 )   		  61.0  
  ( 24 to 82 )  
Gender  
[units: participants]
 		     
Female     80     76     156  
Male     89     92     181  
Region of Enrollment [1]
[units: participants]
 		     
Portugal     0     3     3  
Spain     19     16     35  
Ukraine     24     25     49  
Austria     16     9     25  
Russian Federation     25     24     49  
Israel     0     1     1  
Italy     8     6     14  
France     3     12     15  
Belgium     12     6     18  
Poland     30     31     61  
Romania     18     13     31  
Germany     14     22     36  
[1] Figures refer to randomized and treated participants



  Outcome Measures
  Show All Outcome Measures

1.  Primary:   Best Overall Response Rate - Independent Review Committee (IRC)   [ Time Frame: Evaluations were performed every 6 weeks until progression, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 4 August 2006 ]
  Show Outcome Measure 1

2.  Secondary:   Best Overall Response Rate (Chinese V-Ki-ras2 Kirsten Rat Sarcoma Viral Oncogene Homolog (KRAS) Wild-Type Population)   [ Time Frame: Evaluations were performed every 6 weeks until progression, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 1 Mar 2007 ]
  Show Outcome Measure 2

3.  Secondary:   Best Overall Response Rate (KRAS Mutant Population)   [ Time Frame: Evaluations were performed every 6 weeks until progression, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 1 Mar 2007 ]
  Show Outcome Measure 3

4.  Secondary:   Progression-free Survival Time   [ Time Frame: Time from randomisation to disease progression, death or last tumour assessment, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 01 Mar 2007 ]
  Show Outcome Measure 4

5.  Secondary:   Progression-free Survival Time (KRAS Wild-Type Population)   [ Time Frame: Time from randomisation to disease progression, death or last tumour assessment, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 Nov 2008 ]
  Show Outcome Measure 5

6.  Secondary:   Progression-free Survival Time (KRAS Mutant Population)   [ Time Frame: Time from randomisation to disease progression, death or last tumour assessment, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 Nov 2008 ]
  Show Outcome Measure 6

7.  Secondary:   Overall Survival Time   [ Time Frame: Time from randomisation to death or last day known to be alive, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 Nov 2008 ]
  Show Outcome Measure 7

8.  Secondary:   Overall Survival Time (KRAS Wild-Type Population)   [ Time Frame: Time from randomisation to death or last day known to be alive, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 November 2008 ]
  Show Outcome Measure 8

9.  Secondary:   Overall Survival Time (KRAS Mutant Population)   [ Time Frame: Time from randomisation to death or last day known to be alive, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 November 2008 ]
  Hide Outcome Measure 9

Measure Type Secondary
Measure Title Overall Survival Time (KRAS Mutant Population)
Measure Description Time from randomization to death. Patients without event are censored at the last date known to be alive or at the clinical cut-off date, whatever is earlier.
Time Frame Time from randomisation to death or last day known to be alive, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 November 2008  
Safety Issue No  

Population Description
Explanation of how the number of participants for analysis was determined. Includes whether analysis was per protocol, intention to treat, or another method. Also provides relevant details such as imputation technique, as appropriate.
KRAS Mutant population

Reporting Groups
  Description
Cetuximab Plus FOLFOX-4 Cetuximab plus 5-Fluorouracil(5-FU)/Folinic acid (FA) and oxaliplatin. Cetuximab will always be administered first, followed by oxaliplatin at least 1 hour later. Following completion of the oxaliplatin infusion or simultaneously with oxaliplatin FA will be administered (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day intravenously (IV) over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.
FOLFOX-4 Alone 5-FU/FA and oxaliplatin. Oxaliplatin will always be administered first or simultaneously with FA (at a dose of 200 mg/m^2, infused over 120 minutes, on day 1 and day 2, every two weeks) and then 5-FU (as a bolus of 400 mg/m^2/day IV over 2-4 minutes followed by 600 mg/m^2/day infused over 22-hour, on day 1 and day 2, every two weeks). Until progression or unacceptable toxicity develops. Safety population: includes all treated subjects.

Measured Values
    Cetuximab Plus FOLFOX-4     FOLFOX-4 Alone  
Number of Participants Analyzed  
[units: participants]
 		  77     59  
Overall Survival Time (KRAS Mutant Population)  
[units: months]
Median ( 95% Confidence Interval ) 		  13.4  
  ( 10.5 to 17.7 )   		  17.5  
  ( 14.7 to 24.8 )  


Statistical Analysis 1 for Overall Survival Time (KRAS Mutant Population)
Groups [1] All groups
Method [2] Stratified log rank
P Value [3] 0.2004
Hazard Ratio (HR) [4] 1.290
95% Confidence Interval ( 0.873 to 1.906 )
[1] Additional details about the analysis, such as null hypothesis and power calculation:
  No text entered.
[2] Other relevant information, such as adjustments or degrees of freedom:
  Kaplan-Meier method used to estimate median OS time. HR was calculated using Cox proportional hazards model stratified by randomization strata.
[3] Additional information, such as whether or not the p-value is adjusted for multiple comparisons and the a priori threshold for statistical significance:
  No text entered.
[4] Other relevant estimation information:
  No text entered.



10.  Secondary:   Participants With No Residual Tumor After Metastatic Surgery   [ Time Frame: Time from first dose up to 30 days after the last dose of study treatment, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 30 November 2008 ]
  Show Outcome Measure 10

11.  Secondary:   Disease Control Rate (Cut Off Date 4 August 2006)   [ Time Frame: Evaluations were performed every 6 weeks until progression, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 4 August 2006 ]
  Show Outcome Measure 11

12.  Secondary:   Duration of Response   [ Time Frame: Time from first assessment of Complete Response or Partial Response to disease progression,death or last tumor assessment, reported between day of first patient randomised, 27 Jul 2005, until cut-off date 01 Mar 2007 ]
  Show Outcome Measure 12

13.  Secondary:   Safety - Number of Patients Experiencing Any Adverse Event   [ Time Frame: time from first dose up to 30 after last dose of study treatment, reported between day of first patient dose of study treatment, 27 Jul 2005, until cut-off date 30 Nov 2008 ]
  Show Outcome Measure 13


  Serious Adverse Events
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  Other Adverse Events
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  More Information
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Certain Agreements:  
Principal Investigators are NOT employed by the organization sponsoring the study.
There IS an agreement between Principal Investigators and the Sponsor (or its agents) that restricts the PI's rights to discuss or publish trial results after the trial is completed.
The agreement is:
unchecked The only disclosure restriction on the PI is that the sponsor can review results communications prior to public release and can embargo communications regarding trial results for a period that is less than or equal to 60 days. The sponsor cannot require changes to the communication and cannot extend the embargo.
unchecked Other disclosure agreement that restricts the right of the PI to discuss or publish trial results after the trial is completed.


Limitations and Caveats
Limitations of the study, such as early termination leading to small numbers of participants analyzed and technical problems with measurement leading to unreliable or uninterpretable data
A non-specific outcome measure 'Safety' was deleted from this entry in error. A replacement outcome has been created. The 'Safety' outcome refers to adverse events and these are shown in the 'Adverse Events' section.  


Results Point of Contact:  
Name/Title: Inmaculada Ollero/Clinical Trial Manager
Organization: Merck Serono
phone: +34935655433
e-mail: iollero@merck.es


Publications of Results:


Responsible Party: Merck KGaA
ClinicalTrials.gov Identifier: NCT00125034     History of Changes
Other Study ID Numbers: EMR 62202-047
Study First Received: July 28, 2005
Results First Received: August 23, 2011
Last Updated: August 23, 2011
Health Authority: Germany: Federal Institute for Drugs and Medical Devices