UMIN-CTR Clinical Trial
| Unique ID issued by UMIN | UMIN000000951 |
|---|---|
| Receipt number | R000001143 |
| Scientific Title | Randomized phase II trial of irinotecan(CPT-11) plus tegafur/uracil with oral leucovorin(UFT/LV) compared with FOLFIRI in patients with unresectable/recurrent colorectal cancer |
| Date of disclosure of the study information | 2007/12/19 |
| Last modified on | 2015/10/21 17:10:53 |
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Basic information
Public title
Randomized phase II trial of irinotecan(CPT-11) plus tegafur/uracil with oral leucovorin(UFT/LV) compared with FOLFIRI in patients with unresectable/recurrent colorectal cancer
Acronym
KODK7 RPII
Scientific Title
Randomized phase II trial of irinotecan(CPT-11) plus tegafur/uracil with oral leucovorin(UFT/LV) compared with FOLFIRI in patients with unresectable/recurrent colorectal cancer
Scientific Title:Acronym
KODK7 RPII
Region
| Japan |
Condition
Condition
Patients with previously untreated and unresectable/recurrent colorectal cancer
Classification by specialty
| Gastrointestinal surgery |
Classification by malignancy
Malignancy
Genomic information
NO
Objectives
Narrative objectives1
To evaluate the efficacy and toxicity of CPT-11 plus UFT/LV compared with FOLFIRI in patients with unresectable/recurrent colorectal cancer at random as clinical phase 2 study.
Although the trial allow to use Bevacizumab together if the patient hope that, the group treated by Bevacizumab will be interrupted the entry when the enrollments run into 6 in each group and evaluate the toxicity (step 1).
When the step 1 trial will be finished and be confirmed the safety of Bevacizumab, get into the Step 2 and evaluate the efficacy and toxicity(step 2).
Basic objectives2
Safety,Efficacy
Basic objectives -Others
Trial characteristics_1
Confirmatory
Trial characteristics_2
Pragmatic
Developmental phase
Phase II
Assessment
Primary outcomes
Step1 Toxicity
Step2 Progression-free survival
Key secondary outcomes
Step2 Response rate, toxicity, Time to treatment failure, overall survival
Base
Study type
Interventional
Study design
Basic design
Parallel
Randomization
Randomized
Randomization unit
Individual
Blinding
Open -no one is blinded
Control
Active
Stratification
YES
Dynamic allocation
YES
Institution consideration
Institution is considered as adjustment factor in dynamic allocation.
Blocking
NO
Concealment
Central registration
Intervention
No. of arms
4
Purpose of intervention
Treatment
Type of intervention
| Medicine |
Interventions/Control_1
UFT is administered orally at 300mg/m2/day with 75mg/day of oral leucovorin for 21 consecutive days followed by a 7 days rest.
CPT-11 150mg/m2/day is given intravenously on day 1 and 15 of each cycle.
Cycles are repeated every 4 weeks, until occuring disease progression or severe toxicities.
Interventions/Control_2
The administration is done on the 1st day and the 15th day of each cycle. Cycles are repeated every 4 weeks, until occuring disease progression or severe toxicities.FOLFIRI consisted of CPT-11 150 mg/m2 IV over 90 minutes, LV 400 mg/m2 IV over 2 hours, and FU 400 mg/m2 IV bolus, followed by FU 2.400mg/m2 IV over a 46-hour infusion, repeated every 2 weeks.
Cycles are repeated every 4 weeks, until evidence of disease progression or severe toxicities.
Interventions/Control_3
UFT is administered orally at 300mg/m2/day with 75mg/day of oral leucovorin for 21 consecutive day followed by a 7 days rest.
CPT-11 and Bevacizumab are given intravenously on day 1 and 15 of each cycle.
Bevacizumab is added dilute to 100mL with physiological salt solution and given intravenously over 90 minutes. After the tolerability of the initial administration time is confirmed, the time can be shortened to 60 minutes.
After the tolerability of the second administration time is confirmed, the time can be shortened to 90 minutes.
After the administration of Bevacizumab, CPT-11 150mg/m2/day is given
Cycles are repeated every 4 weeks, until occurring disease progression or severe toxicities Cycles are repeated every 4 weeks, until occurring disease progression or severe toxicities.
Interventions/Control_4
The administration is done on the 1st day and the 15th day of each cycle. Cycles are repeated every 4 weeks, until occurring disease progression or severe toxicities. Bevacizumab is added dilute to 100mL with physiological salt solution and given intravenously over 90 minutes. When the tolerability of the initial administration time is acceptable, then the time can be shortened to 60 minutes.
After the tolerability of the second administration time is confirmed, the time can be shortened to 90 minutes.
5-FU and CPT-11 is given as follows.
FOLFIRI consists of CPT-11 150 mg/m2 over 90 minutes, LV 400 mg/m2 over 2 hours, and FU 400 mg/m2 bolus, followed by FU 2.400mg/m2 over a 46-hours infusion, repeated every 2 weeks.
Interventions/Control_5
Interventions/Control_6
Interventions/Control_7
Interventions/Control_8
Interventions/Control_9
Interventions/Control_10
Eligibility
Age-lower limit
| 20 | years-old | <= |
Age-upper limit
| 75 | years-old | >= |
Gender
Male and Female
Key inclusion criteria
1)colorectal cancer proven histologically
2) with measurable metastatic lesions
3) without prior chemotherapy or with chemotherapy which is completed before 6 months of registration
4) age: >=20 and <=75
5)Performance Status: 0-1 (ECOG)
6)more than 3 months of expected survival period
7)sufficient function of important organs
a) WBC: >=3,500/mm3 and <12,000/mm3
b) Neutrophyl: >=2,000/ mm3
c) Platelet: >=100,000/ mm3
d) Hemoglobin: >=9.0 g/dl
e) GOT, GPT: 2.5 times of normal range in each institute
f) sT.bil: <=1.5 mg/dl
g) sCreatinin: <=1.5 mg/dl
h) normal ECG
8)written informed consent
9)with ability of oral intake
Key exclusion criteria
1)with history of myocardial infarction, drug hypersensitivity within 6 months prior to the registration.
2) Prior ventral irradiation for colorectal cancer.
3)with active infection.
4)with intestinal paralysis, intestinal obstruction, interstitial pneumonitis or pulmonary fibrosis, uncontrolled diabetes mellitus, cardiac failure, renal failure, liver dysfunction, which disturb registration to this study.
5) Massive pleural or ascites that required drainage.
6)with brain metastasis.
7)with diarrhea.
8)with active double cancer.
9)patients receiving Flucytosine or Atazanabil.
10)with mental disorder which disturbs registration to this study.
11)pregnant or nursing women or women who like be pregnant.
12)men with partner willing to get pregnant.
13)patients receiving analgesic drug or steroids.
14)doctor's decision not to be registered to this study.
In addition to the above-mention, patients who hope to use Bevacizumab together has to be checked about the following factors.
1)Urine dipstick for proteinuria should be <2+
2)Patient with a past history of thrombosis, cerebral infarction, myocardial infarction, or pulmonary embolism.
3)Major surgical procedure, open biopsy, or clinically significant traumatic injury within 4 weeks.
4) History of gastrointestinal perforation, intestinal tract paralysis, or ileus within 1 year.
5) Long-term daily treatment with aspirin (>325 mg/day)
6) History of evidence of bleeding tendency or coagulopathy or defect of coagulation factor (INR>=1.5) or patient who taking anticoagulant agent.
Target sample size
72
Research contact person
Name of lead principal investigator
| 1st name | |
| Middle name | |
| Last name | Yuko Kitagawa |
Organization
Keio University School of Medicine
Division name
Department of Surgery
Zip code
Address
35, Shinanomachi, Shinjuku-ku, Tokyo, 160-8582
TEL
Public contact
Name of contact person
| 1st name | |
| Middle name | |
| Last name | Hirotoshi Hasegawa |
Organization
Keio University School of Medicine
Division name
Department of Surgery
Zip code
Address
35, Shinanomachi, Shinjuku-ku, Tokyo, 160-8582
TEL
03-3353-1211
Homepage URL
forum04@sc.itc.keio.ac.jp
Sponsor or person
Institute
Department of Surgery, School of Medicine, Keio University
Institute
Department
Personal name
Funding Source
Organization
None
Organization
Division
Category of Funding Organization
Self funding
Nationality of Funding Organization
Other related organizations
Co-sponsor
Name of secondary funder(s)
IRB Contact (For public release)
Organization
Address
Tel
Secondary IDs
Secondary IDs
NO
Study ID_1
Org. issuing International ID_1
Study ID_2
Org. issuing International ID_2
IND to MHLW
Institutions
Institutions
Other administrative information
Date of disclosure of the study information
| 2007 | Year | 12 | Month | 19 | Day |
Related information
URL releasing protocol
Publication of results
Partially published
Result
URL related to results and publications
Number of participants that the trial has enrolled
Results
Results date posted
Results Delayed
Results Delay Reason
Date of the first journal publication of results
Baseline Characteristics
Participant flow
Adverse events
Outcome measures
Plan to share IPD
IPD sharing Plan description
Progress
Recruitment status
No longer recruiting
Date of protocol fixation
| 2007 | Year | 11 | Month | 12 | Day |
Date of IRB
Anticipated trial start date
| 2007 | Year | 11 | Month | 01 | Day |
Last follow-up date
| 2015 | Year | 06 | Month | 15 | Day |
Date of closure to data entry
| 2015 | Year | 06 | Month | 15 | Day |
Date trial data considered complete
| 2015 | Year | 06 | Month | 15 | Day |
Date analysis concluded
| 2015 | Year | 09 | Month | 30 | Day |
Other
Other related information
Management information
Registered date
| 2007 | Year | 12 | Month | 19 | Day |
Last modified on
| 2015 | Year | 10 | Month | 21 | Day |
Link to view the page
Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000001143
