UMIN-CTR Clinical Trial

Public title

Pharmacogenomic study on colorectal cancer chemotherapy - modified FOLFOX6- (Oxaliplatin with infusional 5-FU/l-Leucovorin) and
FOLFIRI (irinotecan with infusional 5-FU/l-Leucovorin)-based regimen-

Acronym

Pharmacogenomic study on colorectal cancer chemotherapy

Scientific Title

Pharmacogenomic study on colorectal cancer chemotherapy - modified FOLFOX6- (Oxaliplatin with infusional 5-FU/l-Leucovorin) and
FOLFIRI (irinotecan with infusional 5-FU/l-Leucovorin)-based regimen-

Scientific Title:Acronym

Pharmacogenomic study on colorectal cancer chemotherapy

Region

Japan

Condition

Colorectal cancer

Classification by specialty

Gastrointestinal surgery

Classification by malignancy

Malignancy

Genomic information

YES

Narrative objectives1

To assess the efficacy and safety of modified FOLFOX6 and FOLFIRI with or without Bevacizmab for Stage IV unresectable colorectal cancer: Multicentric phase II randomized study. Predictive formulaes for CPT11 and mFOLFOX6 that have been developed for tailored-therapy will be validated for their possibility of application. Novel biomarker candidates will also be explored for these therapies.

Basic objectives2

Safety,Efficacy

Basic objectives -Others

Trial characteristics_1

Exploratory

Trial characteristics_2

Pragmatic

Developmental phase

Phase II

Primary outcomes

Response rate (RECISTv1.1)

Key secondary outcomes

Evaluation of efficacy and safety.
(1) Overall response duration, Complete response duration, Stable duration
(2)Progression free survival
(3)Time to treatment failure
(4)Survival: Overall survival, OS, Median survival Time, 1-year survival, 2-year survival
(5) Toxicity profiles, frequency, grade, timing

Feasibility of novel and known biomarkers
(1)Feasibility of novel biomarkers for prediction of response
(2) Feasiblity of known biomarkers for prediction of efficacy or adverse effects
(3) Establishment of new predictive markers,

Study type

Interventional

Basic design

Parallel

Randomization

Randomized

Randomization unit

Individual

Blinding

Open -no one is blinded

Control

Uncontrolled

Stratification

Dynamic allocation

YES

Institution consideration

Institution is considered as adjustment factor in dynamic allocation.

Blocking

NO

Concealment

Central registration

No. of arms

4

Purpose of intervention

Treatment

Type of intervention

Medicine

Interventions/Control_1

mFOLFOX6 (-BEV):
On Day1, iv infusion of 85 mg/m2 of l-OHP and 175 mg/m2 of L-LV for 2hrs, followed by bolus infusion of 400 mg/m2 5-FU. Then, continuous infusion of 2400 mg/m2 5-FU for 46 hrs. 1 course, 2 weeks. Continue the courses till the discontinuance criteria.

Interventions/Control_2

mFOLFOX6 (+BEV):
The first treatment after the surgery is subject to the mFOLFOX6 (-BEV) regimen. From the 2nd cycle, first infusion of 5 mg/kg BEV. Then follow the mFOLFOX6 (-BEV) regimen. 1 course, 2 weeks. Continue the courses till the discontinuance criteria.

Interventions/Control_3

mFOLFIRI(-BEV):
On Day1, iv infusion of 150 mg/m2 of CPT-11 and 175 mg/m2 of L-LV for 2 hrs, followed by bolus infusion of 400 mg/m2 5-FU. Then, continuous infusion of 2400 mg/m2 5-FU for 46 hrs. 1 course, 2 weeks. Continue the courses till the discontinuance criteria.

Interventions/Control_4

mFOLFIRI (+BEV):
The first treatment after the surgery is subject to the FOLFIRI (-BEV) regimen. From the 2nd cycle, first infusion of 5 mg/kg BEV. Then follow the FOLFIRI (-BEV) regimen. 1 course, 2 weeks. Continue the courses till the discontinuance criteria.

Interventions/Control_5

Interventions/Control_6

Interventions/Control_7

Interventions/Control_8

Interventions/Control_9

Interventions/Control_10

Age-lower limit

20

years-old

<=

Age-upper limit

Not applicable

Gender

Male and Female

Key inclusion criteria

1) Histologically confirmed colorectal cancer.
2) Stage IV unresectable case.
3) The patient must have measurable disease (RECIST)
4) Patient must have appropriate organ function (bone marrow, liver, kidney, cardiac, etc.) and the laboratory value within 7 days before the protocol treatment must be
WBC 4,000/mm3 or more
ANC 2,000/mm3 or more
Platelet 100,000/mm3 or more
Hemoglobin 9.0g/dl or more
AST, ALT x2 institutional ULN or less
(For the liver metastatic cases, x3 institutional ULN or less)
Serum Total Bilirubin 1.5 mg/dL or less
Serum Creatinine 1.5 mg/dL or less
Creatinine clearance 60 ml/min or more
BUN 25mg/dl or less
ECG Normal
5) ECOG Performance Status 0-2
6) Any therapy should not have been given for the current disease.
7) Protocol treatment must be started within 6 weeks after surgery.
8) Collected tissue sample must be enough for genomic analysis.
9) Life expectancy must be 12 weeks or more at the time of registration.
10) Age 20 years or older
11) Written informed consent must be obtained for the study including blood or tissue sampling.

Key exclusion criteria

1) Patients with obvious infectious disease.
2) Patients with watery diarrhea.
3) Patients with intestinal paralysis, obstruction, or subobstruction of bowel (At the time of registration)
4) Patients with interstitial pneumonia or pulmonary fibrosis
5) Patients with considerable cancerous body cavity fluid.
6) Patients with severe paresthesia of functional disorder or dysesthesia
7) Patients with peripheral (sensory or motor) neuropathy Grade 2 or greater (CTCAEv4.0).
8) Patients with treatment-required ischemic heart disease or cardiac disease such as arrhythmia (left ventricular hypertrophy associated with hypertension, mild left ventricular over-loading, or mild right bundle branch block etc. are acceptable for registration)
9) Patients with history of myocardial infarction within 6 months
10) Patients with liver cirrhosis
11) Patients with active bleeding at bowel with necessity for frequent transfusion
12) Patients with clinically serious psycho-neurological disease required for continuation therapy using psychotropic drug
13) Patients with uncontrollable diabetes
14) Patients with active double cancer
15) Patients with history of severe hypersensitivitie for other drugs
16) Patients required for continuous administration of phenytoin
17) Patients with obvious intraperitoneal inflammation
18) Patients with uncured surgical wound of serious operation
19) Patients with congenital hemorrhagic diathesis
20) Patients with administration of anticoagulant such as warfarin potassium
21) Patients with history of thromboembolism
22) Patients who are pregnant or breast feeding or possibility of pregnancy
23) Patients with severe comorbidity who are difficult for continuation of the protocol treatment

Target sample size

210

Name of lead principal investigator

1st name
Middle name
Last name	Masahiko Nishiyama

Organization

Saitama Medical University

Division name

Frontier Medical Development Center

Zip code

Address

1397-1 Yamane, Hidaka, Saitama 350-1298, Japan

TEL

042-984-4668

Email

Name of contact person

1st name
Middle name
Last name	Masahiko Nishiyama

Organization

Saitama Medical University

Division name

Frontier Medical Development Center

Zip code

Address

1397-1 Yamane, Hidaka, Saitama 350-1298, Japan

TEL

042-984-4668

Homepage URL

Email

yamacho@saitama-med.ac.jp

Institute

Personalized Medicine Study Group for Cancer

Institute

Department

Personal name

Organization

None

Organization

Division

Category of Funding Organization

Self funding

Nationality of Funding Organization

Co-sponsor

Name of secondary funder(s)

Organization

Address

Tel

Email

Secondary IDs

YES

Study ID_1

DOFMET Protocol #5

Org. issuing International ID_1

Development Organization for Frontier Medical Therapeutics

Study ID_2

Org. issuing International ID_2

IND to MHLW

Institutions

九州大学大学院医学研究院・消化器総合外科学 （福岡県）、
熊本大学大学院生命科学研究部・消化器外科学　（熊本県）、
鹿児島大学大学院医歯学総合研究科・腫瘍制御学・消化器外科学　（鹿児島県）、
ICSG (Individualized Chemotherapy Study Group)
　関西労災病院・外科　（兵庫県）
　市立堺病院・外科　（大阪府）
　市立吹田市民病院・外科・消化器内科　（大阪府）
　大阪府立成人病センター・消化器外科，臨床腫瘍科　（大阪府）
　兵庫医科大学・下部消化器外科　（兵庫県）
　　医療法人薫風会 佐野病院　（兵庫県）、
岐阜大学大学院医学研究科・腫瘍外科学　（岐阜県）、
北里大学医学部・外科学　（神奈川県）、
帝京大学ちば総合医療センター・外科　（千葉県）、
群馬大学大学院医学研究科病態総合外科学　（群馬県）、
埼玉医科大学総合医療センター・消化管・一般外科　（埼玉県）、
岩手医科大学・外科学　（岩手県）、
埼玉医科大学先端医療開発センター　（埼玉県）

Date of disclosure of the study information

2011

Year

12

Month

19

Day

URL releasing protocol

Publication of results

Unpublished

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

Recruitment status

Completed

Date of protocol fixation

2011

Year

09

Month

29

Day

Date of IRB

2011

Year

11

Month

25

Day

Anticipated trial start date

2011

Year

12

Month

01

Day

Last follow-up date

2015

Year

12

Month

01

Day

Date of closure to data entry

2016

Year

01

Month

30

Day

Date trial data considered complete

2016

Year

01

Month

30

Day

Date analysis concluded

2016

Year

01

Month

30

Day

Other related information

Registered date

2011

Year

12

Month

19

Day

Last modified on

2019

Year

06

Month

25

Day

Link to view the page

Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000008162