Efficacy and Tolerance Evaluation in FOLFIRINOX Dose Adjusted in Elderly Patients With a Metastatic Pancreatic Cancer
NCT ID: NCT02143219
Last Updated: 2022-07-28
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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COMPLETED
PHASE2
72 participants
INTERVENTIONAL
2014-07-31
2020-11-25
Brief Summary
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Although more hematologic (neutropenia) and GI toxicities were observed, FOLFIRINOX was acceptable as a new standard regimen for the majority of patients under the age of 70 with a good Performans Status. To reduce the toxicity of FOLFIRINOX in elderly patients (\> 70 yo), pharmacogenetic monitoring of 5-FU and Irinotecan key metabolism enzymes (DPD and UGTA1) may be easily performed. The methodology of the study is to use the Bryant \& Day statistical method, allowing to consider simultaneously as principal objective, the response rate (efficacy) and the tolerance (preservation of autonomy daily living, Katz index): this design is particularly fitting in a study for elderly patients who represent half of the pancreatic carcinoma population.
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Detailed Description
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Phase II study, opened, multicentric
MAIN OBJECTIVE :
The main objective is the simultaneous evaluation of the objective rate of answer and toxicity of her(it) of the protocol FOLFIRINOX administered to doses adapted at patients of 70 and more years old.
SECONDARY OBJECTIVE :
* Efficiency evaluation;
* Tolerance evaluation;
* Quality of Life (QoL) and clinical profit.
STATISTICAL ANALYSIS:
An analysis in two stages is planned, according to the method of Bryant and Day with a risk ß 5 % to reject wrongly an effective treatment and of acceptable toxicity and a risk a=10 % to accept wrongly a not rather effective or too toxic treatment.
The study will be considered as successful if:
* we obtain at least 11 tumoral answers and
* maxi 30 patients on 72 are in loss of autonomy (decrease of their ADL).
* All the patients who will have received at least an injection will be eligible for the evaluation of the toxicity
* The evaluation of the efficiency will be made after 3 cures at least unless early termination where the scanner will be anticipated.
* All the toxicity will be increased according to criteria of toxicity NCI-CTC v4.0.
* The evaluation of the tumoral answer (CR, PR and SD) will be made according to the criteria RECIST-v1.1.
Conditions
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Study Design
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NA
SINGLE_GROUP
TREATMENT
NONE
Study Groups
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FOLFIRINOX
FOLFIRINOX (D1-D15, for maximum 12 cycles) = Oxaliplatine + Folinic acid + Irinotecan + 5-FU
Oxaliplatine
Oxaliplatine : 85mg/m², 2-hours IV infusion (D1),
Folinic acid
Folinic acid (FA): 400 mg/m² , 2-hour IV infusion (D1),
Irinotecan
Irinotecan (at the dosage determined by the UGT1A1 status), 90 min IV infusion starting 30 min after the FA starts
* Homozygous 6/6 or 6/7: irinotecan will start at 150 mg/m², then will be increased according to clinical/biological tolerance by 10% steps, at each cycle, up to 180 mg/m² at max.
* Homozygous 7/7: irinotecan will start at 130 mg/m² in the first cycle then be increased up to a max of 150 mg/m², by 10% steps, according to tolerance.
5-FU
5-FU (according to the DPD pharmacogenetic status), continuous IV infusion of 46 hours, starting at the end of FA infusion:
* If no DPD deficiency, 5-FU start at 1600 mg/m² and can be modulated according to clinical/biological tolerance after each course, i.e., 1800 mg/m² the 2nd course and 2000 mg/m² the 3rd one
* If partial DPD deficiency: 5-FU start at 1200 mg/m² and can be increased up to 1800, then 2000 if the clinical/biological tolerance are good at the 2nd and 3rd course.
Interventions
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Oxaliplatine
Oxaliplatine : 85mg/m², 2-hours IV infusion (D1),
Folinic acid
Folinic acid (FA): 400 mg/m² , 2-hour IV infusion (D1),
Irinotecan
Irinotecan (at the dosage determined by the UGT1A1 status), 90 min IV infusion starting 30 min after the FA starts
* Homozygous 6/6 or 6/7: irinotecan will start at 150 mg/m², then will be increased according to clinical/biological tolerance by 10% steps, at each cycle, up to 180 mg/m² at max.
* Homozygous 7/7: irinotecan will start at 130 mg/m² in the first cycle then be increased up to a max of 150 mg/m², by 10% steps, according to tolerance.
5-FU
5-FU (according to the DPD pharmacogenetic status), continuous IV infusion of 46 hours, starting at the end of FA infusion:
* If no DPD deficiency, 5-FU start at 1600 mg/m² and can be modulated according to clinical/biological tolerance after each course, i.e., 1800 mg/m² the 2nd course and 2000 mg/m² the 3rd one
* If partial DPD deficiency: 5-FU start at 1200 mg/m² and can be increased up to 1800, then 2000 if the clinical/biological tolerance are good at the 2nd and 3rd course.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Metastatic disease
* First-line treatment : No previous chemotherapy in metastatic stage but adjuvant treatment before relapse (secondary metastatic) is permitted, provide it has been administered more than 6 months before)
* Age of 70 yo or above
* Normal DPD enzyme level or partial defect (excluding total defect)
* Adequate bone marrow reserve: as indicated by : neutrophils \>1500/mm3, platelets \>100,000/ mm3, Hb \>10.0g/dL.
* Adequate Renal function as indicated by: MDRD creatinine clearance \> 50ml/min.
* Adequate hepatic function as indicated by: serum bilirubin \< 1.5 times the upper limit of normal, AST and ALT \< 2.5 times the upper limit of normal, or \< 5 times the upper limit of normal if liver metastases are present.
* Written informed consent must be obtained prior to protocol-specific procedures are being performed
* Patient is affiliated to a social security category
Exclusion Criteria
* Non-metastatic but locally advanced pancreatic adenocarcinoma
* Complete DPD deficiency
* History of Cardiac failure or symptomatic coronary artery disease
* Autonomy Daily Living score by Katz \<4
* Prior treatment with FOLFIRINOX (adjuvant)
* Major comorbidity likely to be an obstacle to treatment
* Active or uncontrolled infection such as HIV or chronic B or C hepatitis
* Uncontrolled diabetes mellitus
* Prior peripheral neuropathy, grade \> 2
* Inflammatory bowel disease localized on the colon or rectum; bowel obstruction or severe uncontrolled diarrhea
* Previous or concomitant malignancies other than effectively treated carcinoma in situ of the cervix or non-melanoma skin cancer
* Hereditary fructose intolerance
* Persons deprived of liberty or under guardianship
* Any social, geographical or psychological condition which would compromise the ability to fully comply with the trial procedures and treatments
70 Years
ALL
No
Sponsors
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Institut Cancerologie de l'Ouest
OTHER
Responsible Party
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Principal Investigators
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Sandrine HIRET, MD
Role: PRINCIPAL_INVESTIGATOR
Institut de Cancérologie de l'Ouest (ICO) - Nantes, France
Locations
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ICO Paul Papin
Angers, , France
CH Vendée
La Roche-sur-Yon, , France
Centre Oscar Lambret
Lille, , France
ICM (Val d'Aurelle)
Montpellier, , France
Centre Eugène marquis
Rennes, , France
ICO René Gauducheau
Saint-Herblain, , France
Countries
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Other Identifiers
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2014-000539-17
Identifier Type: EUDRACT_NUMBER
Identifier Source: secondary_id
ICO-N-2014-01
Identifier Type: -
Identifier Source: org_study_id
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