Efficacy of Nilotinib in First or Second Line Treatment of Primary Melanomas Stage III Unresectable Melanomas. (NILOMEL)

Assistance Publique - Hôpitaux de Paris

Status and phase

Unknown

Phase 2

Conditions

Amplification

Stage III Melanoma

Malignant Skin Melanoma T0

Stage IV Melanoma

Treatments

Drug: Nilotinib

Study type

Interventional

Funder types

Other

Identifiers

NCT01168050

P081237

Details and patient eligibility

About

NILOMEL is a phase II multicentric uncontrolled open national trial assessing the efficacy of Nilotinib in first or second line treatment of primary melanomas , stage III unresectable melanomas, or Stage IV melanomas with c-KIT mutation or amplification. The primary objective is overall response rate (partial and complete response) according to RECIST 1.1 criteria, assessed using CT-SCAN (stage IV melanoma) or MRI (unresectable melanoma) after 6 months therapy with Nilotinib 800 mg/d. Secondary objectives include:

Disease control rate (complete, partial response and stable disease)
Metabolic response
Tolerance NCI CTCAE Version 3.0
Biomarkers associated to response and disease control.

Full description

NILOMEL is a phase II multicentric uncontrolled open national trial assessing the efficacy of Nilotinib in first or second line treatment of primary melanomas , stage III unresectable melanomas, or Stage IV melanomas with c-KIT mutation or amplification (in case of c-KIT amplification, no B-RAF nor N-Ras mutation should be detected). The primary objective is overall response rate (partial and complete response) according to RECIST 1.1 criteria, assessed using CT-SCAN (stage IV melanoma) or MRI (unresectable melanoma) after 6 months therapy with Nilotinib 800 mg/d. Secondary objectives include:

Disease control rate (complete, partial response and stable disease) according to RECIST
Metabolic response rate (TEP-SCAN)
Tolerance NCI CTCAE Version 3.0
Biomarkers associated to response and disease control (evaluated at M0, M1 and M6). Protein analysis of c-KIT, PI3K, MAPK and STAT signalling pathways as well as PDGFR and Ephrin signalling pathways.

Patients with progressive disease after 3 months therapy will be withdrawn. Patient with stable disease after 3 months will continue Nilotinib until evaluation at 6 months. Patients with stable disease or progressive disease at 6 months will continue Nilotinib until progression.

The trial has been planned using a one-stage design (Fleming TR) . We considered that a response rate under 7.5% would define the null hypothesis of no efficacy . To detect a response rate of 30% or more with power 90% using a one-sided test at the 0.05 level, 25 patients have to be recruited.

Accrual for 2.5 years total study duration: 3 years

Enrollment

25 estimated patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patients with histologically proven melanoma with either c-KIT mutation or C-KIT amplification (without BRAF or NRAS mutation)
Unresectable primary or stage III or stage IV melanoma
Measurable disease (RECIST)
The inclusion of patients with primary tumor or metastasis accessible to sequential biopsies will be favored. If such lesions are present, biopsies are mandatory and not optional
No more than 1 previous specific therapy excluding tyrosine kinase inhibitors. 4 weeks wash out will be needed after cytotoxic therapy , 12 weeks wash out after anti -CTLA4 therapy or any immunological treatment
No radiotherapy within 4 weeks ; previously irradiated lesion will not be considered as measurable unless progression at inclusion
ECOG performance status < 2
WBC ≥ 3,000/mm³
PNN ≥ 1,500/mm³ (G-CSF allowed)
platelets ≥ 100,000/mm³
Hb ≥ 9.0 g/dL ( transfusions allowed as well as recombinant erythropoetin)
Creatinin clearance > 40ml/mn
Normal kalemia
Normal magnesemia
Total bilirubin <1.5N ; ASAT and ALAT <2.5N
PT/INR and PTT normal
NYHA class < 3
Signed Written Informed Consent
Affiliated to the National Health Insurance

Exclusion criteria

Patients refusal
Age < 18 years
Fertile women who do not want or cannot use effective contraception during the study and up to 8 weeks after the end of study
Women pregnant or nursing
Women with positive pregnancy test at inclusion or before treatment initiation
Fertile and sexually active men whose partner are fertile women who do not use effective contraception
Clinical and/or radiographic evidence of active cerebral metastases
Severe evolutive infection
Known HIV infection
Concomitant therapy with any other anti-cancer, immunomodulator or immunosuppressing agent or radiotherapy (except palliative care if bone metastases, after acceptance of principal investigator).
Previous use of tyrosine kinase inhibitors
More than one line of prior systemic therapies of melanoma by anti-cancer agent or immunotherapy.
Received experimental treatment within 4 weeks of inclusion
Pace-maker
Cardiac dysfunction, as evaluated by one of:
- Ejection fraction < 45% (less than 28 days from inclusion)
- Congenital prolonged QT
- QTc > 450 ms
- Ventricular tachyarrhythmia within the past 6 months
- Bradycardia at rest < 50/mn
- Major conduction dysfunction
- Myocardial infarction within the previous 6 months
- Unstable angina
Uncontrolled hypertension
Digestive disease that may inhibited NILITINIB absorption
Concomitant medication that may increase QT
Taking CYP3A4 inhibitors
Eating Sevilla oranges (or Sevilla oranges derivates), grapefruit (or grapefruit juice), grapes (or grapes juice), pomegranate (or pomegranate juice)
Hereditary galactose intolerance, Lapp-lactase deficiency or glucose-galactose malabsorption.