Abstract
Background: Nilotinib is an oral tyrosine kinase inhibitor with high selectivity towards Bcr-Abl and approximately 30-fold more potent than imatinib, and is effective in patients with CML after imatinib failure. We initiated a phase II study to evaluate the efficacy of nilotinib as 1st line therapy in pts with newly diagnosed CML-CP.
Aims: To investigate the efficacy and safety of nilotinib as initial therapy for patients with CML-CP.
Methods: The primary objective was to estimate the proportion of pts attaining major molecular response (MMR) at 12 months (mo). Pts with untreated CML-CP (or with <1 months of therapy with imatinib) were eligible and received nilotinib 400mg twice daily. A cohort of patients with previously untreated CML in accelerated phase (AP) was also included.
Results: Forty-nine pts have been treated for a median of 13 months (mo). The median age was 47 years (yrs) (range, 21 to 81); 69% are Sokal low risk. Eight (16%) had received imatinib for <1 months. Overall, 46/48 (96%) of evaluable CP pts achieved a complete cytogenetic response [CCyR]. The rate of CCyR at 3, 6 and 12 mo for pts in CP compares favorably to those observed in historical controls treated with imatinib 400mg or 800 mg daily:
| . | Percent with CCyR (No. evaluable) . | . | ||
|---|---|---|---|---|
| Months on therapy . | Nilotinib . | Imatinib 400mg . | Imatinib 800mg . | P value . |
| 3 | 93 (45) | 37 (49) | 62 (202) | < 0.0001 |
| 6 | 100 (36) | 54 (48) | 82 (199) | < 0.0001 |
| 12 | 96 (27) | 65 (48) | 86 (197) | 0.0003 |
| 18 | 92 (12) | 68 (38) | 89 (179) | 0.0042 |
| 24 | 91 (11) | 70 (40) | 88 (173) | 0.0151 |
| . | Percent with CCyR (No. evaluable) . | . | ||
|---|---|---|---|---|
| Months on therapy . | Nilotinib . | Imatinib 400mg . | Imatinib 800mg . | P value . |
| 3 | 93 (45) | 37 (49) | 62 (202) | < 0.0001 |
| 6 | 100 (36) | 54 (48) | 82 (199) | < 0.0001 |
| 12 | 96 (27) | 65 (48) | 86 (197) | 0.0003 |
| 18 | 92 (12) | 68 (38) | 89 (179) | 0.0042 |
| 24 | 91 (11) | 70 (40) | 88 (173) | 0.0151 |
MMR was observed in 45% at 6 mo and 52% at 12 mo. Two of 44 (5%) evaluable pts have achieved confirmed complete molecular response, and 3 others unconfirmed (ie, only achieved on their last assessment). Grade 3–4 hematologic toxicity (transient) included thrombocytopenia in 10%, neutropenia in 12%, and anemia in 2%. Grade 3–4 non-hematologic adverse events (regardless of causality) included elevation of bilirubin in 8% and lipase in 6%. 19 (36%) pts had transient treatment interruptions and 17 (32%) had dose reductions. The actual median dose is 800mg daily. Three pts have come off study: 1 pt’s choice and 2 because of toxicity (1 liver, 1 pericardial effusion). One of them (liver toxicity) transformed to blast phase shortly after coming off study. Estimated 24 month EFS (event = loss of CHR, loss of MCyR, AP/BP, death, or off because of toxicity) is 95%.
Conclusion: Nilotinib 400 mg twice daily induces a CCyR in nearly all patients as early as 3 months after the start of therapy with a favorable toxicity profile. Accrual is ongoing.
Disclosures: Cortes:Novartis: Research Funding. Borthakur:Novartis: Speakers Bureau. Letvak:Novartis: Employment. Kantarjian:Novartis: Research Funding. Off Label Use: Nilotinib as frontline therapy for CML.
Author notes
Corresponding author
This feature is available to Subscribers Only
Sign In or Create an Account Close Modal