The development of dasatinib as a treatment for chronic myeloid leukemia (CML): from initial studies to application in newly diagnosed patients

The efficacy of oral dasatinib was first assessed in a phase I, open-label, dose-escalation study (Table 1). Patients (n = 84) with various phases of CML or Ph+ ALL intolerant or resistant to imatinib received oral dasatinib (15–240 mg/day) once or twice daily in 4-week treatment cycles (Talpaz et al. 2006). Dasatinib had clinical activity in all CML phases and Ph+ ALL. Complete hematologic response (CHR) was achieved in 92 % of patients (37/40) with CML-CP, and major hematologic response (MHR) was seen in 70 % of patients (31/44) with CML-AP, CML-BP, or Ph+ ALL. The rates of major cytogenetic response (MCyR) were 45 % (18/40) in patients with CML-CP and 43 % (19/44) in patients with CML-AP, CML-BP, or Ph+ ALL. Of note, imatinib-associated side effects, including muscle cramps and nausea, were infrequent with dasatinib, and patients intolerant to imatinib did not have recurrence of the same nonhematologic adverse events (AEs) (e.g., rash and liver function abnormalities) with dasatinib treatment. The major AE associated with dasatinib was reversible myelosuppression. Because dasatinib has a relatively short half-life (3–5 h) (Sprycel^® BMS 2013; Wang et al. 2013), the probability of achieving more continuous BCR–ABL inhibition was thought to be increased by twice-daily dosing (Shah et al. 2010); however, once-daily regimens of dasatinib had similar rates of hematologic and cytogenetic response compared with twice-daily regimens and lower rates of AEs supported by a recent retrospective dasatinib exposure–response analysis (Saglio et al. 2010b; Shah et al. 2008a, 2010; Wang et al. 2013).

A series of phase II trials, the pivotal START (SRC–ABL Tyrosine kinase inhibition Activity Research Trials) trial program (Table 1), followed the phase I dose-escalation study. The primary objective for these trials was to treat patients with resistance or intolerance to imatinib who therefore had a life-threatening medical need. As the pharmacokinetics of the dasatinib 70 mg twice-daily regimen were better understood, it was selected as the preferred dosing option in these patients. These open-label, multicenter trials established the efficacy and safety of second-line dasatinib (70 mg twice daily) in the treatment of imatinib-resistant or imatinib-intolerant patients with CML (all phases) or Ph+ ALL. Data from this program led to the initial approval of dasatinib in these indications.

Two START studies assessed second-line dasatinib 70 mg twice daily in patients with CML-CP. START-C was a single-arm study, and START-R was a randomized, parallel-arm study of dasatinib versus high-dose imatinib (800 mg/day) in patients resistant to standard dose imatinib (Hochhaus et al. 2007, 2008; Kantarjian et al. 2007, 2009a; Mauro et al. 2008). In START-C (N = 387), dasatinib induced MCyR (primary end point) in 62 % of patients after a minimum follow-up of 24 months (Mauro et al. 2008). The corresponding CCyR rate was 53 %. In START-R, rates of MCyR were 53 % in the dasatinib 70 mg twice-daily arm (n = 101) and 33 % in the high-dose imatinib arm (n = 49) (p = 0.017) after a minimum follow-up of 24 months (Kantarjian et al. 2009a). CCyR rates were 44 and 18 %, respectively (p = 0.0025). Although no formal statistical comparison between the study arms was planned, the data suggested relatively greater efficacy for dasatinib compared with imatinib (Kantarjian et al. 2009a). These responses were also durable, as a pooled analysis (N = 387) of the START-C and START-R studies showed that 90 % of patients achieving a CCyR maintained this level of response after 24 months (Baccarani et al. 2008). START-A, START-B, and START-L were single-arm studies of second-line dasatinib 70 mg twice daily in patients with CML-AP, CML-BP, and CML-BP/Ph+ ALL, respectively (Apperley et al. 2009; Cortes et al. 2007a, 2008; Guilhot et al. 2007; Ottmann et al. 2007; Saglio et al. 2008). In the START-A trial (N = 174), after a median follow-up of 14.1 months, 64 % of patients with CML-AP achieved the primary end point of MHR and 45 % achieved a CHR (Apperley et al. 2009). START-B included patients with myeloid CML-BP (N = 109), and START-L included patients with lymphoid CML-BP (n = 48) and a subset of patients with Ph+ ALL (Cortes et al. 2007a). After a minimum follow-up of 24 months, a CHR was achieved in 26 % of patients with myeloid CML-BP and in 29 % of patients with lymphoid CML-BP (Saglio et al. 2008).

The recommended starting dose for dasatinib in patients with CML-CP is now 100 mg once daily (EMA Sprycel^® [dasatinib] 2012; Sprycel^® BMS 2013) following the results of a phase III dose-optimization study showing that 100 mg once daily was associated with similar efficacy as the twice-daily regimen, but with a reduction in toxicity (Shah et al. 2008a). Although the dasatinib half-life of 3–5 h (Sprycel^® BMS 2013) was used as a basis for the initial twice-daily dosing regimen, transient exposure of CML cell lines to dasatinib in vitro has been demonstrated to induce apoptosis (Shah et al. 2008b), supporting the feasibility of once-daily dosing, and data from the phase I study suggested that once-daily and twice-daily dose schedules were associated with similar response rates (Talpaz et al. 2006). Furthermore, due to dose reductions in the START-C and START-R studies, the median total daily dose delivered to patients approximated 100 mg/day (Hochhaus et al. 2007; Kantarjian et al. 2007). It was therefore proposed to compare the 100 mg once-daily dose with other schedules. In this dose-optimization study, patients (N = 670) were randomized to receive dasatinib at 100 mg once daily (n = 167), 140 mg once daily (n = 167), 50 mg twice daily (n = 168), or 70 mg twice daily (n = 168) (Shah et al. 2008a). After a minimum follow-up of 2 years, rates of CCyR and MMR were similar across the different dosing schedules (CCyR 50–54 %; MMR 37–38 %) (Shah et al. 2010). In the 100 mg once-daily arm, the 24-month rates of CCyR and MMR were 50 and 37 %, respectively. Rates of progression-free survival (PFS), overall survival (OS), and transformation to AP/BP by 24 months were 80, 91, and 3 %, respectively (Table 2). The 100 mg once-daily arm was associated with improved safety. Rates of all-grade pleural effusion (p = 0.049), grade ≥3 thrombocytopenia (p = 0.003), all-grade neutropenia (p = 0.034), and all-grade leukocytopenia (p = 0.017) were significantly lower for patients treated with dasatinib 100 mg once daily compared with other schedules (Shah et al. 2010). After a minimum follow-up of 5 years, PFS, OS, and rates of transformation to AP/BP were 57, 78, and 5 %, respectively, in the 100 mg once-daily arm (Shah et al. 2012).

A similar phase III dose-optimization study in patients with CML-AP (Kantarjian et al. 2009b) and CML-BP (Saglio et al. 2010b) led to a recommended dasatinib dose of 140 mg once daily in these indications (EMA Sprycel^® [dasatinib] 2012; Sprycel^® BMS 2013). Patients were randomized to receive dasatinib 70 mg twice daily (n = 159, AP; n = 74, myeloid BP [MBP]; n = 28, lymphoid BP [LBP]) or 140 mg once daily (n = 158, AP; n = 75 MBP; n = 33, LBP). In patients with CML-AP, similar rates of MHR (68 vs 66 %) and MCyR (43 vs 39 %) were observed in both treatment arms after a median follow-up of 15 months. Significantly, fewer patients in the once-daily arm had pleural effusion compared with the twice-daily arm (p < 0.001) (Kantarjian et al. 2009b). After 2 years of follow-up, for patients with myeloid BP, the MHR rates in both arms were 28 %; for those with lymphoid BP, the corresponding rates were 42 % in the once-daily arm and 32 % in the twice-daily arm. AE rates were suggestive of improved safety for dasatinib 140 mg once daily (Saglio et al. 2010b).

Following the success of second-line dasatinib in treating patients with CML, trials were performed to assess the clinical benefit of this agent in the first-line setting. The rationale for performing first-line studies derives partly from the observation that earlier responses to therapy are associated with better outcomes as seen with first-line imatinib (de Lavallade et al. 2008; Druker et al. 2006; Kantarjian et al. 2008; Marin et al. 2008). Similarly, in a retrospective analysis of patients from the dasatinib START-C and START-R, and dose-optimization trials, patients who achieved CCyR at 12 months had a 24-month PFS rate of 97 % (95 % confidence interval [CI], 93–100 %) compared with 78 % (95 % CI, 72–83 %) for patients who did not achieve CCyR or MMR at this time point (Hochhaus et al. 2009b). In exploratory landmark analyses of the second-line dasatinib dose-optimization study, patients receiving dasatinib 100 mg once daily with cytogenetic assessments at 12 months showing achievement of CCyR had higher PFS after 4-year minimum follow-up compared with patients achieving less than partial CyR (PCyR) responses (87 vs 45 %) (Shah et al. 2011). With 5-year follow-up, similar trends were observed for patients achieving ≤10 % BCR–ABL levels compared to patients with >10 % BCR–ABL levels at 3 months (Shah et al. 2012). These landmark analyses demonstrate the importance of achieving an early response to improve patient outcome. Furthermore, dasatinib is more potent than imatinib, and less susceptible to mechanisms of imatinib resistance. Therefore, it may be expected to elicit earlier responses than imatinib with consequently improved long-term outcomes.

The first trial investigating dasatinib as first-line treatment was a phase II, open-label study (Cortes et al. 2010b). Patients with newly diagnosed CML-CP were randomized to receive dasatinib 100 mg once daily (n = 66) or 50 mg twice daily (n = 33) (Pemmaraju et al. 2011). Because of results from a phase III multinational randomized study of first-line dasatinib and trends in favor of the 100 mg once-daily schedule of dasatinib seen in this study and others, the 50 mg twice-daily arm of this trial was closed after 66 patients were enrolled, and all subsequent patients were randomized to the 100 mg once-daily arm. The study continues enrolling patients in the once-daily arm (Cortes et al. 2010b; Pemmaraju et al. 2011). After a median follow-up of 29 months, in patients with ≥3-month follow-up (n = 87), rates of CCyR and MMR were 95 and 86 %, respectively. BCR–ABL levels of ≤0.0032 % (≥4.5-log reduction; MR^4.5) were achieved in 67 % of patients. Responses were achieved rapidly with 94 and 95 % of patients achieving a CCyR after 6 and 12 months, respectively. Similarly, MMR rates at 6 and 12 months were 68 and 73 %, respectively. These data compare favorably with historic response data for imatinib (Pemmaraju et al. 2011).

Dasatinib in the first-line setting was further investigated in the pivotal, open-label, multinational, randomized phase III trial of Dasatinib versus Imatinib Study in Treatment-Naïve CML Patients (DASISION) (Kantarjian et al. 2010). In this study, 519 patients newly diagnosed with CML-CP were randomized to receive dasatinib 100 mg once daily (n = 259) or imatinib 400 mg once daily (n = 260) (Figure 1) (Kantarjian et al. 2010). Efficacy data are shown in Table 3. The primary end point of this study was confirmed CCyR (cCCyR; CCyR on two consecutive assessments) by 12 months. For the dasatinib versus imatinib arms, the rate of cCCyR by 12 months was 77 versus 66 % (p = 0.007), respectively (Kantarjian et al. 2010). Cumulative CCyR, MMR, and MR^4.5 rates were higher for dasatinib across a 24-month period (p = 0.0002, p < 0.0001, and p = 0.002, respectively) (Kantarjian et al. 2012). Responses to dasatinib were rapid and prolonged; median times to CCyR were 3.2 and 6.0 months and median times to MMR were 15 and 36 months in the dasatinib and imatinib arms, respectively (Kantarjian et al. 2012). At 24 months, for dasatinib versus imatinib, cumulative rates of MMR were 64 versus 46 % (p < 0.0001), rates for BCR–ABL ≤ 0.01 % (MR⁴) were 29 versus 19 % (p = 0.0053), and rates of MR^4.5 were 17 versus 8 % (p = 0.0032) (Hochhaus et al. 2012a; Kantarjian et al. 2012). After 2-year follow-up, transformation to AP/BP throughout study follow-up (including on study and after discontinuation) occurred in nine patients (3.5 %) receiving dasatinib and 15 (5.8 %) receiving imatinib (Hochhaus et al. 2012a; Kantarjian et al. 2012). At 2-year follow-up, survival data for this study remain immature, but no difference was observed between dasatinib and imatinib for PFS (93.7 and 92.1 %) and OS (95.3 and 95.2 %). A small difference in failure-free survival for dasatinib versus imatinib was observed (including protocol defined progression; 91.2 vs 87.8 %) (Hochhaus et al. 2012a; Kantarjian et al. 2012).

In exploratory analyses, achieving an early molecular response (BCR–ABL levels of ≤10 %) at 3 months was associated with lower transformation rates (dasatinib: 1.5 vs 8.1 %; imatinib: 2.6 vs 9.4 %), better long-term outcomes (24-month PFS: dasatinib, 97 vs 83 %; imatinib, 96 vs 85 %), and improved response (24-month MMR rates: dasatinib, 76 vs 16 %; imatinib, 66 vs 19 %) in both treatment arms (Hochhaus et al. 2012b). Deeper levels of response were achieved earlier with dasatinib compared with imatinib as equivalent BCR–ABL (international scale [IS]) levels were achieved 6 months earlier with dasatinib, and a higher proportion of patients receiving dasatinib achieved BCR–ABL levels of ≤10 % at 3 months compared with patients receiving imatinib (84 vs 64 %) (Hochhaus et al. 2012b; Saglio et al. 2012). Similar results were found in another first-line study of dasatinib. Results from exploratory analyses of the dasatinib arm of the SPIRIT 2 trial have been reported, and after 2 years of follow-up, 91.4 % of patients receiving dasatinib achieved BCR–ABL levels of ≤10 % at 3 months (Marin et al. 2012a). Compared with patients who had >10 % BCR–ABL levels, patients achieving ≤10 % BCR–ABL at 3 months had significantly higher 2-year cumulative rates of CCyR (91.4 vs 58.8 %, p < 0.001), MMR (79.8 vs 14.3 %, p < 0.001), and MR^4.5 (45.7 vs 0 %, p < 0.001) (Marin et al. 2012a).

In total, 23 % of dasatinib-treated patients and 25 % of imatinib-treated patients discontinued treatment in DASISION; 5 and 7 % due to study-defined disease progression (defined as any of the following: doubling of white cell count to >20 × 10⁹/L in the absence of CHR; loss of CHR; increase in Ph-positive metaphases to >35 %; transformation to AP/BP; death from any cause), 3 and 4 % due to treatment failure, and 7 and 5 % due to drug-related AEs, respectively (Kantarjian et al. 2012). In patients who discontinued treatment, BCR–ABL mutations were found in 10 patients in each arm, with a narrower spectrum of mutations seen with dasatinib versus imatinib (3 vs 9 different amino acids affected). Mutations associated with discontinuation in the dasatinib arm were T315I (n = 7), F317L (n = 2), and F317I/V299L (n = 1) (Kantarjian et al. 2012).

Similar levels of response have been observed in additional studies of first-line dasatinib. In the SWOG S0325 phase II study, newly diagnosed patients were randomized to receive dasatinib 100 mg once daily (n = 123) or imatinib 400 mg once daily (n = 123) (Radich et al. 2012). At 12 months, median reductions in BCR–ABL transcript levels were greater with dasatinib compared with imatinib (3.3 vs 2.8 log; p = 0.063), as were the rates of >3-log BCR–ABL reductions (59 vs 44 %; p = 0.059). Rate of CCyR was significantly different between the dasatinib and imatinib arms (84 and 69 %, respectively; p = 0.040), although cytogenetic responses were only assessed in 53 % of patients (Radich et al. 2012).

Since early clinical trials, some AEs have been consistently reported in patients receiving dasatinib, including myelosuppression, fluid retention, pleural effusion, gastrointestinal disorders, fatigue, headache, musculoskeletal disorders, rash, and infection. Some bleeding events have also been reported. More recently, cases of pulmonary arterial hypertension (PAH), a sub-category of pulmonary hypertension (PH) and atypical of classical PAH with at least partial reversibility upon drug discontinuation, have been reported in a small number of patients receiving dasatinib (Dumitrescu et al. 2011; Fang et al. 2012; Galiè et al. 2009; Hennigs et al. 2011; Mattei et al. 2009; McLaughlin et al. 2009; Montani et al. 2012; Orlandi et al. 2011; Philibert et al. 2011; Rasheed et al. 2009; Sano et al. 2012). In clinical trials of first-line and second-line dasatinib, most AEs occurred within 12–24 months of treatment and were managed with dose modifications (Kantarjian et al. 2012; Shah et al. 2012; Sprycel^® BMS 2013).

In the early phase I, open-label, dose-escalation study, the major AE was reversible myelosuppression, leading to dose interruption in 60 % of patients (Talpaz et al. 2006). Grade 3/4 neutropenia and thrombocytopenia were seen in 45 and 35 % of patients with CML-CP, respectively. Nonhematologic AEs included diarrhea, nausea, and peripheral edema. Treatment-related pleural effusion occurred in 13 % of patients with CML-CP (Talpaz et al. 2006). Rates of AEs in this study may be expected to be elevated, as some patients received doses of dasatinib considerably higher than the current recommended dose of 100 mg once daily (range of dasatinib dose received 15–240 mg/day). A maximum tolerated dose was not determined in this study, and no patient withdrew from treatment as a result of toxic effects (Talpaz et al. 2006).

In the following START-C phase II trial, in which patients with CML-CP received second-line dasatinib 70 mg twice daily, 9 % of patients discontinued treatment because of study drug toxicity after 8 months of follow-up (Hochhaus et al. 2007). Cytopenias were common (grade 3/4 thrombocytopenia, 47 %; neutropenia, 49 %), but generally reversible and manageable with dose adjustments. Pleural effusion was observed in 19 % of patients (grade 3/4 in 3 %) (Hochhaus et al. 2007). Similar results were seen in the START-R phase II trial of dasatinib 70 mg twice daily (Kantarjian et al. 2007). After a median follow-up of 15 months, 28 % of patients had discontinued treatment, 16 % due to study drug intolerance. Cytopenias were common (grade 3/4 thrombocytopenia, 56 %; neutropenia, 61 %) but reversible, and manageable with dose modification. Pleural effusion occurred in 17 % of patients (Kantarjian et al. 2007). Most cases of pleural effusion observed across the START studies were managed with temporary dose interruption, diuretics, or pulse steroid therapy (Apperley et al. 2009; Cortes et al. 2007a; Hochhaus et al. 2007; Kantarjian et al. 2007). In the START-C and START-R trials, patients received dasatinib at 70 mg twice daily, which is higher than the current recommended dose for CML-CP (100 mg once daily). It may therefore be expected that the frequency of AEs and the rate of discontinuation due to study drug intolerance might be higher than expected in these trials compared with patients receiving the current recommended dose for CML-CP.

A single institution subgroup analysis of 138 patients treated with dasatinib in the phase I dose-escalation study and phase II START trials showed that 29 % of patients with CML-CP developed pleural effusion (Quintás-Cardama et al. 2007). Patients receiving 100 mg once-daily dasatinib had a lower incidence of pleural effusion compared with patients receiving 50 or 70 mg twice daily, or 140 mg once daily, while efficacy remained consistent across all four dosing schedules. Furthermore, a separate analysis indicated that intermittent dosing of dasatinib at 100 mg per day for 5 days per week, including a weekend drug holiday where dasatinib was not taken, led to reductions in the rate and severity of AEs including fluid retention and pleural effusion, while efficacy and disease control were maintained (La Rosée et al. 2013). An analysis of risk factors for pleural effusion in patients treated with second-line dasatinib identified prior history of cardiac disease (p = 0.02), hypertension (p = 0.01), and twice-daily dosing schedule (p = 0.05) to be associated with an increased risk of pleural effusion (Quintás-Cardama et al. 2007). In a separate analysis, older age was the only baseline characteristic associated with an increased risk of pleural effusion (Porkka et al. 2010). The development of lymphocytosis during dasatinib treatment was associated with a 1.7-fold increased risk of pleural effusion (95 % CI, 1.1–2.5) (Porkka et al. 2010).

The second-line, phase III dose-optimization study indicated that dasatinib 100 mg once daily was associated with reduced frequency of AEs compared with twice-daily dosing regimens in patients with CML-CP, while efficacy was maintained (Porkka et al. 2010; Shah et al. 2008a, 2012). With a minimum follow-up of 6 months, patients receiving dasatinib 100 mg once daily had lower rates of pleural effusion and grade 3/4 thrombocytopenia compared with patients receiving 70 mg twice daily (7 vs 16 % and 22 vs 37 %, respectively) (Shah et al. 2008a). Fewer patients receiving dasatinib 100 mg once daily required dose interruptions (51 vs 68 %), dose reductions (30 vs 55 %), or discontinuation (16 vs 23 %) (Shah et al. 2008a). With a minimum follow-up of 24 months, 14 % of patients receiving dasatinib 100 mg once daily developed pleural effusion, compared with 25 % of patients receiving 70 mg twice daily (Porkka et al. 2010). Improved tolerability of once-daily dosing may be due to intermittent dasatinib exposure in comparison with continuous exposure achieved by twice-daily dosing (Porkka et al. 2010). After a minimum follow-up of 5 years, grade 3/4 hematologic AEs in the 100 mg once-daily arm included neutropenia (36 %) and thrombocytopenia (24 %). Any-grade nonhematologic AEs included headache (33 %), diarrhea (28 %), fatigue (26 %), and pleural effusion (24 %) (Shah et al. 2012). Grade 3/4 cytopenias and any-grade nonhematologic AEs generally first occurred within 12–24 months of treatment (Shah et al. 2012).

In the first-line setting, similar AEs were observed. Treatment-related AEs led to the discontinuation of dasatinib in 7 % of patients (Kantarjian et al. 2012). Grade 3/4 hematologic AEs were relatively common in patients with CML-CP receiving dasatinib (100 mg once daily) or imatinib (400 mg once daily) in DASISION, after a minimum follow-up of 24 months (neutropenia: 24 vs 21 %; thrombocytopenia: 19 vs 11 %; anemia: 11 vs 8 %) (Kantarjian et al. 2012). Severe biochemical abnormalities were uncommon with the exception of grade 3/4 hypophosphatemia (dasatinib arm, 7 %; imatinib arm, 25 %) (Kantarjian et al. 2012). The most common nonhematologic AEs in DASISION (all grades, dasatinib vs imatinib) were myalgia (22 vs 39 %), diarrhea (19 vs 21 %), pleural effusion (14 vs 0 %), headache (13 vs 11 %), superficial edema (11 vs 36 %), rash (11 vs 17 %), and nausea (10 vs 23 %) (Kantarjian et al. 2012). Grade 3/4 nonhematologic AEs associated with dasatinib were uncommon at 0–2 % (fluid retention, 2 %; pleural effusion, 1 %; diarrhea, <1 %; fatigue, <1 %) (Kantarjian et al. 2012). In DASISION, at 1-year follow-up, 26 patients (10 %) had pleural effusion; all events were grade 1 (2 %) or grade 2 (8 %) (Kantarjian et al. 2010). By 2-year follow-up, pleural effusion events had occurred in 37 patients (14.3 %) and were generally mild-to-moderate in severity (grade 1: n = 9, 3.5 %; grade 2: n = 26, 10.1 %; grade 3: n = 2, 0.8 %) with no grade 4 events observed. Events were largely manageable with treatment interruption (n = 30), dose reduction (n = 19), or the use of diuretics (n = 17) or corticosteroids (n = 15). Four patients required a therapeutic thoracentesis. At 2-year follow-up, five patients (1.9 %) had discontinued dasatinib due to pleural effusion. Notably, the occurrence and management of pleural effusion appeared not to affect the efficacy of dasatinib (Kantarjian et al. 2012; Laneuville et al. 2011).

In some patients receiving dasatinib, large granular lymphocyte (LGL) expansions carrying clonal T-cell receptor gene arrangements occur resulting in lymphocytosis (Kreutzman et al. 2010). Data from a retrospective analysis of patients enrolled in DASISION suggested that dasatinib-treated patients with lymphocytosis had higher rates of any-grade pleural effusion and lower rates of myalgias and arthralgias compared with patients without lymphocytosis (Schiffer et al. 2010a). In a separate analysis of pooled study data, 31 % of patients with CML-CP had lymphocytosis, which was associated with a higher rate of CCyR and longer PFS in patients with advanced disease (Schiffer et al. 2010b). However, no formal statistical testing has been reported for either of these analyses. A subanalysis of DASISION demonstrated no substantial effects of baseline cardiovascular conditions, other comorbidities, or use of baseline medications on the side effects of dasatinib (Guilhot et al. 2010; Khoury et al. 2010; Saglio et al. 2010c).

More recently, rare cases of PAH in patients receiving dasatinib for CML and Ph+ ALL have been reported in the literature (n = 16) (Dumitrescu et al. 2011; Hennigs et al. 2011; Mattei et al. 2009; Montani et al. 2012; Orlandi et al. 2011; Philibert et al. 2011; Rasheed et al. 2009; Sano et al. 2012). By 2-year follow-up of the phase III DASISION trial of dasatinib versus imatinib in newly diagnosed CML-CP, three patients receiving dasatinib developed PH; however, no cases of PAH diagnosed by right heart catheterization (RHC) were recorded (Kantarjian et al. 2012). No patient in DASISION discontinued dasatinib therapy because of PH or PAH (Kantarjian et al. 2012). PAH observed in patients receiving dasatinib is not typical, as this disease is normally progressive, including cases with a drug-induced etiology which do not reverse on treatment withdrawal (Galiè et al. 2009; McLaughlin et al. 2009). To date, however, the typical clinical course for dasatinib-associated cases of PAH is improvement or complete resolution in the majority of cases upon withdrawal of treatment.

Guidelines for the management of AEs occurring in patients receiving dasatinib treatment are largely based on the experience of clinicians treating patients in early clinical trials (Khoury et al. 2009; Quintás-Cardama et al. 2008). For most AEs occurring in patients receiving dasatinib treatment, guidelines recommend dose interruption or dose reduction (NCCN v4. 2013; Sprycel^® BMS 2013). Early studies showed that cytopenias were usually reversible and effectively managed with dose interruption or reduction, with a minority of cases requiring blood transfusions or hospitalization (Apperley et al. 2009; Brave et al. 2008; Cortes et al. 2007a, 2008; Guilhot et al. 2007; Hochhaus et al. 2007; Ottmann et al. 2007; Quintás-Cardama et al. 2009b; Serpa et al. 2010; Shah et al. 2008a). In one study, cytopenias resolved in 60 % of patients upon interruption (Talpaz et al. 2006); in another study, permanent discontinuation was required in only 1 % (Brave et al. 2008). If hematologic AEs occur in patients receiving dasatinib, treatment should be interrupted until the absolute neutrophil count is ≥1.0 × 10⁹/L and platelets ≥50 × 10⁹/L. Dasatinib can then be resumed at the original dose if recovery occurs within 7 days or at a reduced dose of 80/50 mg/day if recovery takes longer than 7 days or if the event was a second/third recurrence. Although not yet licensed in all regions, growth factor support may also be useful for managing hematologic AEs (NCCN v4. 2013; Quintás-Cardama et al. 2009b; Shah et al. 2008a; Sprycel^® BMS 2013). If a severe nonhematologic AE (grade 3/4) develops, guidelines indicate that dasatinib be withheld until resolution or improvement. Treatment can then be resumed at a reduced dose dependent on initial severity of the event (NCCN v4. 2013; Sprycel^® BMS 2013). Early reports indicate that most nonhematologic AEs, including neuropathy, dyspnea, elevated liver enzymes, headache, bone pain, rash, renal failure, cardiac abnormality, infections, pancreatitis, and diarrhea, were effectively managed with dose reductions or interruptions (Apperley et al. 2009; Cortes et al. 2008; Hochhaus et al. 2007; Serpa et al. 2010). Consistent with reports, guidelines indicate that most pleural effusion events can be managed through dose reduction or interruption, and/or corticosteroids and diuretics, with a minority of cases requiring thoracentesis, oxygen therapy, or pleurodesis (Brave et al. 2008; Cortes et al. 2007a, 2008; Guilhot et al. 2007; Hochhaus et al. 2007; Kantarjian et al. 2012; Laneuville et al. 2011; Shah et al. 2008a; Talpaz et al. 2006). Once resolved, treatment can be resumed at the same or at a reduced dasatinib dose depending on event severity. A retrospective analysis of an intermittent treatment schedule of dasatinib at different doses demonstrated a reduction in the grade of pleural effusion and in hematologic toxicity without compromising efficacy (La Rosée et al. 2013). Other fluid retention events can be managed with diuretics and supportive care. To reduce the risk of PAH, patients should be evaluated for signs and symptoms of underlying cardiopulmonary disease before initiating dasatinib treatment. Upon confirmation of a PAH diagnosis based on RHC, guidelines indicate that dasatinib should be permanently discontinued (NCCN v4. 2013; Sprycel^® BMS 2013). PAH may be at least partially reversible upon treatment discontinuation. For bleeding events, recommended management steps include dose interruption and transfusion (Quintás-Cardama et al. 2009a; Sprycel^® BMS 2013). Rash may be managed with topical or systemic steroids, in addition to dose reduction, interruption, or discontinuation. Specific supportive medication is also indicated in case of headache and diarrhea (NCCN v4. 2013; Sprycel^® BMS 2013). A subanalysis of DASISION showed that dose modifications taken to manage AEs had no apparent effect on response (Jabbour et al. 2011).