The goal of this clinical trial is to learn if pacritinib works better than hydroxyurea to treat advanced proliferative chronic myelomonocytic leukemia in adults. The main questions it aims to answer are: * Does pacritinib improve disease control compared to hydroxyurea? * What medical problems do participants have when taking pacritinib or hydroxyurea? Researchers will compare pacritinib to hydroxyurea to see if pacritinib is more effective and better tolerated in people with advanced proliferative chronic myelomonocytic leukemia. Participants will be randomly assigned to receive either pacritinib twice a day or hydroxyurea for up to 48 weeks. After treatment ends, participants will be followed for up to one year.
This is a randomized, multicenter, open-label Phase 2 clinical trial evaluating the efficacy and safety of pacritinib compared to hydroxyurea in adult participants with advanced proliferative chronic myelomonocytic leukemia (CMML). Approximately 66 participants will be randomized in a 2:1 ratio to receive either pacritinib 200 mg twice daily (n=44) or hydroxyurea (n=22) for up to 48 weeks. Randomization will be stratified based on prior therapy (i.e., prior use of hydroxyurea or hypomethylating agents vs. no prior therapy). The study includes: * A 28-day screening period * A 48-week treatment period * A 30-day post-treatment follow-up * A survival follow-up phase lasting approximately one year after randomization Participants receiving pacritinib who are not deriving benefit by Week 24, as assessed by the treating physician, will discontinue treatment. Participants in the hydroxyurea arm who are not deriving benefit by Week 24-or who experience non-leukemic disease progression-may switch to pacritinib for the remainder of the treatment period, provided they meet predefined "Safe to Switch" criteria. Participants who discontinue study therapy due to toxicity, disease progression, or other protocol-defined criteria will enter survival follow-up to monitor overall survival, event-free survival, leukemic-free survival, and receipt of allogeneic hematopoietic stem cell transplant. Data will be collected at least every three months until death, hematopoietic stem cell transplant, or leukemic transformation. An independent data monitoring committee will oversee safety, with the first review after enrollment of \~18 participants and subsequent reviews approximately every 6 months.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
66
100-mg capsules
capsules or tablets
MD Anderson Cancer Center
Houston, Texas, United States
RECRUITINGClinical benefit at Week 24, defined as achieving erythroid response in the absence of leukemic transformation.
For participants with baseline hemoglobin \<10 g/dL, response is defined as either a ≥1.5 g/dL hemoglobin increase lasting ≥8 weeks without red blood cell transfusion, or, if transfusion-dependent at baseline (≥4 units in the 8 weeks pre-enrollment), achieving ≥8 weeks of red blood cell transfusion independence, excluding transfusions given for pretreatment Hb ≤8.5 g/dL. Leukemic transformation is defined as ≥20% blasts or blast equivalents in the peripheral blood or bone marrow biopsy, or development of granulocytic sarcoma.
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Clinical benefit at Week 24, defined as achieving platelet response in the absence of leukemic transformation.
For participants with baseline platelet counts \<100 × 10⁹/L, response is defined as one of the following: an increase to ≥20 × 10⁹/L and by ≥100% for ≥8 weeks without platelet transfusion (if baseline \<20 × 10⁹/L); an increase of ≥30 × 10⁹/L for ≥8 weeks without transfusion (if baseline 20-\<100 × 10⁹/L); or, if transfusion-dependent at baseline (≥4 units in the 8 weeks pre-enrollment), achieving ≥8 weeks of platelet transfusion independence. Leukemic transformation is defined as ≥20% blasts or blast equivalents in the peripheral blood or bone marrow biopsy, or development of granulocytic sarcoma.
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Clinical benefit at Week 24, defined as achieving neutrophil response in the absence of leukemic transformation.
For participants with baseline ANC ≤1 × 10⁹/L, response is defined as either an increase to \>0.5 × 10⁹/L and by ≥100% for ≥8 weeks without myeloid growth factors (if baseline ANC ≤0.5 × 10⁹/L), or an increase by ≥50% for ≥8 weeks without myeloid growth factors (if baseline ANC \>0.5 to ≤1 × 10⁹/L). Leukemic transformation is defined as ≥20% blasts or blast equivalents in the peripheral blood or bone marrow biopsy, or development of granulocytic sarcoma.
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Clinical benefit at Week 24, defined as achieving spleen response in the absence of leukemic transformation.
For participants with baseline spleen ≥5 cm below the left costal margin (midclavicular line), spleen response is defined as a ≥35% reduction in spleen volume at endpoint assessment by MRI or CT. Leukemic transformation is defined as ≥20% blasts or blast equivalents in the peripheral blood or bone marrow biopsy, or development of granulocytic sarcoma.
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Clinical benefit at Week 24, defined as achieving symptom response in the absence of leukemic transformation.
Among participants with baseline Total Symptom Score (TSS) ≥20 per the MPN-SAF TSS: achieving ≥50% TSS reduction from baseline at the time of endpoint assessment. Leukemic transformation is defined as ≥20% blasts or blast equivalents in the peripheral blood or bone marrow biopsy, or development of granulocytic sarcoma.
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Clinical benefit at any time, defined as achieving at least one of the primary endpoint clinical benefit response criteria at any time on study.
Time frame: Measured from the start of study treatment to the end of treatment, for up to 48 weeks.
Achieving response at Week 24 and 48 according to the IWG 2015 criteria), including the following subtypes: complete response, complete cytogenetic remission, partial remission, marrow response
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Duration of response for primary endpoint (clinical benefit by Week 24)
Time frame: Measured from Week 24 through the end of treatment, up to 48 weeks.
Event-free survival
Event-free survival is defined as the time without death from any cause, transformation to AML (including granulocytic sarcoma), or disease progression after ≥3 cycles (Week 12), including CMML-1 to CMML-2 with ≥5% absolute blast increase or worsening splenomegaly.
Time frame: Measured from the start of study treatment to the end of treatment, for up to 48 weeks.
Leukemia-free survival, where events include death from any cause or transformation to AML (including granulocytic sarcoma)
Time frame: Measured from the start of study treatment to the end of treatment, for up to 48 weeks.
Overall survival
Time frame: Measured from the date of initiating study treatment to the date of death from any cause, assessed up to 24 months.
Incidence of allogeneic hematopoietic stem cell transplant.
Time frame: Measured from the date of initiating study treatment to the date of allogeneic hematopoietic stem cell transplant., assessed for up to 24 months
Adverse events and laboratory abnormalities as graded by NCI CTCAE v5.0.
Time frame: From the start of the adverse event collection period through 30 days following the last dose of study treatment.
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Change in arterial blood pressure measured in mmHg.
Time frame: From the start of the study treatment through 30 days following the last dose of study treatment.
Change in pulse rate measured in beats per minute.
Time frame: From the start of the study treatment through 30 days following the last dose of study treatment.
Change in respiratory rate measured in breaths per minute.
Time frame: From the start of the study treatment through 30 days following the last dose of study treatment.
Change in corrected QT interval measured in milliseconds using 12-lead electrocardiogram.
Time frame: From the start of the study treatment through 30 days following the last dose of study treatment.