This is a multicenter 2-part, Phase 1b study designed to assess the safety, tolerability, pharmacokinetics (PK) and preliminary efficacy of PU-H71 in subjects taking concomitant ruxolitinib. The first part (Dose Escalation) will employ a standard 3+3 dose escalation design to determine Maximum Tolerated Dose (MTD). The second part of the study (Dose Confirmation) will confirm the recommended Phase 2 dose (RP2D) in an expanded population.
This is a multicenter 2-part, Phase 1b study designed to assess the safety, tolerability, PK and preliminary efficacy of PU-H71 (dihydrochloride salt) in subjects taking concomitant ruxolitinib. The first part (Dose Escalation) will employ a standard 3+3 dose escalation design to determine MTD. The second part of the study (Dose Confirmation) will confirm the RP2D in an expanded population. Up to 30 subjects who have active disease despite having received a minimum of 6 months of ruxolitinib therapy (including last 2 months at a daily dose of ≥5 mg twice daily and no more than one dose reduction 2-8 weeks prior to the baseline visit)stable dose will be enrolled to evaluate the safety, PK, and MTD of IV PU-H71 administered in combination ruxolitinib. Four ascending dose levels are planned. The planned dose levels of PU-H71 are 225 mg/m2, 300 mg/m2, 400 mg/m2, and 600 mg/m2. Additional dosing cohorts may be added at the discretion of the Safety Review Committee (SRC). Following a 28-day screening period, eligible subjects will receive PU-H71 once weekly intravenously for three consecutive weeks, followed by one week off on a 28-day cycle (D1, D8, D15, every 28 days). Ruxolitinib will be administered twice daily per the package insert at the stable dose the subject had been receiving prior to enrolling in the study. Subjects will have pk samples taken and ECGs performed at various time points throughout the study. Subjects will have safety evaluations including physical examinations, vital signs, laboratory assessments, and AE reporting. If deemed necessary, additional safety measurements will be performed at the discretion of the Investigator or the SRC. Subjects will be treated until disease progression, DLT, death, or study termination. At each dose level, a 3+3 dose escalation design will be employed. If none of the initial 3 subjects in the cohort experience a DLT within the first cycle, a new cohort of 3 subjects will be treated at the next higher dose level. If 1 of the 3 subjects in a cohort experiences a DLT, then 3 additional subjects will be treated at the same dose level as described under Dose Limiting Toxicities. Once the MTD has been determined in the dose escalation portion of the study, up to 15 patients may be enrolled for further evaluation of safety, PK, and preliminary clinical activity in a dose confirmation phase. A safety review committee (SRC) will assess the safety, tolerability, and available PK information collected for each dose level, decide whether to proceed to the next cohort, and determine the dose for the cohort.
Study Type
INTERVENTIONAL
Allocation
NON_RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
4
PU-H71 treatments will be administered by IV infusion on days 1, 8, and 15 of each 28-day cycle.
Dosing will be in accordance with current package insert and dose subject was on during study entry.
Yale Cancer Center
New Haven, Connecticut, United States
Ochsner Clinic Foundation
New Orleans, Louisiana, United States
University of Michigan
Ann Arbor, Michigan, United States
Karmanos Cancer Institute
Detroit, Michigan, United States
University of Nebraska Medical Center
Omaha, Nebraska, United States
Duke University Medical Center
Durham, North Carolina, United States
Cleveland Clinic - Taussig Cancer Institute
Cleveland, Ohio, United States
Abramson Cancer Center - University of Pennsylvania
Philadelphia, Pennsylvania, United States
MD Anderson Cancer Center
Houston, Texas, United States
Mays Cancer Center UT Health San Antonio
San Antonio, Texas, United States
Incidence of adverse events
Safety of PU-H71 in combination with ruxolitinib as assessed by the incidence and severity of adverse events (AEs) and serious AEs as determined by the NCI CTCAE v4.03.
Time frame: 12 months
Maximum Tolerated Dose of PU-H71 (MTD)
MTD as assessed by the occurrences of dose limiting toxicities of PU-H71 in combination with ruxolitinib. The MTD will be defined as the dose that does not exceed an acceptable threshold of toxicity.
Time frame: 7 months
Recommended Phase 2 Dose of PU-H71 (RP2D)
The RP2D is the dose with an acceptable risk/benefit ratio that warrant study in future trials
Time frame: 12 months
Pharmacokinetic profile of PU-H71: Area under the plasma concentration versus time curve (AUC)
Area under the plasma concentration versus time curve (AUC)
Time frame: 12 months
Pharmacokinetic profile of PU-H71: Trough plasma concentration (Cmin)
Trough plasma concentration (Cmin)
Time frame: 12 months
Pharmacokinetic profile of PU-H71: Peak plasma concentration (Cmax)
Peak plasma concentration (Cmax)
Time frame: 12 months
Pharmacokinetic profile of PU-H71: Time to maximum plasma concentration (Tmax)
Time to maximum plasma concentration (Tmax)
Time frame: 12 months
Pharmacokinetic profile of PU-H71: Plasma half-life (T1/2)
Plasma half-life (T1/2)
Time frame: 12 months
Treatment Response
Treatment response is to be evaluated using the revised IWG-MRT response criteria.
Time frame: 12 months
Symptom Burden Assessment
The symptomatic burden will be serially evaluated using the MPN-SAF TSS.
Time frame: 12 months
Biological Markers
Assess the effects of treatment on biological markers of the disease (i.e., bone marrow histology; JAK2V617F, CALR, or MPLW515L/K allele burden; cytogenetic response; serum cytokine profiles; and other biomarkers of disease activity).
Time frame: 12 months
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