Maintenance Therapy With Selinexor and Azacitidine in TP53 Mutant AML/MDS After Transplantation
- Sponsor
- Daihong Liu
- Study ID
- NCT07094464
- Phase
- PHASE1
- Status
- Active Not Recruiting
Conditions
- Allogeneic Hematopoietic Stem Cell Transplantation
- TP53-mutated MDS and AML
Eligibility Criteria
- Sex
- ALL
- Age
- 14 Years - 75 Years
- Healthy Volunteers
- Not accepted
Interventions
- Maintenance Therapy with Selinexor and Azacitidine — DRUG1. Selinexor: Oral administration in 4 cycles: \- Dose Escalation Phase: Cohort 1: Selinexor, 20 mg, twice a week for 2 weeks Cohort 2: Selinexor, 40 mg, twice a week for 2 weeks Cohort 3: Selinexor, 60 mg, twice a week for 2 weeks \- Dose Expansion: MTD/RP2D will be determined based on safety. 2. Azacitidine: 35 mg/m² for 5 days.
Study Details
This study aims to explore the safety and efficacy of selinexor combined with azacitidine for maintenance therapy in TP53 mutant AML/MDS patients following transplantation.
Key Dates
- Start date
- Jun 1, 2025
- Status verified
- Jul 2025
- Primary completion
- Jun 30, 2027
- Completion
- Dec 30, 2028
Study Design
- Enrollment
- 20 participants (estimated)
- Allocation
- NA
- Intervention model
- SINGLE_GROUP
- Primary purpose
- TREATMENT
Arms
- Experimental: Assigned Interventions1)Treatment will begin approximately 3 months post-transplant. The study duration will be 1 year with treatment cycles every 3 months, totaling 4 cycles. 1. Selinexor: Single-arm phase I study with sequential dose escalation of Selinexor. Three dose levels will be tested in separate cohorts: * Cohort 1: Selinexor, 20 mg, twice a week for 2 weeks * Cohort 2: Selinexor, 40 mg, twice a week for 2 weeks * Cohort 3: Selinexor, 60 mg, twice a week for 2 weeks 2. Azacitidine: 35 mg/m² for 5 days. 2)Bone marrow morphology, characteristic gene mutation or fusion gene quantification, immunophenotyping, chimerism, or transplant-related FISH will be assessed before and after each treatment cycle, according to the follow-up schedule post-transplant. Patients with hematological relapse at any time will discontinue from the experimental group and receive an alternative treatment.
Primary Outcome Measure
Disease relapse [ Time Frame: 1 year after transplantation ]
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