This phase II trial tests the effect of adding ruxolitinib to standard graft versus host disease (GVHD) prevention in treating older patients with myelofibrosis (MF) or myelodysplastic syndrome/myeloproliferative neoplasm (MDS/MPN) overlap syndromes before, during, and after a donor (allogeneic) hematopoietic cell transplant (HCT). Allogeneic HCT is a procedure in which a person receives blood-forming stem cells (cells from which all blood cells develop) from a genetically similar, but not identical donor. Giving chemotherapy, such as cytoxan and busulfan or fludarabine and melphalan, before a donor transplant helps kill cancer cells in the body and helps make room in the patient's bone marrow for new blood-forming cells (stem cells) to grow. However, sometimes the transplanted cells from a donor can attack the body's normal cells (called GVHD). Giving standard prevention (prophylaxis) therapies, such as tacrolimus and methotrexate, after the transplant may stop this from happening. Methotrexate, a type of antifolate, is in a class of medications called antimetabolites. Methotrexate stops cells from using folic acid to make deoxyribonucleic acid and may kill cancer cells. Tacrolimus is used to help reduce the risk of rejection by the body of organ and bone marrow transplants. Ruxolitinib, a type of Janus-associated kinase (JAK) inhibitor, blocks a protein called JAK, which may help keep abnormal blood cells or cancer cells from growing. It may also lower the body's immune response and prevent the development of GVHD. Giving ruxolitinib before, during and after allogeneic HCT in addition to standard GVHD prophylaxis may be safe, tolerable and effective in preventing GVHD and improving outcomes in older patients with MF or MDS/MPN overlap syndrome.
OUTLINE: PART 1: Patients receive ruxolitinib or an alternate JAK-inhibitor for at least 8 weeks prior to the start of HCT conditioning. Starting on day -4, patients receive 5 mg of ruxolitinib orally (PO) twice daily (BID) for 12 months then PO once daily (QD) until 18 months. Patients receive high intensity conditioning with cyclophosphamide intravenously (IV) on days -7 and -6 and busulfan IV over 3 hours on days -5 to -2 or reduced intensity conditioning with fludarabine IV over 30 minutes on days -6 to -2 and melphalan IV over 15-30 minutes on days -3 and -2. PART 2: Patients receive stem cells infusion on day 0. Starting on day -3, patients receive tacrolimus IV over 1-2 hours or PO every 12 hours for at least 100 days. Patients also receive methotrexate IV on days 1, 3, 6, and 11. Additionally, patients undergo urine sample collection, echocardiography, chest computed tomography (CT) and pulmonary function testing prior to conditioning and blood sample collection, bone marrow biopsy and aspiration and spleen ultrasound or CT at multiple time points before and after transplant. After completion of study treatment, patients are followed at days 28, 100, 180, and at 9 months, 1 year, 18 months and 2 years.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
50
Given PO
Given infusion
Given IV
Undergo CT
Given IV
Undergo echocardiography
Given IV
Given JAK inhibitor
Given IV
Given IV
Given IV or PO
Undergo urine and blood sample collection
Undergo bone marrow biopsy and aspiration
Undergo bone marrow biopsy and aspiration
Fred Hutch/University of Washington Cancer Consortium
Seattle, Washington, United States
RECRUITINGIncidence of grade II-IV graft versus host disease (GVHD) requiring systemic immune suppression
Will be estimated as a simple proportion, and the upper bound of the one-sided 95% confidence interval for the estimated proportion will be estimated using the Clopper-Pearson method. The exact binomial test will be used to compare the observed probability to the benchmark of 65%.
Time frame: Up to day-100
Incidence of grade III-IV acute GVHD
Will be estimated as simple proportions and informally compared to the results from the historical cohort.
Time frame: Up to day-100
Incidence of any-grade chronic GVHD
Will be treated as time-to-event endpoints, with specified point estimates.
Time frame: Up to 1 and 2 years
Incidence of moderate-to-severe chronic GVHD
Will be treated as time-to-event endpoints, with specified point estimates.
Time frame: Up to 1 and 2 years
Non-relapse mortality (NRM)
Will be estimated as simple proportions and informally compared to the results from the historical cohort.
Time frame: At day-100
NRM
Will be treated as time-to-event endpoints, with specified point estimates.
Time frame: At 1 year
Remission status
Will be estimated as simple proportions and informally compared to the results from the historical cohort.
Time frame: At day-100
Relapse rate
Will be treated as time-to-event endpoints, with specified point estimates.
Time frame: At 1 and 2 years
Overall survival
Will be treated as time-to-event endpoints, with specified point estimates.
Time frame: Up to 1 year and by end of study, assessed up to 2 years
Incidence of graft failure
Will be estimated as simple proportions and informally compared to the results from the historical cohort.
Time frame: Up to day-100
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