Eligibility |
Inclusion Criteria:
I. Acute myelogenous leukemia (AML)
- Complete first remission (CR1) at high risk for relapse such as any of the following:
- Known prior diagnosis of myelodysplasia (MDS) or myeloproliferative disorder
- Therapy-related AML
- White cell count at presentation > 100,000
- Presence of extramedullary leukemia at diagnosis
- Any unfavorable subtype by FAB or WHO classification
- High-risk cytogenetics (e.g. those associated with MDS, abnormalities of 5, 7, 8,
complex karyotype) or high risk molecular abnormalities
- Requirement for 2 or more induction to achieve CR1
- Any patient with newly diagnosed AML with intermediate risk cytogenetics who elects
allograft with curative intent over consolidation chemotherapy
- Any patient unable to tolerate consolidation chemotherapy as would have been deemed
appropriate by the treating physician
- Other high risk features not defined above
- Complete second remission (CR2)
- Primary refractory or relapsed AML with less than 10% blasts before transplant.
Persistent/relapsed AML with cytogenetic, flow cytometric, or molecular aberrations in
>/= 10% of cells are eligible
II. Acute lymphoblastic leukemia (ALL)
- Complete first remission (CR1) at high risk for relapse such as any of the following:
- White cell count at presentation > 30,000 for B-cell lineage and > 100,00 for T-cell
lineage
- Presence of any high-risk cytogenetic abnormalities such as t(9;22), t(1;19), t(4;11)
or other MLL rearrangements (11q23) or other high-risk molecular abnormality
- Failure to achieve complete remission after four weeks of induction therapy
- Persistence or recurrence of minimal residual disease on therapy
- Any patient with newly diagnosed ALL >/= 50 years-old
- Any patient unable to tolerate consolidation and/or maintenance chemotherapy as would
have been deemed appropriate by the treating physician
- Other high risk features not defined above
- Complete second remission (CR2)
- Primary refractory or relapsed ALL with less than 5% blasts before transplant.
Persistent/relapsed ALL with cytogenetic, flow cytometric or molecular aberrations in
>/=5% of cells are eligible.
III. Other acute leukemias: leukemias of ambiguous lineage or of other types e.g. blastic
plasmacytoid dendritic cell neoplasm with less than 5% blasts. Persistent/relapsed disease
with cytogenetic, flow cytometric or molecular aberrations in >/=5% of cells are eligible
IV. Myelodysplastic Syndrome (MDS)/ Myeloproliferative Disorders (MPD) other than
myelofibrosis:
- International prognostic scoring system (IPSS) risk score of INT-2 or high risk at the
time of diagnosis
- Any IPSS risk category if life-threatening cytopenia(s) exists
- Any IPSS risk category with karyotype or genomic changes that indicate high risk for
progression to acute myelogenous leukemia
- MDS/ myeloproliferative disorder overlap syndromes without myelofibrosis
- MDS/ MPD patients must have less than 10% bone marrow myeloblasts and ANC >/= 0.2
(growth factor supported if necessary) at transplant work-up
V. Non-Hodgkin lymphoma (NHL) or Hodgkin lymphoma (HL) at high-risk of relapse or
progression if not in remission:
- Eligible patients with aggressive histologies (such as, but not limited to, diffuse
large B-cell NHL, mantle cell NHL, and T-cell histologies) in CR
- Eligible patients with indolent B cell NHL (such as, but not limited to, follicular,
small cell or marginal zone NHL) will have 2nd or subsequent progression with stable
disease/CR/PR with no single lesion equal to or more than 5 cm.
- Eligible patients with HL will be without progression of disease (POD) after salvage
chemotherapy with no single lesion equal to or more than 5cm.
Organ Function and Performance Status Criteria:
- Karnofsky score >/= 70% (inpatient Leukemia service transfers without discharge are
acceptable provided patient has equivalent KPS as if were outpatient)
- Calculated creatinine clearance >/= 60 ml/min
- Bilirubin < 1.5 mg/dL (unless benign congenital hyperbilirubinemia)
- ALT </= 3 x upper limit of normal
- Pulmonary function (spirometry and corrected DLCO) >/= 50% predicted
- Left ventricular ejection fraction greater than 50%
- Albumin >/= 3.0
- Age-adjusted Hematopoietic Cell Transplantation-Comorbidity Index (aaHCT-CI) less than
or equal to 7
Graft Criteria:
2 CB units will be selected according to current MSKCC unit selection algorithm. High
resolution 8 allele HLA typing and recipient HLA antibody profile will be performed. Unit
selection will occur based on HLA-match, total nucleated cell (TNC) and CD34+ cell dose
adjusted per patient body weight. The bank of origin will also be taken into account. Donor
specific HLA antibodies, if present, will also be taken into consideration and may
influence the selection of the graft.
- Each CB unit must be at least 3/8 HLA-matched to the patient considering high
resolution 8-allele HLA typing
- Each CB unit will be required to have a cryopreserved TNC dose of at least 1.5 x 10^7
TNC/ recipient body weight (TNC/ kg)
- Each CB unit will be required to have a cryopreserved CD34+ cell dose of at least 1.0
x 10^5 CD34+ cells/ recipient body weight (CD34+/kg).
- A minimum of one domestic will be reserved as a backup unit.
Exclusion Criteria:
- Indolent NHL or Hodgkin lymphoma with POD after most recent salvage chemotherapy
- Diagnosis of myelofibrosis or other malignancy with moderate-severe bone marrow
fibrosis
- Any diagnosis without prior immunosuppressive chemotherapy within 3 months of intended
admission for transplant
- Prior checkpoint inhibitors/ blockade in the last 12 months
- Two prior stem cell transplants of any kind
- One prior autologous stem cell transplant within the preceding 12 months
- One prior allogeneic stem cell transplant within the preceding 24 months
- Prior radiation therapy with 400cGy or more of TBI
- Active and uncontrolled infection at time of transplantation
- HIV infection
- Seropositivity for HTLV-1.
- Inadequate performance status/ organ function.
- Pregnancy or breast feeding
- Patient or guardian unable to give informed consent or unable to comply with the
treatment protocol including appropriate supportive care, long-term follow-up, and
research tests.
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