Abstract 1306

Donor-derived myelodysplastic syndrome (DD-MDS) and acute leukemia (DD-AL) are rare complications of allogeneic HSCT with approximately 40 cases identified in the literature. While the estimated incidence of DD-MDS/AL is between 0.12–5% for recipients of allogeneic HSCTs, more precise estimates by HSCT source have been impaired by differences in follow-up and changes in diagnostic tools over time. To this end, we evaluated all allogeneic transplants performed at the University of Minnesota between 1992 and 2009 in whom molecular assays for chimerism were performed. Patients transplanted for malignancy also had routine marrow examinations for evidence of recurrent disease. During this interval, there were 226 related donor transplants (47 marrow, 164 peripheral blood, 3 marrow and peripheral blood, 12 umbilical cord blood [UCB]), and 1254 unrelated donor transplants (436 marrow, 16 peripheral blood, 802 UCB). Of the entire cohort, 73% had a malignant and 27% had a non-malignant disease with 60% male, and 57% aged >18 years. The median follow-up among survivors was 3.5 years (range, 0.5 to 15.1). Eight cases of DD-MDS/AL were identified with the event diagnosed between 3 months and 15 years (median 33 months) after transplant. At 5 years, the incidence of DD-MDS/AL by donor type was 3.4% after matched sibling donor, 0% after unrelated marrow/peripheral blood donor and 0.4% after unrelated UCB donor transplant. Main characteristics of the 8 cases are described in Table 1. Four patients had CMV reactivation during their post-transplant course requiring antiviral therapy; three had poor hematopoietic recovery with prolonged courses of hematopoietic growth factor therapy. Five had monosomy 7, including all 4 UCB cases. Time to DD-MDS/AL varied by HSCT source: 22 months for UCB and 50 months for MSD cases. Underlying mechanisms are not yet known but have been postulated to include inherited or chemotherapy-induced marrow stroma and microenvironment abnormalities, bystander injury due to residual low-level chemotherapy and radiation damage, impaired tumor surveillance, chronic antigenic stimulation, premature aging of donor cells, transfer of oncogenic material from host to donor cells and the presence of preleukemic clones found rarely in UCB samples. Interestingly, one patient with DD-MDS had a sustained complete remission and loss of the cytogenetic clone by removing GCSF. The patient with DD-acute lymphocyte leukemia completed Children’s Cancer Group protocol 1961 and remains disease-free currently out 43 months from DD-AL occurrence. Two of the DD-acute myeloid leukemia cases were treated with high dose Ara-C containing regimens and one patient went on to a second HSCT. Two of the DD-MDS cases were treated with a second HSCT, while one was given decitabine. These 8 cases illustrate the rarity of the event and potentially provide more accurate estimates of the risk of this complication by HSCT source for counseling patients. Furthermore, therapeutic interventions are limited but removal of hematopoietic growth factor may alone be effective in some cases.

Table 1:

Donor Derived Myelodysplastic Syndrome and Acute Leukemia Case Characteristics

Age# (years)Primary DiagnosisYear of HSCTDonoraGVHDcGVHDMonths to EventEvent TypeOutcome
1* LCH 2000 UCB No No 42 AML Dead 
11 AML 2005 UCB Yes Yes 19 MDS Dead 
38 AML 2005 UCB Yes No MDS Alive 
57 MDS/AML 2007 UCB No Yes 25 MDS Dead 
AML 1992 MSD Yes Yes 180 ALL Alive 
11 FA 2000 MSD No No 16 AML Dead 
34* CLL/tMDS 1996 MSD No Yes 41 MDS Dead 
47 MDS 1998 MSD No No 71 AML Dead 
Age# (years)Primary DiagnosisYear of HSCTDonoraGVHDcGVHDMonths to EventEvent TypeOutcome
1* LCH 2000 UCB No No 42 AML Dead 
11 AML 2005 UCB Yes Yes 19 MDS Dead 
38 AML 2005 UCB Yes No MDS Alive 
57 MDS/AML 2007 UCB No Yes 25 MDS Dead 
AML 1992 MSD Yes Yes 180 ALL Alive 
11 FA 2000 MSD No No 16 AML Dead 
34* CLL/tMDS 1996 MSD No Yes 41 MDS Dead 
47 MDS 1998 MSD No No 71 AML Dead 
#

Age at initial diagnosis.

*

Previously published cases. LCH = Langerhans Cell Histiocytosis, AML = Acute Myeloid Leukemia, MDS = Myelodysplastic Syndrome, FA = Fanconi Anemia, CLL = Chronic Lymphocytic Leukemia, tMDS = Therapy Related MDS, aGVHD = Acute Graft Versus Host Disease, cGVHD = Chronic Graft Versus Host Disease

Disclosures:

No relevant conflicts of interest to declare.

Author notes

*

Asterisk with author names denotes non-ASH members.

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