Abstract 2038

Background:

Cytogenetic abnormalities in leukemic blasts at time of diagnosis are the most important prognostic factors in acute myelogenous leukemia (AML). However, approximately 50% of patients (pts) with AML have normal cytogenetics (NC-AML). Within this population, the presence of somatic mutations further refines the prognosis. Mutations such as the internal tandem duplication of FLT-3 (FLT-3 ITD), and mutations in NPM1 and IDH1 have been all been shown to have significant prognostic value in determining response to chemotherapy and overall survival (OS). FLT-3 ITD is present in approximately 30% of pts with NC-AML and is considered the most significant predictor of poor prognosis following chemotherapy. However, it is not clear whether the presence of FLT-3 ITD influences the outcome of patients who undergo hematopoietic stem cell transplant (HSCT). We therefore performed a retrospective analysis of all adult patients with NC-AML and FLT-3 ITD present at time of diagnosis who underwent HSCT at MSKCC between 2007 and 2012.

Methods:

A total of 196 pts with AML underwent HSCT during this period. For this analysis, we excluded 112 pts with abnormal cytogenetics, 5 pts who had no cytogenetic testing performed, and 27 pts with normal cytogenetics who did not have molecular analysis performed.

Results:

A total of 52 pts with normal cytogenetics had molecular testing done; of these, 35 were FLT-3 negative (67%) and 17 were FLT-3 positive (33%). Characteristics of the 2 groups are shown below:

FLT-3 Negative (n=35)FLT-3 Positive (n=17)
Median age years (range) 55 (27–57) 55 (19–71) 
M/F 22/13 7/10 
Transplanted in CR1 22 (63%) 13 (76%) 
Transplanted in CR-2 5 (14%) 1 (6%) 
Transplanted in other 8 (23%) 3 (18%) 
Donor: Matched sib donor 15 (43%) 6 (35%) 
Matched unrelated donor 11 (31%) 6 (35%) 
Mismatched unrelated donor 9 (26%) 5 (29%) 
Source: Bone marrow 1 (6%) 
    Mobilized blood 32 (91%) 12 (71%) 
    Cord blood 3 (9%) 4 (24%) 
Unmodified transplant 10 (29%) 6 (25%) 
T-depleted transplant 25 (71%) 11 (65%) 
Median f/u mos (range) 22 (2–22) 26 (3–44) 
Relapses 3 (9%) 2 (12%) 
Death (all causes) 11 (31%) 4 (24%) 
Overall survival at 2 years: 70% 82% 
FLT-3 Negative (n=35)FLT-3 Positive (n=17)
Median age years (range) 55 (27–57) 55 (19–71) 
M/F 22/13 7/10 
Transplanted in CR1 22 (63%) 13 (76%) 
Transplanted in CR-2 5 (14%) 1 (6%) 
Transplanted in other 8 (23%) 3 (18%) 
Donor: Matched sib donor 15 (43%) 6 (35%) 
Matched unrelated donor 11 (31%) 6 (35%) 
Mismatched unrelated donor 9 (26%) 5 (29%) 
Source: Bone marrow 1 (6%) 
    Mobilized blood 32 (91%) 12 (71%) 
    Cord blood 3 (9%) 4 (24%) 
Unmodified transplant 10 (29%) 6 (25%) 
T-depleted transplant 25 (71%) 11 (65%) 
Median f/u mos (range) 22 (2–22) 26 (3–44) 
Relapses 3 (9%) 2 (12%) 
Death (all causes) 11 (31%) 4 (24%) 
Overall survival at 2 years: 70% 82% 
View Large
Conclusion:

Both groups had similar clinical and transplant characteristics, relapse rates, and OS (p=NS in all categories). We conclude that in this relatively small group of pts (1) HSCT appears to overcome the negative prognostic effect of FLT-3 ITD and (2) use of a T cell depleted graft does not influence transplant outcomes. A larger cooperative group analysis will be needed to confirm these findings.

Disclosures:

No relevant conflicts of interest to declare.

Topics:
cytogenetics, hematopoietic stem cell transplantation, leukemia, myelocytic, acute, ms-like tyrosine kinase 3, brachial plexus neuritis, impedance threshold device, transplantation, chemotherapy regimen, prognostic factors, receptors, complement 3d

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Author notes

*

Asterisk with author names denotes non-ASH members.

© 2012 by The American Society of Hematology
2012
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