Abstract
INTRODUCTION: Obesity is increasingly common in the US and is frequently associated with co-morbid medical conditions that may increase the risk of HCT, often the optimal treatment for AML. HCT risk and outcomes for AML on the basis of body mass index (BMI) have not been well-characterized. Using data from the Center for International Blood and Marrow Transplant Research (CIBMTR), we have previously shown no significant difference in outcomes for autologous HCT for lymphoma among normal weight, overweight, and obese patients (pts) but worse outcomes for underweight pts (Navarro et al, BBMT 2006, 12(5): 541–51). Here, we compare outcomes by weight groups for AML patients who underwent autologous, related, or unrelated HCT.
METHODS: Our final population included patients age ≥ 18 who underwent myeloablative unpurged autologous or allogeneic HCT for AML in 1st or 2nd complete remission, primary induction failure, or 1st relapse reported to the CIBMTR from 1995 to 2004. Cord blood HCTs were excluded. Four weight groups were defined based on BMI (BMI=weight (kg)/ height (m2)): underweight <18; normal=18–25; overweight >25–30; and obese >30. Treatment-related mortality (TRM), relapse, leukemia-free survival (LFS), and overall survival (OS) were compared using multivariable proportional hazards regression analysis accounting for patient, disease and HCT-related variables.
RESULTS: We included 373 autologous, 2041 related, and 1801 unrelated transplant recipients. Patient-, disease-, and transplant characteristics were well-matched across weight groups and transplant types. Multivariable analysis examining risks (95% confidence intervals) relative to the normal weight group are:
HCT Type . | Normal . | Underweight . | Overweight . | Obese . |
---|---|---|---|---|
-- =not done due to insufficient number of pts; NS=not significant; treatment failure = death or recurrence of disease. | ||||
Autologous | n=164 | n=5 | n=112 | n=81 |
Death | -- | NS | NS | |
Treatment failure | -- | NS | NS | |
Relapse | -- | NS | NS | |
TRM | -- | NS | NS | |
Related Allogeneic | n=1161 | n=31 | n=543 | n=268 |
Death | 1.86 (1.24–2.78) | NS | 1.23 (1.04–1.47) | |
Treatment failure | 2.08 (1.37–3.15) | NS | 1.19 (1.00–1.42) | |
Relapse | 2.02 (1.18–3.47) | NS | NS | |
TRM | 2.22 (1.17–4.22) | NS | 1.32 (1.02–1.70) | |
Unrelated Allogeneic | n=846 | n=31 | n=523 | n=368 |
Death | NS | NS | NS | |
Treatment failure | NS | NS | NS | |
Relapse | NS | 0.82 (0.68–0.99) | 0.76 (0.60–0.96) | |
TRM | NS | NS | NS |
HCT Type . | Normal . | Underweight . | Overweight . | Obese . |
---|---|---|---|---|
-- =not done due to insufficient number of pts; NS=not significant; treatment failure = death or recurrence of disease. | ||||
Autologous | n=164 | n=5 | n=112 | n=81 |
Death | -- | NS | NS | |
Treatment failure | -- | NS | NS | |
Relapse | -- | NS | NS | |
TRM | -- | NS | NS | |
Related Allogeneic | n=1161 | n=31 | n=543 | n=268 |
Death | 1.86 (1.24–2.78) | NS | 1.23 (1.04–1.47) | |
Treatment failure | 2.08 (1.37–3.15) | NS | 1.19 (1.00–1.42) | |
Relapse | 2.02 (1.18–3.47) | NS | NS | |
TRM | 2.22 (1.17–4.22) | NS | 1.32 (1.02–1.70) | |
Unrelated Allogeneic | n=846 | n=31 | n=523 | n=368 |
Death | NS | NS | NS | |
Treatment failure | NS | NS | NS | |
Relapse | NS | 0.82 (0.68–0.99) | 0.76 (0.60–0.96) | |
TRM | NS | NS | NS |
CONCLUSIONS: There were no significant differences in risk of TRM, LFS, relapse or OS for normal weight, overweight or obese patient groups who received autologous HCT. Obese recipients of related HCT for AML had increased risk of death, treatment failure, and TRM, though the magnitude was small, an effect was not seen in the unrelated HCT group. Underweight patients who received a related, but not unrelated HCT, fared substantially worse than normal weight patients for all outcomes. It may be that the higher risk of the unrelated HCT procedure masks important but less obvious risks associated with being underweight whereas in the related donor HCT setting, such risks become manifest. Small numbers of patients limit the ability to better characterize this finding in underweight patients. Disproportionately, fewer transplants have been reported in underweight patients which suggest they experience disease and patient-related factors that preclude transplantation. No differences were observed for incidence of acute or chronic GVHD for any weight group. Overweight and obesity should not be a barrier to HCT; however, caution should be exercised in selecting underweight patients for HCT.
Disclosures: No relevant conflicts of interest to declare.
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