Abstract

IntroductionIron overload (IO) has been shown to be an important cause of mortality and morbidity in patients who underwent allogeneic hematopoietic stem cell transplantation (alloHSCT). This study aimed to evaluate the possible effect of oral iron-chelation treatment (deferasirox) on survival in alloHSCT recipients in the posttransplant period. Materials and methodsA total of 80 alloHSCT recipients with IO were analyzed, retrospectively. Pretransplant and posttransplant data were obtained from the patients’ files. Patients were divided into two groups. Group 1; patients who did not receive any chelator treatment due to side effects or compliance problems. These patients were treated by phlebotomy. Group 2 consisted of patients who received deferasirox treatment. ResultsThe median treatment duration with deferasirox was 122days (min–max:91–225). The iron chelating treatment significantly reduced serum ferritin levels administered at a dosage of 20–30mg/kg/day (p<0.001). The median OS in Group 1 was found 16.0 (min–max:1.0–63.0) months and 25.0 (min–max:3.0–72.0) months in Group 2. In univariate and multivariate analysis, patients in Group 1 showed poorer OS compared to those in Group 2 with an increase in risk of death (HR:3.22, min–max:1.67–6.23, p=0.001 and HR:3.51,, min–max:1.75–6.99, p<0.001; respectively). The median DFS in Group 1 was found 11.0 (min–max:3.0–24.0) months and 22.0 (min–max:8.0–43.0) months in Group 2. The difference was found statistically significant (p=0.023). The other factors that we found significant difference in multivariate analysis between groups were; presence of acute GVHD (patients with aGVHD had increased risk of death compared to patients without aGVHD (HR:2.49, min–max: 1.32–4.69, p=0.005), chronic GVHD (HR:2.57, min–max:1.23–5.41, p=0.013), median interval to tx (HR: 2.23, min–max:1.17–4.26, p=0.015) and HLA match (HR:3.01, min–max:1.35–6.73, p=0.007) ConclusionOral deferasirox (Exjade) treatment may improve survival in patients with iron overload who underwent alloHSCT.

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