Improved survival in red blood cell transfusion dependent patients with primary myelofibrosis (PMF) receiving iron chelation therapy
β Scribed by Heather A. Leitch; Jocelyn M. Chase; Trisha A. Goodman; Hatoon Ezzat; Meaghan D. Rollins; Dominic H.C. Wong; Maha Badawi; Chantal S. Leger; Khaled M. Ramadan; Michael J. Barnett; Lynda M. Foltz; Linda M. Vickars
- Publisher
- John Wiley and Sons
- Year
- 2009
- Tongue
- English
- Weight
- 173 KB
- Volume
- 28
- Category
- Article
- ISSN
- 0278-0232
- DOI
- 10.1002/hon.902
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β¦ Synopsis
Abstract
Many patients with primary myelofibrosis (PMF) become red blood cell (RBC) transfusion dependent (TD), risking iron overload (IOL). Iron chelation therapy (ICT) may decrease the risk of haemosiderosis associated organ dysfunction, though its benefit in PMF is undefined. To assess the effect of TD and ICT on survival in PMF, we retrospectively reviewed 41 patients. Clinical data were collected from the database and by chart review. The median age at PMF diagnosis was 64 (range 43β86) years. Median white blood cell (WBC) count at diagnosis was 7.6 (range 1.2β70.9)βΓβ10^9^/L; haemoglobin 104 (62β145)βG/L; platelets 300 (38β2088)βΓβ10^9^/L. Lille, Strasser, Mayo and International Prognostic System (IPS) scores were: low risk, nβ=β15, 8, 11, 3; intermediate, nβ=β15, 19, 9, 16; high, nβ=β5, 11, 5, 7; respectively. Primary PMF treatment was: supportive care, nβ=β23; hydroxyurea, nβ=β10; immunomodulatory, nβ=β4; splenectomy, nβ=β2. Sixteen patients were RBC transfusion independent (TI) and 25 TD; of these 10 received ICT for a median of 18.3 (0.1β117) months. PreβICT ferritin levels were a median of 2318 (range 263β8400) and at follow up 1571 (1005β3211Β΅g/L (pβ=β0.01). In an analysis of TD patients, factors significant for overall survival (OS) were: WBC count at diagnosis (pβ=β0.002); monocyte count (pβ=β0.0001); Mayo score (pβ=β0.05); IPS (pβ=β0.02); number of RBC units (NRBCU) transfused (pβ=β0.02) and ICT (pβ=β0.003). In a multivariate analysis, significant factors were: NRBCU (pβ=β0.001) and ICT (pβ=β0.0001). Five year OS for TI, TDβICT and TDβNO ICT were: 100, 89 and 34%, respectively (pβ=β0.003). The hazard ratio (HR) for receiving >20 RBCU was 7.6 (95% Confidence Intervals [CI] 1.2β49.3) and for ICT was 0.15 (0.03β0.77). In conclusion, 61% of PMF patients developed RBCβTD which portended inferior OS; however patients receiving ICT had comparatively improved OS, suggesting a clinical benefit. Prospective studies of IOL and the impact of ICT in PMF are warranted. Copyright Β© 2009 John Wiley & Sons, Ltd.