OBJECTIVES: It is widely assumed that, at matched transfusional iron-loading rates, responses to chelation therapy are similar, irrespective of the underlying condition. However, data are limited for rare transfusion-dependent anaemias, and it remains to be elucidated if response differs, depending on whether the anaemia has a primary haemolytic or production mechanism. METHODS: The efficacy and safety of deferasirox (Exjade®) in rare transfusion-dependent anaemias were evaluated over 1 yr, with change in serum ferritin as the primary efficacy endpoint. Initial deferasirox doses were 10-30 mg/kg/d, depending on transfusion requirements; 34 patients had production anaemias, and 23 had haemolytic anaemias. RESULTS: Patients with production anaemias or haemolytic anaemias had comparable transfusional iron-loading rates (0.31 vs. 0.30 mL red blood cells/kg/d), mean deferasirox dosing (19.3 vs. 19.0 mg/kg/d) and baseline median serum ferritin (2926 vs. 2682 ng/mL). Baseline labile plasma iron (LPI) levels correlated significantly with the transfusional iron-loading rates and with serum ferritin levels in both cohorts. Reductions in median serum ferritin levels were initially faster in the production than the haemolytic anaemias, but at 1 yr, similar significant reductions of 940 and 617 ng/mL were attained, respectively (-26.0% overall). Mean LPI decreased significantly in patients with production (P < 0.0001) and haemolytic (P = 0.037) anaemias after the first dose and was maintained at normal mean levels (< 0.4 μm) subsequently. The most common drug-related, investigator-assessed adverse events were diarrhoea (n = 16) and nausea (n = 12). CONCLUSIONS: At matched transfusional iron-loading rates, the responses of rare transfusion-dependent anaemias to deferasirox are similar at 1 yr, irrespective of the underlying pathogenic mechanism. © 2011 John Wiley & Sons A/S.

Response of iron overload to deferasirox in rare transfusion-dependent anaemias: equivalent effects on serum ferritin andlabile plasma iron for haemolytic or production anaemias

PIGA, Antonio Giulio;SAGLIO, Giuseppe;
2011-01-01

Abstract

OBJECTIVES: It is widely assumed that, at matched transfusional iron-loading rates, responses to chelation therapy are similar, irrespective of the underlying condition. However, data are limited for rare transfusion-dependent anaemias, and it remains to be elucidated if response differs, depending on whether the anaemia has a primary haemolytic or production mechanism. METHODS: The efficacy and safety of deferasirox (Exjade®) in rare transfusion-dependent anaemias were evaluated over 1 yr, with change in serum ferritin as the primary efficacy endpoint. Initial deferasirox doses were 10-30 mg/kg/d, depending on transfusion requirements; 34 patients had production anaemias, and 23 had haemolytic anaemias. RESULTS: Patients with production anaemias or haemolytic anaemias had comparable transfusional iron-loading rates (0.31 vs. 0.30 mL red blood cells/kg/d), mean deferasirox dosing (19.3 vs. 19.0 mg/kg/d) and baseline median serum ferritin (2926 vs. 2682 ng/mL). Baseline labile plasma iron (LPI) levels correlated significantly with the transfusional iron-loading rates and with serum ferritin levels in both cohorts. Reductions in median serum ferritin levels were initially faster in the production than the haemolytic anaemias, but at 1 yr, similar significant reductions of 940 and 617 ng/mL were attained, respectively (-26.0% overall). Mean LPI decreased significantly in patients with production (P < 0.0001) and haemolytic (P = 0.037) anaemias after the first dose and was maintained at normal mean levels (< 0.4 μm) subsequently. The most common drug-related, investigator-assessed adverse events were diarrhoea (n = 16) and nausea (n = 12). CONCLUSIONS: At matched transfusional iron-loading rates, the responses of rare transfusion-dependent anaemias to deferasirox are similar at 1 yr, irrespective of the underlying pathogenic mechanism. © 2011 John Wiley & Sons A/S.
2011
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4
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Porter JB; Lin KH; Beris P; Forni GL; Taher A; Habr D; Domokos G; Roubert B; Thein SL; EPIC study investigators including Agaoglu L; Alimena G; Alonso D; Ame S; Angelucci E; Arrizabalaga B; Athanasiou-Metaxa M; Augustson B; Aydinok Y; Baba A; Baccarani M; Beck J; Beyne-Rauzy O; Birgens H; Bordessoule D; Borgna-Pignatti C; Bosly A; Bouabdallah K; Bowen D; Bron D; Cappellini MD; Capra M; Cartron G; Cazzola M; Chalkias C; Chan LL; Chancharunee S; Chapman C; Charoenkwan P; Chasapopoulou E; Cheze S; Chuansumrit A; Cianciulli P; Dauriac C; Delforge M; Dölken G; Dombret H; Duyster J; Economopoulos T; Ehninger G; Elalfy M; El-Beshlawy A; Enggaard L; Fenaux P; Fillet G; Filosa A; Galanello R; Ganser A; Gastl G; Gattermann N; Giraudier S; Goldfarb A; Grigg A; Guerci-Bresler A; Gumruk F; Ha SY; Haase D; Heinrich B; Hertzberg M; Ho J; Hsu HC; Huang S; Hunault-Berger M; Inusa B; Jalumes D; Jensen J; Kattamis A; Kilinc Y; Kim KH; Kinsey S; Kjeldsen L; Koren A; Lai ME; Lai Y; Lee JW; Lee KH; Lee SH; Legros L; Li C; Li CK; Li Q; Linkesch W; Lübbert M; Lutz D; Mohamed Thalha AJ; Mufti G; Muus P; Nobile F; Ozsahin H; Papadopoulos N; Perrotta S; Petrini M; Pfeilstöcker M; Piga A; Poole J; Pungolino E; Quarta G; Ravoet C; Remacha AF; Rose C; Roy L; Saglio G; Sanz G; Schmid M; Schmugge M; Schots H; Secchi G; Seymour JF; Shah F; Shah H; Shen Z; Slama B; Sutcharitchan P; Tamary H; Taylor K; Tesch HJ; Troncy J; Vassilieff D; Villegas A; Viprakasit V; Wainwright L; Wassmann B; Wettervald M; Will A; Wörmann B; Wright J; Yeh SP; Yoon SS; Zoumbos NC; Zweegman S
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2318/107549
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