Effective chelation of iron in beta thalassaemia with the oral chelator 1,2-dimethyl-3-hydroxypyrid-4-one.
George J. Kontoghiorghes,M A Aldouri,A. V. Hoffbrand,J. Barr,Beatrix Wonke,T Kourouclaris,L Sheppard +6 more
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The results suggest that the oral chelator 1,2-dimethyl-3-hydroxypyrid-4-one is as effective as subcutaneous desferrioxamine in increasing urinary iron excretion in patients loaded with iron.Abstract:
The main iron chelator used for transfusional iron overload is desferrioxamine, which is expensive, has toxic side effects, and has to be given subcutaneously. An orally active iron chelator is therefore required. The effects of oral 1,2-dimethyl-3-hydroxypyrid-4-one on urinary iron excretion were studied in eight patients who had received multiple transfusions: four had myelodysplasia and four beta thalassaemia major. Different daily doses of the drug up to 100 mg/kg/day, alone or in combination with ascorbic acid, were used. In three patients with thalassaemia the effect of the drug was compared with that of subcutaneous desferrioxamine at the same daily dose. In all eight patients a single dose of oral 1,2-dimethyl-3-hydroxypyrid-4-one resulted in substantial urinary iron excretion, mainly in the first 12 hours. Urinary iron excretion increased with the dose and with the degree of iron loading of the patient. Giving two or three divided doses over 24 hours resulted in higher urinary iron excretion than a single dose of the same amount over the same time. In most patients coadministration of oral ascorbic acid further increased urinary iron excretion. 1,2-Dimethyl-3-hydroxypyrid-4-one caused similar iron excretion to that achieved with subcutaneous desferrioxamine at a comparable dose. In some cases the iron excretion was sufficiently high (maximum 99 mg/day) to suggest that a negative iron balance could be easily achieved with these protocols in patients receiving regular transfusions. No evidence of toxicity was observed on thorough clinical examination or haematological and biochemical testing in any of the patients. None of the patients had any symptoms that could be ascribed to the drug. These results suggest that the oral chelator 1,2-dimethyl-3-hydroxypyrid-4-one is as effective as subcutaneous desferrioxamine in increasing urinary iron excretion in patients loaded with iron. Its cheap synthesis, oral activity, and lack of obvious toxicity at effective doses suggest that it should be developed quickly and thoroughly tested for the management of transfusional iron overload.read more
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Iron-chelating therapy and the treatment of thalassemia
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Improved survival of thalassaemia major in the UK and relation to T2* cardiovascular magnetic resonance
TL;DR: Since 1999, there has been a marked improvement in survival in thalassaemia major in the UK, which has been mainly driven by a reduction in deaths due to cardiac iron overload.
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Protection against tissue damage in vivo by desferrioxamine: what is its mechanism of action?
TL;DR: Desferrioxamine (deferoxamine) is an inhibitor of iron-dependent free radical reactions that has been used to investigate the role of such reactions in several animal model systems for human disease as mentioned in this paper.
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Practical management of iron overload
TL;DR: The ability to estimate the distribution of excess tissue iron, to predict its consequences and therefore to tailor treatment accordingly is surprisingly imprecise and the safest and most effective ways of removing excess iron vary depending on the degree and rate of iron loading as well as the underlying condition being treated.
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A delicate balance: Iron metabolism and diseases of the brain
TL;DR: This review focuses on how iron metabolism is maintained in the brain, and how an alteration to iron and iron metabolism adversely affects neurological function.
References
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Visual and Auditory Neurotoxicity in Patients Receiving Subcutaneous Deferoxamine Infusions
Nancy F. Olivieri,Buncic,Emily Y. Chew,Tsvi Gallant,Robert V. Harrison,Nancy K. Keenan,William J. Logan,David J. Mitchell,Ricci G,Barry Skarf +9 more
TL;DR: Of 89 patients receiving nightly subcutaneous deferoxamine for transfusion-dependent thalassemia major or Diamond-Blackfan anemia, 13 presented with visual loss or deafness of acute onset or both, and detailed ophthalmologic, audiologic, and evoked-potential studies uncovered abnormalities caused by neurotoxicity in 27 more.
Journal ArticleDOI
Continuous Subcutaneous Administration of Deferoxamine in Patients with Iron Overload
Richard D. Propper,Richard D. Propper,Barry J. Cooper,Barry J. Cooper,Robert R. Rufo,Robert R. Rufo,Arthur W. Nienhuis,Arthur W. Nienhuis,W. French Anderson,W. French Anderson,H. Franklin Bunn,H. Franklin Bunn,Amnon Rosenthal,David G. Nathan,David G. Nathan +14 more
TL;DR: Constant subcutaneous deferoxamine administration may prove to be an effective and practical means of eliminating large quantities of iron in siderosis.
Journal ArticleDOI
1,2-dimethyl-3-hydroxypyrid-4-one, an orally active chelator for treatment of iron overload
TL;DR: Urinary iron excretion increased substantially in all three patients and in the one tested was equal to that achieved with comparable doses of subcutaneous desferrioxamine, and the drug was well tolerated.
Journal ArticleDOI
Ferrioxamine excretion in iron-loaded man
M. J. Pippard,M. J. Pippard,Sheila T. Callender,Sheila T. Callender,Clement A. Finch,Clement A. Finch +5 more
TL;DR: These studies indicate the importance of biliary iron excretion in monitoring the effectiveness of desferrioxamine and suggest that large chelator doses may remove established iron overload much more rapidly than has previously been realized.
Journal ArticleDOI
Subcutaneous infusion and intramuscular injection of desferrioxamine in patients with transfusional iron overload
TL;DR: Continuous subcutaneous infusion of D.F. produces more iron excretion in patients with iron overload than intramuscular injection, and may prove a valuable means of preventing or treating iron overload in anaemic patients maintained on regular blood-transfusions.