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  4. Iron chelation therapy in the management of thalassemia: The Asian perspectives
 
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Iron chelation therapy in the management of thalassemia: The Asian perspectives

Journal
International Journal of Hematology
Journal Volume
90
Journal Issue
4
Pages
435-445
Date Issued
2009
Author(s)
KAI-HSIN LIN  
Viprakasit, Vip
Lee-Lee, Chan
Chong, Quah Thuan
Lin, Kai-Hsin
Khuhapinant, Archrob
DOI
10.1007/s12185-009-0432-0
URI
http://www.scopus.com/inward/record.url?eid=2-s2.0-73449090407&partnerID=MN8TOARS
http://scholars.lib.ntu.edu.tw/handle/123456789/353804
Abstract
Worldwide, thalassemia is the most commonly inherited hemolytic anemia, and it is most prevalent in Asia and the Middle East. Iron overload represents a significant problem in patients with transfusion-dependent β-thalassemia. Chelation therapy with deferoxamine has traditionally been the standard therapeutic option but its usage is tempered by suboptimal patient compliance due to the discomfort and demands associated with the administration regimen. Therefore, a great deal of attention has been focused on the development of oral chelating agents. Deferiprone, even though available for nearly two decades in Asia with recent encouraging data on cardiac iron removal and long-term efficacy, has serious adverse effects including agranulocytosis and neutropenia which has impeded it from routine clinical practice. A novel oral chelator; deferasirox is effective throughout a 24 h dosing period and both preclinical and clinical data indicate that it successfully removes both hepatic and cardiac iron. In Asia, optimal management of severe thalassemia patients and the availability and access to oral iron chelators still presents a major challenge in many countries. In this regard, the development and implementation of consensus guidelines for management of Asian patients with transfusion-dependent thalassemia will be a major step towards improving and maintaining the continuity of patient care. ? 2009 The Japanese Society of Hematology.
Subjects
Deferasirox; Deferiprone; Deferoxamine; Iron chelation therapy; Thalassemia
SDGs

[SDGs]SDG3

Other Subjects
creatinine; deferasirox; deferiprone; deferoxamine; deferoxamine mesylate; ferritin; transferrin; abdominal discomfort; agranulocytosis; arthralgia; arthritis; arthropathy; Asia; beta thalassemia; blood transfusion; bone growth; clinical practice; clinical trial; continuous infusion; creatinine blood level; drug bioavailability; drug dose escalation; drug dose reduction; drug dose titration; drug efficacy; drug eruption; drug excretion; drug half life; drug megadose; drug protein binding; drug substitution; drug withdrawal; eye toxicity; ferritin blood level; gastrointestinal symptom; growth retardation; human; iron chelation; iron overload; kidney failure; leukocyte count; maximum plasma concentration; monotherapy; nausea; neutropenia; ototoxicity; patient care; patient compliance; practice guideline; recommended drug dose; retina disease; retinal toxicity; review; side effect; thalassemia; vomiting; Asia; beta-Thalassemia; Blood Transfusion; Chelation Therapy; Cross-Cultural Comparison; Drug Administration Routes; Health Care Costs; Humans; Iron Chelating Agents; Iron Overload; Practice Guidelines as Topic; Prevalence; Thalassemia
Type
journal article

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