2010
DOI: 10.1124/dmd.109.030833
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Pharmacokinetics, Metabolism, and Disposition of Deferasirox in β-Thalassemic Patients with Transfusion-Dependent Iron Overload Who Are at Pharmacokinetic Steady State

Abstract: ABSTRACT:Deferasirox (ICL670) is a novel once-daily, orally administered iron chelator to treat chronic iron overload in patients with transfusiondependent anemias. Absorption, distribution, metabolism, and excretion of [ 14 C]deferasirox at pharmacokinetic steady state was investigated in five adult ␤-thalassemic patients. Deferasirox (1000 mg) was given orally once daily for 6 days to achieve steady state. On day 7, patients received a single oral 1000-mg dose (ϳ20 mg/kg) of [ 14 C]deferasirox (2.5 MBq). Blo… Show more

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Cited by 81 publications
(56 citation statements)
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“…16,19,21 Recent availability of an intravenous preparation of deferasirox (for investigational use only) has allowed pharmacokinetic assessments of bioavailability and volume of distribution, 22 and a radiolabeled form allows detailed description of metabolism in thalassemic patients. 23 We have studied patients with inadequate responses in liver iron or ferritin at doses above 30 mg/kg and compared them against patients with good response at lower doses. The two groups are distinguished by much lower exposure (area under the concentration/time curve) in the poor responders, an effect likely due to differential bioavailability (and not compliance or transfusion burden alone).…”
Section: Update On Clinical Trialsmentioning
confidence: 99%
“…16,19,21 Recent availability of an intravenous preparation of deferasirox (for investigational use only) has allowed pharmacokinetic assessments of bioavailability and volume of distribution, 22 and a radiolabeled form allows detailed description of metabolism in thalassemic patients. 23 We have studied patients with inadequate responses in liver iron or ferritin at doses above 30 mg/kg and compared them against patients with good response at lower doses. The two groups are distinguished by much lower exposure (area under the concentration/time curve) in the poor responders, an effect likely due to differential bioavailability (and not compliance or transfusion burden alone).…”
Section: Update On Clinical Trialsmentioning
confidence: 99%
“…In recent years, numerous papers have reported the use of high throughput bioanalytical procedures for the quantification of iron chelating drugs [8], [10], [13], [19], [20], [21], [22] and [23]. Those reporting the use of high performance liquid chromatography coupled with ultraviolet determination (HPLC UV) methods [8], [10], [13], [20] and [23], all applied methodology developed by Rouan in 2001 [19].…”
Section: Introductionmentioning
confidence: 99%
“…Those reporting the use of high performance liquid chromatography coupled with ultraviolet determination (HPLC UV) methods [8], [10], [13], [20] and [23], all applied methodology developed by Rouan in 2001 [19]. More recently liquid chromatographic methods based on mass spectrometry (LC MS MS) detection have been developed to this purpose [21] and [22], although MS facilities are not always available in standard hospital laboratories.…”
Section: Introductionmentioning
confidence: 99%
“…The synthetic chelator deferasirox is a bis-hydroxyphenyl-triazole that, in contrast to deferoxamine, is well absorbed from the gastrointestinal tract and cleared from the circulation slowly with a plasma half-life of 11 -19 h, supporting once-daily oral dosing Nisbet-Brown et al 2003;Waldmeier et al 2010). Because of low water solubility of the free ligand, deferasirox is administered as a suspension in water or fruit juice (Novartis Pharmaceuticals 2010).…”
Section: Chemistry Pharmacology and Administration In Practicementioning
confidence: 99%
“…Hepatocytes readily take up deferasirox, which chelates hepatocellular iron. Deferasirox-iron complexes are excreted in the bile (Waldmeier et al 2010).…”
Section: Chemistry Pharmacology and Administration In Practicementioning
confidence: 99%