Pharmacokinetics of the oral iron chelator deferiprone (L1) in patients with iron overload

Abstract

Summary. Single oral dose pharmacokinetics of the iron chelator deferiprone (L₁) were studied in 24 patients with chronic iron overload and correlated with 24h urinary iron excretion (UIE) and creatinine clearance. Absorption of L₁ was rapid with a t_1/2 of 22·2 pL 17·7 (mean pL SD) min. The elimination half‐life (elt_1/2) of the drug was 91·1 pL 33·1 min and of its metabolite, L₁‐glucuronide (L₁G) 147·7pL 52·0 min. Creatinine clearance of the patients correlated significantly with the elimination t_1/2 of L₁G (r= ‐0·79, P= 0·002). There was also a significant correlation between 24 h UIE in the 14 patients studied and L₁ versus time area under the curve (AUC) (P= 0·007). The total amount of L₁ recovered in urine in 24 h comprised 77·9 pL 13·3% of the L₁ dose. L₁ efficiency (the 24 h UIE divided by the amount of iron the oral dose of L₁ is capable of binding) in the 14 patients was 3·8 pL 1·9%. These data show for the first time that the urinary elimination of L₁G is influenced by the renal function of the patient. Although no significant accumulation of L₁ and L₁G will occur in most of the patients if L₁ is given more than once daily, in some patients with impaired renal function, L₁G may accumulate.