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HBED配体:去铁胺治疗慢性铁过载和急性铁中毒潜在替代物的临床前研究

HBED ligand: preclinical studies of a potential alternative to deferoxamine for treatment of chronic iron overload and acute iron poisoning.

作者信息

Bergeron Raymond J, Wiegand Jan, Brittenham Gary M

机构信息

Department of Medicinal Chemistry, University of Florida, Gainesville 32610, USA.

出版信息

Blood. 2002 Apr 15;99(8):3019-26. doi: 10.1182/blood.v99.8.3019.

Abstract

We have continued the preclinical evaluation of the efficacy and safety of the hexadentate phenolic aminocarboxylate iron chelator N, N'-bis(2-hydroxybenzyl) ethylenediamine-N, N'-diacetic acid monosodium salt (NaHBED) for the treatment of both chronic transfusional iron overload and acute iron poisoning. We examined the effect of route of administration by giving equimolar amounts of NaHBED and deferoxamine (DFO) to Cebus apella monkeys as either a subcutaneous (SC) bolus or a 20-minute intravenous (IV) infusion. By both routes, NaHBED was consistently about twice as efficient as DFO in producing iron excretion. For both chelators at a dose of 150 micromol/kg, SC was more efficient than IV administration. The biochemical and histopathologic effects of NaHBED administration were assessed. No systemic toxicity was found after either IV administration once daily for 14 days to iron-loaded dogs or after SC administration every other day for 14 days to dogs without iron overload. Evidence of local irritation was found at some SC injection sites. When the NaHBED concentration was reduced to 15% or less in a volume comparable to a clinically useful one, no local irritation was found with SC administration in rats. Because treatment of acute iron poisoning may require rapid chelator infusion, we compared the effects of IV bolus administration of the compounds to normotensive rats. Administration of DFO produced a prompt, prolonged drop in blood pressure and acceleration of heart rate; NaHBED had little effect. NaHBED may provide an alternative to DFO for the treatment of both chronic transfusional iron overload and of acute iron poisoning.

摘要

我们继续对六齿酚氨基羧酸盐铁螯合剂N,N'-双(2-羟基苄基)乙二胺-N,N'-二乙酸单钠盐(NaHBED)治疗慢性输血性铁过载和急性铁中毒的疗效和安全性进行临床前评估。我们通过给僧帽猴皮下(SC)推注或20分钟静脉(IV)输注等摩尔量的NaHBED和去铁胺(DFO)来研究给药途径的影响。通过这两种途径,NaHBED在促进铁排泄方面的效率始终约为DFO的两倍。对于剂量为150微摩尔/千克的两种螯合剂,皮下给药比静脉给药更有效。评估了NaHBED给药的生化和组织病理学影响。对铁负荷犬每日静脉给药一次,持续14天,或对无铁过载犬隔日皮下给药,持续14天,均未发现全身毒性。在一些皮下注射部位发现了局部刺激的证据。当在与临床可用体积相当的体积中将NaHBED浓度降至15%或更低时,大鼠皮下给药未发现局部刺激。由于治疗急性铁中毒可能需要快速输注螯合剂,我们比较了化合物静脉推注对血压正常大鼠的影响。给予DFO会导致血压迅速、持续下降和心率加快;NaHBED的影响很小。NaHBED可能为治疗慢性输血性铁过载和急性铁中毒提供一种替代DFO的药物。

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