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焦磷酸盐和去铁胺给药后高铁血症小鼠体内[59Fe]柠檬酸铁生物分布的改变。

Alterations of the [59Fe]ferric citrate biodistribution in hyperferremic mice after the administration of pyrophosphate and desferrioxamine.

作者信息

Sawas-Dimopoulou C, Soulpi C

出版信息

J Pharmacol Exp Ther. 1983 Feb;224(2):415-8.

PMID:6296362
Abstract

One of the most efficient anions in enhancing the ability of desferrioxamine (DFO) to remove iron from transferrin in vitro has been shown to be pyrophosphate (PYP). To evaluate the in vivo effect of PYP in hyperferremic mice, the biodistribution of [59Fe]ferric citrate was studied after the i.p. administration of: 1) only saline in the control animals; 2) an aqueous solution of tetrasodium diphosphate (PYP; 40 gm/2 g of b.wt.); 3) desferral (DFO; 12 mg/20 g of b.wt.); and 4) PYP + DFO at the respective dosages shown above. The radioactivity in each organ, blood, urine and feces was measured and referred to as percentage of the injected dose. PYP administered alone acted as a weaker chelator of iron than DFO. The combined administration of DFO and PYP contributed more than DFO or PYP separately, to the increase of urinary excretion of 59Fe and to the significant decrease of the radioiron concentration in liver (.01 less than P less than .05). The above induced changes are not, however, the additive result of the separate effect of DFO and PYP. That observation would suggest that DFO + PYP combined in a unique treatment, interact with iron through a common reaction pathway and that PYP plays in vivo a synergistic role in that interaction. The kind of iron with which DFO + PYP interacts is then suggested to be the transferrin-bound iron located in extracellular spaces of tissues.

摘要

已证明焦磷酸(PYP)是在体外增强去铁胺(DFO)从转铁蛋白中去除铁能力的最有效阴离子之一。为了评估PYP对高铁血症小鼠的体内作用,在腹腔注射以下物质后研究了[59Fe]柠檬酸铁的生物分布:1)对照组动物仅注射生理盐水;2)焦磷酸四钠水溶液(PYP;40克/2克体重);3)去铁胺(DFO;12毫克/20克体重);4)上述各自剂量的PYP + DFO。测量每个器官、血液、尿液和粪便中的放射性,并将其表示为注射剂量的百分比。单独给予PYP作为铁螯合剂的作用比DFO弱。DFO和PYP联合给药比单独给予DFO或PYP对59Fe尿排泄的增加和肝脏中放射性铁浓度的显著降低(0.01 < P < 0.05)贡献更大。然而,上述诱导变化并非DFO和PYP单独作用的累加结果。该观察结果表明,DFO + PYP联合用于独特治疗时,通过共同反应途径与铁相互作用,并且PYP在该相互作用中在体内起协同作用。然后推测DFO + PYP与之相互作用的铁是位于组织细胞外空间的转铁蛋白结合铁。

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