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实验性炎症急性和慢性期的铁代谢与氧化应激:右旋糖酐铁和去铁胺的作用

Iron metabolism and oxidative stress during acute and chronic phases of experimental inflammation: effect of iron-dextran and deferoxamine.

作者信息

Muntané J, Puig-Parellada P, Mitjavila M T

机构信息

Department of Physiology, Faculty of Biology, University of Barcelona, Spain.

出版信息

J Lab Clin Med. 1995 Nov;126(5):435-43.

PMID:7595028
Abstract

Iron overload induces a rise in lipid peroxidation, but there are no data on the effects of iron administered in vivo on the production of free radicals by inflammatory cells. Further, there is lack of agreement about the benefits of deferoxamine (Dfx) in the treatment of anemia and oxidative stress during inflammation and chronic diseases. In this study, iron-dextran (Fe-dextran) or Dfx was administered subcutaneously during the acute and chronic phases of carrageenan-induced granuloma. Several parameters related to iron metabolism, inflammatory cell activity, and lipid peroxidation were measured in liver, plasma, and the inflammatory exudate. Treatment with Fe-dextran increased iron content in plasma and in stores, increased production of superoxide anion (O2-) by inflammatory cells and lipid peroxidation, and also altered the inflammatory process. Dfx mobilized iron from stores without modifying essential parameters related to anemia or to the level of lipid peroxidation induced by inflammation. We conclude that treatment with Fe-dextran had a beneficial effect on recovery from the anemia of inflammation. Nevertheless, the high levels of loosely-bound iron found after Fe-dextran treatment in plasma and in exudate contribute to the increase in oxidative stress. Dfx treatment had no effect on anemia or on lipid peroxidation.

摘要

铁过载会导致脂质过氧化增加,但尚无关于体内给予铁对炎症细胞产生自由基影响的数据。此外,对于去铁胺(Dfx)在治疗炎症和慢性疾病期间的贫血及氧化应激方面的益处,尚无定论。在本研究中,在角叉菜胶诱导的肉芽肿急性期和慢性期皮下给予右旋糖酐铁(Fe-右旋糖酐)或Dfx。在肝脏、血浆和炎性渗出物中测量了与铁代谢、炎症细胞活性和脂质过氧化相关的几个参数。Fe-右旋糖酐治疗增加了血浆和储存铁中的铁含量,增加了炎症细胞产生超氧阴离子(O2-)和脂质过氧化,并且还改变了炎症过程。Dfx从储存中动员铁,而不改变与贫血或炎症诱导的脂质过氧化水平相关的基本参数。我们得出结论,Fe-右旋糖酐治疗对炎症性贫血的恢复有有益作用。然而,Fe-右旋糖酐治疗后在血浆和渗出物中发现的高水平松散结合铁导致氧化应激增加。Dfx治疗对贫血或脂质过氧化没有影响。

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