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铁螯合剂可抑制人体血小板聚集、血栓素A2合成及脂氧合酶活性。

Iron chelators inhibit human platelet aggregation, thromboxane A2 synthesis and lipoxygenase activity.

作者信息

Barradas M A, Jeremy J Y, Kontoghiorghes G J, Mikhailidis D P, Hoffbrand A V, Dandona P

机构信息

Department of Chemical Pathology and Human Metabolism, Royal Free Hospital and School of Medicine, London, England.

出版信息

FEBS Lett. 1989 Mar 13;245(1-2):105-9. doi: 10.1016/0014-5793(89)80201-7.

Abstract

The iron chelators desferrioxamine and 1,2-dimethyl-3-hydroxypyrid-4-one (L1) inhibited human platelet aggregation in vitro as well as thromboxane A2 synthesis and conversion of arachidonate to lipoxygenase-derived products. Non-chelating compounds related to L1 were without effect on cyclooxygenase or lipoxygenase activity. Since both cyclooxygenase and lipoxygenase are iron-containing enzymes, it is suggested that the inhibition of platelet function by these iron chelators may be related to the removal or binding of iron associated with these enzymes. These iron chelators may therefore be of potential therapeutic value as platelet antiaggregatory agents and of possible use in the treatment of atherosclerotic and inflammatory joint diseases.

摘要

铁螯合剂去铁胺和1,2 - 二甲基 - 3 - 羟基吡啶 - 4 - 酮(L1)在体外可抑制人血小板聚集以及血栓素A2的合成,并抑制花生四烯酸向脂氧合酶衍生产物的转化。与L1相关的非螯合化合物对环氧化酶或脂氧合酶活性无影响。由于环氧化酶和脂氧合酶都是含铁酶,因此有人提出这些铁螯合剂对血小板功能的抑制可能与去除或结合与这些酶相关的铁有关。因此,这些铁螯合剂作为血小板抗聚集剂可能具有潜在的治疗价值,并可能用于治疗动脉粥样硬化和炎性关节疾病。

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