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花生四烯酸的12-氢过氧化物衍生物对人血小板中二十碳烯酸脂氧化作用的增强

Enhancement of eicosaenoic acid lipoxygenation in human platelets by 12-hydroperoxy derivative of arachidonic acid.

作者信息

Croset M, Lagarde M

出版信息

Lipids. 1985 Nov;20(11):743-50. doi: 10.1007/BF02534397.

Abstract

Human platelet lipoxygenase activity toward several eicosaenoic acids was measured in intact cells as well as in subcellular fractions (cytosol and membranes). In whole platelets, the lipoxygenation of eicosaenoic acids was enhanced greatly by high concentration of aspirin, which partially inhibit the peroxidase activity associated with the pathway. The lipoxygenation also was increased by arachidonic acid (AA) or its lipoxygenase product, 12-hydroxyperoxy-eicosatetraenoic acid (12-HPETE). Similarly, prostanoid precursors, dihomogammalinolenic (DHLA) and eicosapentaenoic (EPA) acids also were better converted by cyclooxygenase in the presence of AA or 12-HPETE. Among the eicosaenoic acids tested, EPA oxygenation was affected most. Using cytosol or membranes as the lipoxygenase source instead of whole cells led to completely different results. AA exerted a competitive inhibition upon the other eicosaenoic acid oxygenation except that of EPA, for which a dual effect of AA was observed. This makes questionable the use of platelet subfractions for investigating lipoxygenase activity. We conclude that platelet lipoxygenation of eicosaenoic acids appears peroxide-dependent, especially for apparent poor substrates like EPA. This might be relevant in respect to 12-HPETE, which is the main hydroperoxy derivative to be produced during platelet activation.

摘要

在完整细胞以及亚细胞组分(胞质溶胶和细胞膜)中测定了人血小板脂氧合酶对几种二十碳烯酸的活性。在完整血小板中,高浓度阿司匹林可极大地增强二十碳烯酸的脂氧合作用,阿司匹林可部分抑制与该途径相关的过氧化物酶活性。花生四烯酸(AA)或其脂氧合酶产物12-羟基过氧化二十碳四烯酸(12-HPETE)也可增加脂氧合作用。同样,在存在AA或12-HPETE的情况下,前列腺素前体二高-γ-亚麻酸(DHLA)和二十碳五烯酸(EPA)也能被环氧化酶更好地转化。在所测试的二十碳烯酸中,EPA的氧化受到的影响最大。使用胞质溶胶或细胞膜作为脂氧合酶来源而非完整细胞会导致完全不同的结果。除了EPA外,AA对其他二十碳烯酸的氧化具有竞争性抑制作用,而对于EPA,观察到AA具有双重作用。这使得使用血小板亚组分来研究脂氧合酶活性存在疑问。我们得出结论,二十碳烯酸的血小板脂氧合作用似乎依赖于过氧化物,尤其是对于像EPA这样明显较差的底物。这可能与12-HPETE有关,12-HPETE是血小板激活过程中产生的主要氢过氧化物衍生物。

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