脂氧合酶代谢产物花生四烯酸和亚油酸通过调节蛋白激酶C调节肿瘤细胞对内皮细胞的粘附。

B Liu, J Timar, J Howlett, C A Diglio, K V Honn
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引用次数: 116

摘要

12(S)-羟基二十碳四烯酸(12[S]-HETE)和13(S)-羟基十八碳二烯酸(13[S]-HODE)分别是花生四烯酸和亚油酸的脂氧合酶代谢物,在转移过程中被认为调节肿瘤细胞对内皮的粘附。经12(S)-HETE处理后,大鼠沃克癌肉瘤(W256)细胞对大鼠内皮细胞单层的粘附增强,这种12(S)-HETE增强的粘附被13(S)-HODE阻断。蛋白激酶抑制剂staurosporine、calphostin C和1-(5-异喹啉-磺酰基)-2-甲基哌嗪可抑制12(S)- hete增强的W256细胞粘附。用phorbol 12-肉豆蔻酸-13-醋酸酯消耗W256细胞的蛋白激酶C (PKC),使其对12(S)-HETE的反应能力丧失。用12(S)-HETE处理W256细胞诱导PKC膜相关活性增加100%,而13(S)-HODE抑制12(S)-HETE对PKC易位的影响。高效液相色谱分析表明,在W256细胞中,12-HETE和13-HODE分别是花生四烯酸和亚油酸的两种主要脂氧合酶代谢产物。因此,这两种代谢物可能为PKC的调控提供了另一种信号通路。此外,这些发现表明,12(S)-HETE和13(S)-HODE对肿瘤细胞粘附内皮的调节可能是一个依赖pkc的过程。
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Lipoxygenase metabolites of arachidonic and linoleic acids modulate the adhesion of tumor cells to endothelium via regulation of protein kinase C.

12(S)-hydroxyeicosatetraenoic acid (12[S]-HETE) and 13(S)-hydroxyoctadecadienoic acid (13[S]-HODE), lipoxygenase metabolites of arachidonic acid and linoleic acid, respectively, previously have been suggested to regulate tumor cell adhesion to endothelium during metastasis. Adhesion of rat Walker carcinosarcoma (W256) cells to a rat endothelial cell monolayer was enhanced after treatment with 12(S)-HETE and this 12(S)-HETE enhanced adhesion was blocked by 13(S)-HODE. Protein kinase inhibitors, staurosporine, calphostin C, and 1-(5-isoquinoline-sulfonyl)-2-methylpiperazine, inhibited the 12(S)-HETE enhanced W256 cell adhesion. Depleting W256 cells of protein kinase C (PKC) with phorbol 12-myristate-13-acetate abolished their ability to respond to 12(S)-HETE. Treatment of W256 cells with 12(S)-HETE induced a 100% increase in membrane-associated PKC activity whereas 13(S)-HODE inhibited the effect of 12(S)-HETE on PKC translocation. High-performance liquid chromatographic analysis revealed that in W256 cells 12-HETE and 13-HODE were two of the major lipoxygenase metabilites of arachidonic acid and linoleic acid, respectively. Therefore, these two metabolites may provide an alternative signaling pathway for the regulation of PKC. Further, these findings suggest that the regulation of tumor cell adhesion to endothelium by 12(S)-HETE and 13(S)-HODE may be a PKC-dependent process.

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