5(S),15(S)-dihydroxyeicosatetraenoic acid and lipoxin generation in human polymorphonuclear cells: dual specificity of 5-lipoxygenase towards endogenous and exogenous precursors.

C Chavis; I Vachier; P Chanez; J Bousquet; P Godard

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5(S),15(S)-dihydroxyeicosatetraenoic acid and lipoxin generation in human polymorphonuclear cells: dual specificity of 5-lipoxygenase towards endogenous and exogenous precursors.

机译：5（S），15（S）-二羟基二十碳四烯酸和人多形核细胞中脂蛋白的生成：5-脂氧合酶对内源性和外源性前体的双重特异性。

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5-Lipoxygenase activation of human blood polymorphonuclear cells (PMN) from asthmatic patients (asthmatics) was studied to investigate whether differences may exist with healthy subjects (controls). The respective cell capacities to produce lipoxins (LXs), leukotrienes, and 5(S), 15(S)-dihydroxyeicosatetraenoic acid [5(S),15(S)-diHETE] were compared under in vitro stimulation by ionophore A23187, with or without exogenous 15(S)-hydroxyeicosatetraenoic acid [15(S)-diHETE]. Eicosanoids were analyzed by elution with an isocratic reverse-phase high performance liquid chromatography system, and their profiles, detected by simultaneous monitoring at 302, 280, and 246 nm, were evaluated on the basis of chromatographic behavior: UV spectral characteristics and coelution with synthetic standards. In the presence of exogenous 15(S)-HETE, human PMN were able to produce LXs and 5(S),15(S)-diHETE, PMN from asthmatics were able to produce 5(S), 5(S),15(S)-diHETE, and LXs from endogenous sources, whereas in the same experimental conditions, no detectable amounts of these compounds were released by PMN from controls. The levels of 5(S),15(S)-diHETE, and LXs biosynthesized from endogenous arachidonic acid were highly correlated. Two different LX patterns were observed involving two possible metabolic pathways: (a) via the intermediate 5,6-epoxytetraene alone for LXs generation from exogenous 15(S)-HETE; and (b) via 5,6- and/or 14,15-epoxytetraenes leading to the formation of an enzyme-bound delocalized carbocation for LXs generation from endogenous arachidonate, respectively. The enhanced 5-lipoxygenase activation of blood PMN from asthmatics and the metabolism of exogenous 15(S)-HETE may reflect a priming induced by various mediators released from environmental cells, and could be considered as a model of transcellular signalization between PMN and endothelial cells.

机译：研究哮喘患者（哮喘患者）的人血多形核细胞（PMN）的5-脂氧合酶激活，以研究与健康受试者（对照组）是否存在差异。在离子载体A23187体外刺激下，比较了产生脂蛋白（LXs），白三烯和5（S），15（S）-二羟基二十碳四烯酸[5（S），15（S）-diHETE]的各个细胞的能力。或不含外源15（S）-羟基二十碳四烯酸[15（S）-diHETE]。通过使用等度反相高效液相色谱系统洗脱来分析类花生酸，并根据色谱行为评估其分布图，并同时在302、280和246 nm处进行监测：紫外光谱特征和与合成的共洗脱标准。在存在外源15（S）-HETE的情况下，人类PMN能够产生LX，而5（S），15（S）-diHETE则来自哮喘患者的PMN能够产生5（S），5（S），15 （S）-diHETE和LX来自内源，而在相同的实验条件下，PMN不能从对照中释放出可检测量的这些化合物。由内源性花生四烯酸生物合成的5（S），15（S）-diHETE和LXs的水平高度相关。观察到两种不同的LX模式，涉及两种可能的代谢途径：（a）仅通过中间体5,6-环氧四烯用于从外源15（S）-HETE产生LXs; （b）通过5，6-和/或14，15-环氧四烯分别导致内源性花生四烯酸生成LXs的酶结合的离域碳正离子化。哮喘患者血液中PMN的5-脂氧合酶激活增强以及外源15（S）-HETE的代谢可能反映了由环境细胞释放的各种介体诱导的启动作用，可以被视为PMN与内皮细胞之间的跨细胞信号转导模型。

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《The Journal of Experomental Medicine》 |1996年第4期|共11页
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C Chavis; I Vachier; P Chanez; J Bousquet; P Godard;
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6. 5(S)15(S)-dihydroxyeicosatetraenoic acid and lipoxin generation in human polymorphonuclear cells: dual specificity of 5-lipoxygenase towards endogenous and exogenous precursors [O] . 1996

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7. 5(S),15(S)-dihydroxyeicosatetraenoic acid and lipoxin generation in human polymorphonuclear cells: dual specificity of 5-lipoxygenase towards endogenous and exogenous precursors [O] . 1996

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5(S),15(S)-dihydroxyeicosatetraenoic acid and lipoxin generation in human polymorphonuclear cells: dual specificity of 5-lipoxygenase towards endogenous and exogenous precursors.

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