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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Characterization of prostaglandin E2 generation through the cyclooxygenase (COX)-2 pathway in human neutrophils.
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Characterization of prostaglandin E2 generation through the cyclooxygenase (COX)-2 pathway in human neutrophils.

机译:表征人类中性粒细胞中通过环氧合酶(COX)-2途径产生的前列腺素E2。

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摘要

In the present study, we characterized the generation of prostaglandin (PG)E2 in human neutrophils. We found that the Ca2+-dependent type IV cytosolic phospholipase A2 (cPLA2) was pivotally involved in the COX-2-mediated generation of PGE2 in response to a calcium ionophore, as determined by the use of selected PLA2 inhibitors. PGE2 biosynthesis elicited by bacterial-derived peptides or by phagocytic stimuli acting on cell surface receptors also showed to be dependent on cPLA2 activity. We then assessed metabolism of unesterified arachidonic acid (AA), and observed that PGE2 production becomes favored over that of LTB4 with higher AA concentrations. Withdrawal of calcium prevented the generation of PGE2 in response to a calcium ionophore but did not affect the up-regulation of COX-2 or its capacity to convert AA, thus limiting its implication at the level of cPLA2 activation. Of the main eicosanoids produced by neutrophils, only LTB4 was able to up-regulate COX-2 expression. Finally, the only PGE synthase isoform found in neutrophils is microsomal PGE synthase-1; it co-localized with COX-2 and its expression appeared mainly constitutive. These results highlight key differences in regulatory processes of the 5-LO and COX pathways, and enhance our knowledge at several levels in the PGE2 biosynthesis in neutrophils.
机译:在本研究中,我们表征了人类嗜中性粒细胞中前列腺素(PG)E2的产生。我们发现,Ca2 +依赖的IV型胞质磷脂酶A2(cPLA2)关键地参与了COX-2介导的PGE2的生成,以响应钙离子载体,这通过使用选定的PLA2抑制剂来确定。由细菌衍生的肽或作用于细胞表面受体的吞噬刺激物引起的PGE2生物合成也显示依赖于cPLA2活性。然后,我们评估了未酯化花生四烯酸(AA)的代谢,并观察到PGA2的生产变得比具有较高AA浓度的LTB4的生产更受青睐。钙的吸收阻止了响应钙离子载体的PGE2的生成,但不影响COX-2的上调或其转化AA的能力,因此限制了它对cPLA2活化水平的影响。在中性粒细胞产生的主要类花生酸中,只有LTB4能够上调COX-2的表达。最后,在嗜中性粒细胞中发现的唯一PGE合酶同工型是微粒体PGE合酶-1。它与COX-2共定位,其表达主要是组成型的。这些结果突出了5-LO和COX途径调控过程的关键差异,并增强了我们在嗜中性粒细胞PGE2生物合成中几个层面的知识。

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