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依洛前列素可抑制猪肺动脉中由血栓素A2类似物U46619、8-异前列腺素F2α、前列腺素F2α、细胞因子和内毒素诱导的超氧化物形成及gp91phox表达。

Iloprost inhibits superoxide formation and gp91phox expression induced by the thromboxane A2 analogue U46619, 8-isoprostane F2alpha, prostaglandin F2alpha, cytokines and endotoxin in the pig pulmonary artery.

作者信息

Muzaffar Saima, Shukla Nilima, Lobo Clinton, Angelini Gianni D, Jeremy Jamie Y

机构信息

Department of Cardiac Surgery, Bristol Heart Institute, Bristol Royal Infirmary, University of Bristol.

出版信息

Br J Pharmacol. 2004 Feb;141(3):488-96. doi: 10.1038/sj.bjp.0705626. Epub 2004 Jan 12.

Abstract

Since the roles of thromboxane A2 (TXA2), prostacyclin (PGI2) and 8-isoprostane F2alpha in mediating vascular O2*- formation and its relation to adult respiratory distress syndrome (ARDS) is unknown, the effects of these eicosanoids on the expression of gp91phox (catalytic subunit of NADPH oxidase) and O2*- release from cultured pig pulmonary artery (PA) segments, PA vascular smooth muscle cells (PAVSMCs) and PA endothelial cells (PAECs) were investigated. PA segments, PAVSMCs and PAECs were incubated with the TXA2 analogue, U46619, (+/-LPS, tumour necrosing factor-alpha (TNF-alpha) or IL-1alpha), 8-isoprostane F2alpha and+/-iloprost (a stable PGI2 analogue) for 16 h. The formation of superoxide dismutase-inhibitable O2*- was then measured spectrophotometrically and gp91phox expression assessed using Western blotting. In parallel experiments, whole PA segments were treated with LPS, TNF-alpha and IL-alpha after which time TXA2, PGI2, PGF2alpha and 8-isoprostane F2alpha formation was measured using enzyme-linked immunoassays. U46619, PGF2alpha and 8-isoprostane F2alpha promoted the formation of O2*- in PA segments, PAVSMCs and PAECs, an effect inhibited by diphenyleneiodonium and apocynin (both NADPH oxidase inhibitors) and upregulated the expression of gp91phox in PAECs and PAVSMCs. These effects were augmented by LPS, TNF-alpha and IL-1alpha but inhibited by iloprost. Under identical incubation conditions, IL-1alpha, LPS and TNF-alpha all induced an increase in the formation of TXA2, PGF2alpha and 8-isoprostane F2alpha but reduced the concomitant formation of PGI2. These data demonstrate that LPS and cytokines influence the relative balance of TXA2, PGI2, PGF2alpha and 8-isoprostane F2alpha in pig PA, which in turn alter NADPH oxidase expression and O2*- formation. These novel findings have implications in devising effective strategies for treating ARDS.British Journal of Pharmacology (2004) 141, 488-496. doi:10.1038/sj.bjp.0705626

摘要

由于血栓素A2(TXA2)、前列环素(PGI2)和8-异前列腺素F2α在介导血管超氧阴离子(O2*)形成中的作用及其与成人呼吸窘迫综合征(ARDS)的关系尚不清楚,因此研究了这些类花生酸对培养的猪肺动脉(PA)段、PA血管平滑肌细胞(PAVSMC)和PA内皮细胞(PAEC)中gp91phox(NADPH氧化酶的催化亚基)表达和O2释放的影响。将PA段、PAVSMC和PAEC与TXA2类似物U46619、(±脂多糖、肿瘤坏死因子-α(TNF-α)或白细胞介素-1α)、8-异前列腺素F2α和±伊洛前列素(一种稳定的PGI2类似物)孵育16小时。然后用分光光度法测定超氧化物歧化酶抑制性O2的形成,并使用蛋白质免疫印迹法评估gp91phox的表达。在平行实验中,用脂多糖、TNF-α和白细胞介素-α处理整个PA段,之后使用酶联免疫吸附测定法测量TXA2、PGI2、PGF2α和8-异前列腺素F2α的形成。U46619、PGF2α和8-异前列腺素F2α促进PA段、PAVSMC和PAEC中O2的形成,二亚苯基碘鎓和夹竹桃麻素(均为NADPH氧化酶抑制剂)可抑制这种作用,并且上调PAEC和PAVSMC中gp91phox的表达。脂多糖、TNF-α和白细胞介素-1α增强了这些作用,但伊洛前列素可抑制这些作用。在相同的孵育条件下,白细胞介素-1α、脂多糖和TNF-α均诱导TXA2、PGF2α和8-异前列腺素F2α的形成增加,但减少了PGI2的同时形成。这些数据表明,脂多糖和细胞因子影响猪PA中TXA2、PGI2、PGF2α和8-异前列腺素F2α的相对平衡,这反过来又改变了NADPH氧化酶的表达和O2的形成。这些新发现对设计治疗ARDS的有效策略具有重要意义。《英国药理学杂志》(2004年)141卷,488 - 496页。doi:10.1038/sj.bjp.0705626

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