首页> 外文期刊>Lipids >2-Polyunsaturated acyl lysophosphatidylethanolamine attenuates inflammatory response in zymosan A-induced peritonitis in mice.
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2-Polyunsaturated acyl lysophosphatidylethanolamine attenuates inflammatory response in zymosan A-induced peritonitis in mice.

机译:2-多不饱和酰基溶血磷脂酰乙醇胺可减轻酵母聚糖A诱发的小鼠腹膜炎的炎症反应。

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In the present study, the anti-inflammatory action of lysophosphatidylethanolamine (lysoPtdEtn), orally administered, in zymosan A-induced peritonitis was examined. Oral administration of 2-DHA-lysoPtdEtn (ED(50), ~111 mug/kg) or 2-ARA-lysoPtdEtn (ED(50), 221 mug/kg) was found to inhibit the plasma leakage in mice treated with zymosan A. In support of this, 2-polyunsaturated acyl-lysoPtdEtn diminished the formation of LTC(4), a lipid mediator responsible for vascular permeability. Next, 2-DHA-lysoPtdEtn (ED(50), 110 mug/kg) or 2-ARA-lysoPtdEtn (ED(50), 123 mug/kg) effectively inhibited the leukocyte extravasation into the peritoneum. Consistent with this, each polyunsaturated-lysoPtdEtn diminished the formation of LTB(4) and 12-HETE, potent chemotactic factors. Additionally, the level of pro-inflammatory mediator (IL-1 beta, IL-6, TNF-alpha or NO) was lowered remarkably in contrast to the augmentation of anti-inflammatory interleukin IL-10. Furthermore, 2-(15-HETE)-lysoPtdEtn and 2-(17-HDHE)-lysoPtdEtn, 15-lipoxygenation product of 2-ARA-lysoPtdEtn and 2-DHA-lysoPtdEtn, respectively, were more potent than corresponding lysoPtdEtn, suggesting the action of 2-acyl-lysoPtdEtn might be expressed through 15-lipoxygenation. In support of this, the formation of 15-HETE and LXA(4) was upgraded in accordance with an increasing dose of 2-ARA-lysoPtdEtn. Separately, anti-inflammatory actions, 2-polyunsaturated acyl-lysoPtdEtns also drastically diminished leukocyte infiltration in a later phase of zymosan A-induced peritonitis, indicating that these lipids also possess pro-resolving activity. Taken together, it is suggested that polyunsaturated lysoPtdEtns and their lipoxygenation derivatives, could be classified as potent anti-inflammatory lipids.
机译:在本研究中,研究了口服溶血磷脂酰乙醇胺(lysoPtdEtn)在酵母聚糖A诱导的腹膜炎中的抗炎作用。发现口服2-DHA-lysoPtdEtn(ED(50),〜111杯/公斤)或2-ARA-lysoPtdEtn(ED(50),221杯/公斤)抑制了经酵母聚糖A处理的小鼠的血浆渗漏为此,2-多不饱和酰基-lysoPtdEtn减少了LTC(4)的形成,LTC(4)是负责血管渗透性的脂质介体。接下来,2-DHA-lysoPtdEtn(ED(50),110杯/千克)或2-ARA-lysoPtdEtn(ED(50),123杯/千克)有效抑制白细胞渗入腹膜。与此相一致,每个多不饱和的lysoPtdEtn减少了LTB(4)和12-HETE(有效的趋化因子)的形成。此外,与抗炎性白介素IL-10的增加相反,促炎性介质(IL-1β,IL-6,TNF-α或NO)的水平显着降低。此外,2-ARA-lysoPtdEtn和2-DHA-lysoPtdEtn的2-(15-HETE)-lysoPtdEtn和2-(17-HDHE)-lysoPtdEtn分别比相应的lysoPtdEtn更有效。 2-酰基-lysoPtdEtn的作用可能通过15-脂氧合来表达。支持这一点的是,根据2-ARA-lysoPtdEtn剂量的增加,升级了15-HETE和LXA(4)的形成。另外,抗发炎作用是,2-多不饱和酰基-lysoPtdEtns在后来的酵母聚糖A诱导的腹膜炎的后期也显着减少了白细胞浸润,表明这些脂质也具有促分解活性。两者合计,建议多不饱和的lysoPtdEtns及其脂氧合衍生物,可以归类为有效的抗炎脂质。

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