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通过大豆或兔网织红细胞脂氧合酶氧化作用生成的具有氧化缩短型亚油酸残基的磷脂酰胆碱的结构鉴定。

Structural identification of phosphatidylcholines having an oxidatively shortened linoleate residue generated through its oxygenation with soybean or rabbit reticulocyte lipoxygenase.

作者信息

Tokumura A, Sumida T, Toujima M, Kogure K, Fukuzawa K, Takahashi Y, Yamamoto S

机构信息

Laboratory of Health Chemistry, School of Medicine, The University of Tokushima, 1-78 Shomachi, Tokushima 770-8505, Japan.

出版信息

J Lipid Res. 2000 Jun;41(6):953-62.

Abstract

Phosphatidylcholines (PCs) with platelet-activating factor (PAF)-like biological activities are known to be generated by fragmentation of the sn-2-esterified polyunsaturated fatty acyl group. The reaction is free radical-mediated and triggered by oxidants such as metal ions, oxyhemoglobin, and organic hydroperoxides. In this study, we characterized the PAF-like phospholipids produced on reaction of PC having a linoleate group with lipoxygenase enzymes at low oxygen concentrations. When the oxidized PCs were analyzed by gas chromatography-mass spectrometry, two types of oxidatively fragmented PC were detected. One PC had an sn-2-short chain saturated or unsaturated acyl group (C(8)-C(13)) with an aldehydic terminal; the abundant species were PCs with C(9) and C(13). The other PC had a short chain saturated acyl group (C(6)-C(9)) with a methyl terminal, and the most predominant species was PC with C(8). When the extracts of oxidation products were subjected to catalytic hydrogenation, PCs having saturated acyl groups (C(6)-C(14)) were detected; the most abundant was C(12) species. The less regiospecific formation of PAF-like lipids suggests that they were generated by oxidative fragmentation of PC hydroperoxides formed by non-stereoselective oxygenation of the alkyl radical of esterified linoleate that escaped from the active centers of lipoxygenases. One of the PAF-like PC with an aldehydic terminal was found to be bioactive; it inhibited the production of nitric oxide induced by lipopolysaccharide and interferon-gamma in vascular smooth muscle cells from rat aorta.

摘要

已知具有血小板活化因子(PAF)样生物活性的磷脂酰胆碱(PCs)是由sn-2-酯化多不饱和脂肪酰基的断裂产生的。该反应由自由基介导,并由金属离子、氧合血红蛋白和有机氢过氧化物等氧化剂引发。在本研究中,我们对在低氧浓度下具有亚油酸基团的PC与脂氧合酶反应产生的PAF样磷脂进行了表征。当通过气相色谱-质谱分析氧化的PC时,检测到两种类型的氧化断裂PC。一种PC具有带有醛基末端的sn-2-短链饱和或不饱和酰基(C(8)-C(13));丰富的种类是具有C(9)和C(13)的PCs。另一种PC具有带有甲基末端的短链饱和酰基(C(6)-C(9)),最主要的种类是具有C(8)的PC。当氧化产物的提取物进行催化氢化时,检测到具有饱和酰基(C(6)-C(14))的PCs;最丰富的是C(12)种类。PAF样脂质的区域特异性形成较少,这表明它们是由从脂氧合酶活性中心逸出的酯化亚油酸烷基自由基的非立体选择性氧化形成的PC氢过氧化物的氧化断裂产生的。发现一种带有醛基末端的PAF样PC具有生物活性;它抑制了大鼠主动脉血管平滑肌细胞中脂多糖和干扰素-γ诱导的一氧化氮的产生。

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