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首页> 外文期刊>Chemical research in toxicology >Nitration of unsaturated fatty acids by nitric oxide-derived reactive nitrogen species peroxynitrite, nitrous acid, nitrogen dioxide, and nitronium ion.
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Nitration of unsaturated fatty acids by nitric oxide-derived reactive nitrogen species peroxynitrite, nitrous acid, nitrogen dioxide, and nitronium ion.

机译:一氧化氮衍生的反应性氮物种过氧亚硝酸盐,亚硝酸,二氧化氮和硝化氮离子硝化不饱和脂肪酸。

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摘要

Reactive nitrogen species derived from nitric oxide are potent oxidants formed during inflammation that can oxidize membrane and lipoprotein lipids in vivo. Herein, it is demonstrated that several of these species react with unsaturated fatty acid to yield nitrated oxidation products. Using HPLC coupled with both UV detection and electrospray ionization mass spectrometry, products of reaction of ONOO- with linoleic acid displayed mass/charge (m/z) characteristics of LNO2 (at least three products at m/z 324, negative ion mode). Further analysis by MS/MS gave a major fragment at m/z 46. Addition of a NO2 group was confirmed using [15N]ONOO- which gave a product at m/z 325, fragmenting to form a daughter ion at m/z 47. Formation of nitrated lipids was inhibited by bicarbonate, superoxide dismutase (SOD), and Fe3+-EDTA, while the yield of oxidation products was decreased by bicarbonate and SOD, but not by Fe3+-EDTA. Reaction of linoleic acid with both nitrogen dioxide (*NO2) or nitronium tetrafluoroborate (NO2BF4) also yielded nitrated lipid products (m/z 324), with HPLC retention times and MS/MS fragmentation patterns identical to the m/z 324 species formed by reaction of ONOO- with linoleic acid. Finally, reaction of HPODE, but not linoleate, with nitrous acid (HONO) or isobutyl nitrite (BuiONO) yielded a product at m/z 340, or 341 upon reacting with [15N]HONO. MS/MS analysis gave an NO2- fragment, and 15N NMR indicated that the product contained a nitro (RNO2) functional group, suggesting that the product was nitroepoxylinoleic acid [L(O)NO2]. This species could form via homolytic dissociation of LOONO to LO* and *NO2 and rearrangement of LO* to an epoxyallylic radical L(O)* followed by recombination of L(O)* with *NO2. Since unsaturated lipids of membranes and lipoproteins are critical targets of reactive oxygen and nitrogen species, these pathways lend insight into mechanisms for the formation of novel nitrogen-containing lipid products in vivo and provide synthetic strategies for further structural and functional studies.
机译:源自一氧化氮​​的反应性氮物质是在炎症过程中形成的强氧化剂,可在体内氧化膜和脂蛋白脂质。在此,证明了这些物质中的几种与不饱和脂肪酸反应而生成硝化的氧化产物。使用HPLC结合紫外检测和电喷雾电离质谱,ONOO-与亚油酸的反应产物显示出LNO2的质量/电荷(m / z)特性(在m / z 324处,至少有三种产物为负离子模式)。通过MS / MS进行的进一步分析给出了一个在m / z 46处的主要片段。使用[15N] ONOO-确认了NO2基团的加入,其在m / z 325处产生了一个产物,在m / z 47处发生了断裂,形成了子离子。碳酸氢盐,超氧化物歧化酶(SOD)和Fe3 + -EDTA抑制了硝化脂质的形成,而碳酸氢盐和SOD降低了氧化产物的产率,但Fe3 + -EDTA却没有。亚油酸与二氧化氮(* NO2)或四氟硼酸硝基鎓(NO2BF4)的反应也产生了硝化的脂质产物(m / z 324),HPLC保留时间和MS / MS碎片图谱与由与亚油酸反应。最后,HPODE与亚硝酸(HONO)或亚硝酸异丁酯(BuiONO)反应,但不与亚油酸酯反应,与[15N] HONO反应后,生成的产品的m / z值为340或341。 MS / MS分析给出了NO2-片段,并且15N NMR表明该产物含有硝基(RNO2)官能团,表明该产物为硝基环氧亚油酸[L(O)NO2]。这种物质可以通过将LOONO均质分解为LO *和* NO2,然后将LO *重排为环氧自由基L(O)*,然后将L(O)*与* NO2重组而形成。由于膜和脂蛋白的不饱和脂质是活性氧和氮物质的关键靶标,因此这些途径有助于深入了解体内新型含氮脂质产物形成的机制,并为进一步的结构和功能研究提供了合成策略。

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