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补充ω-3脂肪酸和抗氧化剂的混合型高脂血症男性吸烟者低密度脂蛋白的过氧化作用

Peroxidation of LDL from combined-hyperlipidemic male smokers supplied with omega-3 fatty acids and antioxidants.

作者信息

Brude I R, Drevon C A, Hjermann I, Seljeflot I, Lund-Katz S, Saarem K, Sandstad B, Solvoll K, Halvorsen B, Arnesen H, Nenseter M S

机构信息

Institute for Nutrition Research, University of Oslo, Norway.

出版信息

Arterioscler Thromb Vasc Biol. 1997 Nov;17(11):2576-88. doi: 10.1161/01.atv.17.11.2576.

Abstract

The effects of marine omega-3 polyunsaturated fatty acids (FAs) and antioxidants on the oxidative modification of LDL were studied in a randomized, double-blind, placebo-controlled trial. Male smokers (n = 41) with combined hyperlipidemia were allocated to one of four groups receiving supplementation with omega-3 FAs (5 g eicosapentaenoic acid and docosahexaenoic acid per day), antioxidants (75 mg vitamin E, 150 mg vitamin C, 15 mg beta-carotene, and 30 mg coenzyme Q10 per day), both omega-3 FAs and antioxidants, or control oils. LDL and human mononuclear cells were isolated from the patients at baseline and after 6 weeks of supplementation. LDL was subjected to cell-mediated oxidation by the patients' own mononuclear cells, as well as to Cu(2+)-catalyzed and 2,2'-azobis-(2-amidinopropane hydrochloride) (AAPH)-initiated oxidation. Extent of LDL modification was measured as lag time, the formation rate of conjugated dienes (CDs), the maximum amount of CDs formed, formation of lipid peroxides, and the relative electrophoretic mobility of LDL on agarose gels. Dietary supplementation with omega-3 FAs increased the concentration of total omega-3 FAs in LDL and reduced the concentration of vitamin E in serum. The omega-3 FA-enriched LDL particles were not more susceptible to Cu(2+)-catalyzed, AAPH-initiated, or autologous cell-mediated oxidation than control LDL. In fact, enrichment with omega-3 FAs significantly reduced the formation rate of CDs when LDL was subjected to AAPH-induced oxidation. Supplementation with moderate amounts of antioxidants significantly increased the concentration of vitamin E in serum and increased the resistance of LDL to undergo Cu(2+)-catalyzed oxidation, measured as increased lag time, reduced formation of lipid peroxides, and reduced relative electrophoretic mobility compared with control LDL. Supplementation with omega-3 FAs/antioxidants showed oxidizability of LDL similar to that of control LDL and omega-3 FA-enriched LDL. In conclusion, omega-3 FAs neither rendered the LDL particles more susceptible to undergo in vitro oxidation nor influenced mononuclear cells' ability to oxidize autologous LDL, whereas moderate amounts of antioxidants protected LDL against oxidative modification.

摘要

在一项随机、双盲、安慰剂对照试验中,研究了海洋ω-3多不饱和脂肪酸(FAs)和抗氧化剂对低密度脂蛋白(LDL)氧化修饰的影响。将合并高脂血症的男性吸烟者(n = 41)分为四组,分别接受ω-3 FAs补充剂(每天5克二十碳五烯酸和二十二碳六烯酸)、抗氧化剂(每天75毫克维生素E、150毫克维生素C、15毫克β-胡萝卜素和30毫克辅酶Q10)、ω-3 FAs和抗氧化剂联合补充剂或对照油。在基线时以及补充6周后从患者中分离出LDL和人单核细胞。LDL分别通过患者自身的单核细胞进行细胞介导的氧化,以及进行铜(2+)催化和2,2'-偶氮二(2-脒基丙烷盐酸盐)(AAPH)引发的氧化。LDL修饰程度通过延迟时间、共轭二烯(CDs)形成速率、形成的CDs最大量、脂质过氧化物的形成以及LDL在琼脂糖凝胶上的相对电泳迁移率来衡量。膳食补充ω-3 FAs可增加LDL中总ω-3 FAs的浓度,并降低血清中维生素E的浓度。富含ω-3 FA的LDL颗粒与对照LDL相比,对铜(2+)催化、AAPH引发或自体细胞介导的氧化并不更敏感。事实上,当LDL进行AAPH诱导的氧化时,富含ω-3 FAs可显著降低CDs的形成速率。补充适量的抗氧化剂可显著增加血清中维生素E的浓度,并增加LDL对铜(2+)催化氧化的抗性,与对照LDL相比,表现为延迟时间增加、脂质过氧化物形成减少以及相对电泳迁移率降低。补充ω-3 FAs/抗氧化剂显示LDL的氧化能力与对照LDL和富含ω-3 FA的LDL相似。总之,ω-3 FAs既不会使LDL颗粒更易发生体外氧化,也不会影响单核细胞氧化自体LDL的能力,而适量的抗氧化剂可保护LDL免受氧化修饰。

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