Reilly M, Delanty N, Lawson J A, FitzGerald G A
Center for Experimental Therapeutics, University of Pennsylvania, Philadelphia 19104, USA.
Circulation. 1996 Jul 1;94(1):19-25. doi: 10.1161/01.cir.94.1.19.
Free radical-induced oxidative damage is thought to be involved in the pathogenesis of diseases associated with cigarette smoking. We examined the production of 8-epi-prostaglandin (PG) F2 alpha, a stable product of lipid peroxidation in vivo, and its modulation by aspirin and antioxidant vitamins in chronic cigarette smokers.
We performed the following studies: (1) a cross-sectional comparison of smokers and control subjects, (2) an examination of the dose-response relationship, (3) an exploration of the effect of smoking cessation (3 weeks) and nicotine patch supplementation, (4) the effect of aspirin consumption, and (5) the effects of 5 days' dosing with vitamin E (100 and 800 U), vitamin C (2 g), and their combination. 8-epi-PGF2 alpha excretion (in pmol/mmol, mean +/- SEM) was 176.5+/-30.6 in heavy smokers, 92.7+/-4.8 (P<.05) in moderate smokers, and 54.1+/-2.7 (P<.005) in nonsmokers. Urinary levels fell from 145.5+/-24.9 to 114.6+/-27.1 (week 2, P<.05) and 112.6+/-24.9 (week 3, P<.05) on cessation of smoking. Aspirin treatment failed to suppress urinary levels of 8-epi-PGF2 alpha despite a significant reduction in urinary 11-dehydro-TxB2 production and suppression of 8-epi-PGF2 alpha and TxB2 in serum. Vitamin C (pre, 194.6+/-40.9; post, 137.2+/-34.1; P<.05) and a combination of vitamin C and E (pre, 171.0+/-39.8; post, 133.5+/-29.6 P<.05) suppressed urinary 8-epi-PGF2 alpha, whereas vitamin E alone had no effect.
Urinary 8-epi-PGF2 alpha may represent a noninvasive, quantitative index of oxidant stress in vivo. Elevated levels of 8-epi-PGF2 alpha in smokers may be modulated by quitting cigarettes and switching to nicotine patches or by antioxidant vitamin therapy.
自由基诱导的氧化损伤被认为与吸烟相关疾病的发病机制有关。我们检测了体内脂质过氧化的稳定产物8-表-前列腺素(PG)F2α的生成情况,以及阿司匹林和抗氧化维生素对慢性吸烟者中该产物的调节作用。
我们进行了以下研究:(1)吸烟者与对照受试者的横断面比较;(2)剂量反应关系研究;(3)戒烟(3周)及补充尼古丁贴片的效果探究;(4)阿司匹林摄入的影响;(5)维生素E(100和800单位)、维生素C(2克)及其联合用药5天的效果。重度吸烟者8-表-PGF2α排泄量(以皮摩尔/毫摩尔计,均值±标准误)为176.5±30.6,中度吸烟者为92.7±4.8(P<0.05),非吸烟者为54.1±2.7(P<0.005)。戒烟后尿中水平从145.5±24.9降至114.6±27.1(第2周,P<0.05)和112.6±24.9(第3周,P<0.05)。阿司匹林治疗虽使尿中11-脱氢-TxB2生成显著减少且血清中8-表-PGF2α和TxB2受到抑制,但未能抑制尿中8-表-PGF2α水平。维生素C(用药前194.6±40.9;用药后137.2±34.1;P<0.05)以及维生素C与E联合用药(用药前171.0±39.8;用药后133.5±29.6,P<0.05)可抑制尿中8-表-PGF2α,而单独使用维生素E则无此作用。
尿中8-表-PGF2α可能代表体内氧化应激的一种非侵入性定量指标。吸烟者中升高的8-表-PGF2α水平可通过戒烟并改用尼古丁贴片或抗氧化维生素治疗来调节。
