Kadiiska Maria B, Basu Samar, Brot Nathan, Cooper Christopher, Saari Csallany A, Davies Michael J, George Magdalene M, Murray Dennis M, Jackson Roberts L, Shigenaga Mark K, Sohal Rajindar S, Stocker Roland, Van Thiel David H, Wiswedel Ingrid, Hatch Gary E, Mason Ronald P
National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC, USA.
Faculty of Medicine, Uppsala University, Uppsala, Sweden; Biochemistry, Molecular Biology and Nutrition Department, University of Auvergne, Clermont-Ferrand, France.
Free Radic Biol Med. 2013 Aug;61:408-15. doi: 10.1016/j.freeradbiomed.2013.04.023. Epub 2013 Apr 19.
Ozone exposure effect on free radical-catalyzed oxidation products of lipids, proteins, and DNA in the plasma and urine of rats was studied as a continuation of the international Biomarker of Oxidative Stress Study (BOSS) sponsored by NIEHS/NIH. The goal was to identify a biomarker for ozone-induced oxidative stress and to assess whether inconsistent results often reported in the literature might be due to the limitations of the available methods for measuring the various types of oxidative products. The time- and dose-dependent effects of ozone exposure on rat plasma lipid hydroperoxides, malondialdehyde, F2-isoprostanes, protein carbonyls, methionine oxidation, and tyrosine- and phenylalanine oxidation products, as well as urinary malondialdehyde and F2-isoprostanes were investigated with various techniques. The criterion used to recognize a marker in the model of ozone exposure was that a significant effect could be identified and measured in a biological fluid seen at both doses at more than one time point. No statistically significant differences between the experimental and the control groups at either ozone dose and time point studied could be identified in this study. Tissue samples were not included. Despite all the work accomplished in the BOSS study of ozone, no available product of oxidation in biological fluid has yet met the required criteria of being a biomarker. The current negative findings as a consequence of ozone exposure are of great importance, because they document that in complex systems, as the present in vivo experiment, the assays used may not provide meaningful data of ozone oxidation, especially in human studies.
作为美国国立环境卫生科学研究所/美国国立卫生研究院赞助的国际氧化应激生物标志物研究(BOSS)的延续,研究了臭氧暴露对大鼠血浆和尿液中脂质、蛋白质和DNA的自由基催化氧化产物的影响。目标是确定一种臭氧诱导氧化应激的生物标志物,并评估文献中经常报道的不一致结果是否可能是由于测量各种氧化产物的现有方法的局限性。采用各种技术研究了臭氧暴露对大鼠血浆脂质氢过氧化物、丙二醛、F2-异前列腺素、蛋白质羰基、蛋氨酸氧化以及酪氨酸和苯丙氨酸氧化产物,以及尿丙二醛和F2-异前列腺素的时间和剂量依赖性影响。在臭氧暴露模型中用于识别标志物的标准是,在不止一个时间点的两种剂量下,在生物流体中都能识别并测量到显著影响。在本研究中,在所研究的臭氧剂量和时间点,实验组和对照组之间均未发现统计学上的显著差异。未纳入组织样本。尽管在BOSS臭氧研究中完成了所有工作,但生物流体中尚无可用的氧化产物符合作为生物标志物的要求标准。当前臭氧暴露的阴性结果非常重要,因为它们证明在复杂系统中,如当前的体内实验,所使用的检测方法可能无法提供臭氧氧化的有意义数据,尤其是在人体研究中。