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用苯并[a]芘处理的大鼠血液中的脂质过氧化、抗氧化酶和苯并[a]芘醌

Lipid peroxidation, antioxidant enzymes, and benzo[a]pyrene-quinones in the blood of rats treated with benzo[a]pyrene.

作者信息

Kim H S, Kwack S J, Lee B M

机构信息

Division of Toxicology, College of Pharmacy, Sungkyunkwan University, Chunchum-Dong 300, 440-476, Kyunggi-Do, Suwon, South Korea.

出版信息

Chem Biol Interact. 2000 Jul 3;127(2):139-50. doi: 10.1016/s0009-2797(00)00177-0.

Abstract

The lipid peroxidation (as malondialdehyde, MDA), activities of superoxide dismutase (SOD) and catalase (CAT), and benzo[a]pyrene (BaP) metabolites were investigated in sera and erythrocytes of male Sprague-Dawley rats treated with BaP (20 mg per rat). MDA levels were significantly increased in sera (16.98+/-3.29 nmol/ml serum, P<0.05) 12 h after BaP treatment and persisted up to 96 h (13.80+/-1. 65 nmol/ml serum, P<0.05), but no significant change in NIDA levels was observed in erythrocytes. SOD and CAT activities were significantly increased in erythrocytes shortly after BaP exposure, and they were slightly decreased in sera, indicating an inverse correlation between lipid peroxidation and antioxidant enzyme activity. BaP and BaP-quinones (BaP-1,6-quinone and BaP-3,6-quinone) were measured in sera during the study period. A rapid increase of unmetabolized BaP was observed in sera (41.27+/-4.14 pmol/ml serum) 3 h after BaP treatment, reaching a peak at 6 h (48.56+/-4.62 pmol/ml serum) followed by a sharp decrease. Formation of the BaP-1, 6-quinone and BaP-3,6-quinone started in sera 3 h after BaP treatment, reached a peak at 24 h (7.23+/-1.02 pmol/ml serum) and 12 h (9.20+/-0.98 pmol/ml serum), respectively, and then decreased gradually. The time-dependent pattern of serum lipid peroxidation and the level of erythrocyte antioxidant enzymes were shown to be related to the concentrations of the BaP-quinone metabolites. These results suggest that BaP treatment, probably via the formation of BaP-quinones, oxidatively altered lipids and antioxidant enzymes in the blood, and might be associated with BaP-related vascular toxicity including carcinogenesis.

摘要

对用苯并[a]芘(每只大鼠20毫克)处理的雄性斯普拉格-道利大鼠的血清和红细胞中的脂质过氧化(以丙二醛,即MDA表示)、超氧化物歧化酶(SOD)和过氧化氢酶(CAT)的活性以及苯并[a]芘(BaP)代谢产物进行了研究。苯并[a]芘处理12小时后,血清中的MDA水平显著升高(16.98±3.29纳摩尔/毫升血清,P<0.05),并持续至96小时(13.80±1.65纳摩尔/毫升血清,P<0.05),但红细胞中的MDA水平未观察到显著变化。苯并[a]芘暴露后不久,红细胞中的SOD和CAT活性显著增加,而血清中的这些酶活性略有下降,表明脂质过氧化与抗氧化酶活性呈负相关。在研究期间测定了血清中的BaP和BaP-醌(BaP-1,6-醌和BaP-3,6-醌)。苯并[a]芘处理3小时后,血清中未代谢的BaP迅速增加(41.27±4.14皮摩尔/毫升血清),在6小时达到峰值(48.56±4.62皮摩尔/毫升血清),随后急剧下降。BaP-1,6-醌和BaP-3,6-醌的形成在苯并[a]芘处理3小时后开始于血清中,分别在24小时(7.23±1.02皮摩尔/毫升血清)和12小时(9.20±0.98皮摩尔/毫升血清)达到峰值,然后逐渐下降。血清脂质过氧化的时间依赖性模式和红细胞抗氧化酶水平显示与BaP-醌代谢产物的浓度有关。这些结果表明,苯并[a]芘处理可能通过BaP-醌的形成,氧化改变了血液中的脂质和抗氧化酶,并且可能与包括致癌作用在内的与BaP相关的血管毒性有关。

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