首页> 外文期刊>Food and Chemical Toxicology: An International Journal Published for the British Industrial Biological Research >No enhancing effects of diacylglycerol oil on tumor development in a medium-term multi-organ carcinogenesis bioassay using male F344 rats.
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No enhancing effects of diacylglycerol oil on tumor development in a medium-term multi-organ carcinogenesis bioassay using male F344 rats.

机译:在使用雄性F344大鼠的中期多器官致癌生物测定中,二酰基甘油油对肿瘤发展没有增强作用。

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The modifying potential of diacylglycerol (DAG) oil on tumor development was investigated in a medium-term multi-organ carcinogenesis bioassay. DAG oil is a cooking oil that contains >80% diglycerides, <20% triglycerides and <5% monoglycerides. Male 6-week-old F344 rats (20 in each group) were sequentially treated with five carcinogens for initiation in different organ target sites for 4 weeks (DMBDD treatment), and then administered DAG oil at dietary levels of 0% (control), 1.375%, 2.75% or 5.5% [triacylglycerol (TGs), with the same fatty acid composition as DAG oil were also added at dietary levels of 5.5%, 4.125%, 2.75% and 0%, respectively, to maintain the same lipid level], or 5.5% high linoleic acid TG (HLTG), 5.5% high oleic acid TG (HOTG), or 5.5% medium-chain TG (MCTG) (as reference substances, mostly consisting of triacylglycerols) admixed into AIN-93G semi-synthetic diet, for an additional 24 weeks. Controls received standard diet without any supplementation as non-treated control. All animals were killed at the end of week 28, and the major organs were carefully examined for preneoplastic and neoplastic lesions. No DAG oil treatment-related changes were noted in survival, general conditions, body weights, food consumption and organ weights. Upon quantitative analysis of glutathione S-transferase placental form (GST-P) positive foci of the liver, DAG oil was not found to exert any effects. The incidence of colon adenomas was significantly increased in rats given 1.375% DAG oil, but not 2.75% and 5.5% DAG oil, when compared to the control (5.5% TG group) value. Furthermore, incidences and multiplicity of hyperplasias and adenomas and/or adenocarcinomas were comparable across all DAG oil-treated groups. In contrast, incidences of colon adenomas and/or adenocarcinomas were significantly increased in rats given 5.5% HOTG, and adenomas with MCTG, but not 5.5% HLTG, as compared to the 5.5% TG value. Preneoplastic and neoplastic lesions induced by DMBDD treatment in various organs other than the large intestine were comparable in all cases. Thus, the current results indicate that DAG oil may not exert modifying potential on tumor development, even in the colon because of the lack of dose-dependence. DAG oil was equivalent to HOTG (standard cocking oil composed of naturally occurring fatty acids), with regard to colon tumor development. Further dose-response study concerning HOTG may be needed to confirm whether the enhancing effect of large intestine carcinogenesis exert or not.
机译:在中期多器官致癌生物测定中研究了二酰基甘油(DAG)油对肿瘤发展的修饰潜力。 DAG油是一种食用油,其中包含> 80%的甘油二酸酯,<20%的甘油三酸酯和<5%的甘油单酸酯。雄性6周大的F344大鼠(每组20只)依次接受五种致癌剂治疗,以在不同的器官靶位点引发4周(DMBDD治疗),然后以0%的饮食水平(对照)给予DAG油,还分别添加了饮食含量分别为5.5%,4.125%,2.75%和0%的1.375%,2.75%或5.5%[脂肪酸与DAG油相同的三酰甘油(TGs),以保持相同的脂质水平]或5.5%高亚油酸TG(HLTG),5.5%高油酸TG(HOTG)或5.5%中链TG(MCTG)(作为参考物质,主要由三酰基甘油组成)混入AIN-93G半合成饮食,另外需要24周。对照组接受标准饮食,不加任何补充作为未治疗的对照组。在第28周结束时杀死所有动物,并仔细检查主要器官的肿瘤前和肿瘤性病变。在存活率,一般状况,体重,食物消耗和器官重量方面,未发现与DAG油处理有关的变化。通过对肝脏的谷胱甘肽S-转移酶胎盘形式(GST-P)阳性灶进行定量分析,未发现DAG油具有任何作用。与对照组(5.5%TG组)相比,给予1.375%DAG油的大鼠结肠腺瘤的发生率显着增加,但未给2.75%和5.5%DAG油的大鼠显着增加。此外,在所有DAG油治疗组中,增生,腺瘤和/或腺癌的发生率和多样性均相当。相反,与5.5%TG值相比,在5.5%HOTG和MCTG而不是5.5%HLTG的大鼠中,结肠腺瘤和/或腺癌的发生率显着增加。在所有情况下,DMBDD处理在大肠以外的其他器官中诱发的肿瘤前病变和肿瘤病变具有可比性。因此,目前的结果表明,由于缺乏剂量依赖性,即使在结肠中,DAG油也可能不会对肿瘤的发展发挥修饰作用。就结肠肿瘤的发展而言,DAG油相当于HOTG(由天然脂肪酸组成的标准公鸡油)。可能需要进一步进行有关HOTG的剂量反应研究,以确认是否发挥大肠癌变的增强作用。

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