首页> 外文会议>221st National American Chemical Society (ACS) Meeting; Apr, 2001; San Diego, California >In Vivo Inhibition of Mammary Carcinogenesis, Formation of DNA-Carcinogen Adducts, and Mammary Proliferation by Dietary Dibenzoylmethane
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In Vivo Inhibition of Mammary Carcinogenesis, Formation of DNA-Carcinogen Adducts, and Mammary Proliferation by Dietary Dibenzoylmethane

机译:饮食中二苯甲酰甲烷的体内乳腺癌变抑制,DNA致癌物加合物的形成和乳腺增生

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Dibenzoylmethane (DBM) is a minor constituent in licorice and has anti-inflammatory activity. Feeding 1% DBM in the diet to Sencar mice during both the initiation and post-initiation stages strongly inhibited 7,12-dimethylbenz[a]-anthracene (DMBA)-induced mammary tumorigenesis in both tumor incidence and tumor multiplicity. Feeding 1% DBM in the diet to immature mice for 4-5 weeks decreased uterine wet weight, inhibited proliferation of uterus and mammary gland, and lowered serum estradiol levels. In addition, feeding 1% DBM in the diet to mice increased liver weight and levels of hepatic cytochrome P-450 as well as increased hepatic hydroxylation and glucuronidation of estradiol. In further studies, feeding 1% DBM in the diet to mice at 2 weeks before, during and for a week after DMBA treatment (intubation of 1 mg DMBA in corn oil per mouse once a week for 2 or 5 weeks) markedly inhibited formation of mammary gland DMBA-DNA adducts by a [~(32)P]post-labeling assay. Adding various doses of DBM to an incubation of DMBA with mouse liver microsomes in vitro inhibited DMBA metabolism and formation of DMBA-DNA adducts in a dose-dependent manner. In an assay of competitive binding to estrogen receptors with [~3H]estradiol in vitro, DBM showed only weak binding affinity.
机译:二苯甲酰甲烷(DBM)是甘草中的次要成分,具有抗炎活性。在初始阶段和初始阶段后,在饮食中向Sencar小鼠饲喂1%DBM会强烈抑制7,12-二甲基苯并[a]-蒽(DMBA)诱导的乳腺肿瘤发生,无论其发病率还是肿瘤多样性。在未成年小鼠中喂食1%DBM,持续4-5周可降低子宫湿重,抑制子宫和乳腺的增殖,并降低血清雌二醇水平。此外,在饮食中向小鼠饲喂1%DBM会增加肝脏的重量和肝细胞色素P-450的水平,并增加肝羟基化和雌二醇的葡萄糖醛酸化。在进一步的研究中,在DMBA治疗之前,治疗期间和治疗之后的2周(小鼠每星期一次向小鼠注入1 mg DMBA玉米油,持续2或5周)中向小鼠饲喂1%DBM的饮食可显着抑制DMBA的形成。 [〜(32)P]标记后分析检测乳腺DMBA-DNA加合物。在体外用小鼠肝微粒体孵育DMBA时,添加各种剂量的DBM以剂量依赖的方式抑制DMBA代谢和DMBA-DNA加合物的形成。在体外用[〜3H]雌二醇竞争性结合雌激素受体的试验中,DBM仅显示弱结合亲和力。

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