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膳食有机硒苯甲基硒氰酸盐对F344大鼠结肠癌发生的化学预防作用。

Chemoprevention of colon carcinogenesis by dietary organoselenium, benzylselenocyanate, in F344 rats.

作者信息

Reddy B S, Sugie S, Maruyama H, el-Bayoumy K, Marra P

机构信息

Division of Nutrition and Endocrinology, Naylor Dana Institute for Disease Prevention, American Health Foundation, Valhalla, New York 10595.

出版信息

Cancer Res. 1987 Nov 15;47(22):5901-4.

PMID:3664491
Abstract

The effect of feeding benzylselenocyanate (BSC) and its sulfur analogue, benzylthiocyanate (BTC), 2 wk before, during, and until 1 wk after carcinogen administration (initiation phase) on intestinal carcinogenesis induced by azoxymethane (CAS:25843-45-2) was studied in male F344 rats. Weanling rats were raised on a semipurified diet (AIN-76A diet; control diet). Beginning at 5 wk of age, groups of animals consuming the control diet were fed one of the diets containing 25 ppm BSC or BTC. An additional group was continued on the control diet. At 7 wk of age, all animals in 3 groups, except the vehicle-treated controls, were administered s.c. injections of azoxymethane (15 mg/kg body weight, once weekly for 2 wk). Animals were continued on the control diet and BSC and BTC diets until 1 wk after carcinogen treatment, when those groups receiving BSC and BTC diets were fed the control diet until termination of the experiment. Tissue and blood plasma glutathione peroxidase activity was measured in vehicle-treated animals fed the control diet and BSC and BTC diets for 5 wk. The results indicate that body weights were comparable among the various dietary groups. BSC in the diet significantly inhibited the incidence (percentage of animals with tumors) and multiplicity (tumors/animal) of adenocarcinomas in the colon and multiplicity of adenocarcinomas in the small intestine compared to those fed the control diet. BTC in the diet had no effect on colon and small intestinal tumors. Selenium-dependent glutathione peroxidase activity was significantly increased in kidneys and colon and small intestinal mucosae of animals fed the BSC diet compared to animals fed the BTC and control diets.

摘要

研究了在给雄性F344大鼠施用致癌物(启动阶段)前2周、施用期间以及施用后1周,喂食苄基硒氰酸盐(BSC)及其硫类似物苄基硫氰酸盐(BTC)对由偶氮甲烷(CAS:25843-45-2)诱导的肠道癌变的影响。断奶大鼠采用半纯化饮食(AIN-76A饮食;对照饮食)饲养。从5周龄开始,食用对照饮食的动物组被喂食含25 ppm BSC或BTC的饮食之一。另一组继续食用对照饮食。7周龄时,除溶剂处理的对照组外,3组中的所有动物均皮下注射偶氮甲烷(15 mg/kg体重,每周1次,共2周)。动物继续食用对照饮食以及BSC和BTC饮食,直到致癌物处理后1周,此时接受BSC和BTC饮食的组改喂对照饮食直至实验结束。对食用对照饮食以及BSC和BTC饮食5周的溶剂处理动物的组织和血浆谷胱甘肽过氧化物酶活性进行了测量。结果表明,各饮食组之间体重相当。与喂食对照饮食的动物相比,饮食中的BSC显著抑制了结肠腺癌的发生率(有肿瘤动物的百分比)和多发性(肿瘤数/动物)以及小肠腺癌的多发性。饮食中的BTC对结肠和小肠肿瘤没有影响。与喂食BTC和对照饮食的动物相比,喂食BSC饮食的动物的肾脏、结肠和小肠黏膜中硒依赖性谷胱甘肽过氧化物酶活性显著增加。

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