Reddy B S, Simi B, Patel N, Aliaga C, Rao C V
Division of Nutritional Carcinogenesis, American Health Foundation, Valhalla, New York 10595, USA.
Cancer Res. 1996 May 15;56(10):2314-20.
It is evident from many studies that the effect of dietary fat on colon tumor promotion depends not only on the amount of fat but especially on fatty acid composition. Animal model studies have shown that diets which are high in omega-6 fatty acids increase colon tumor promotion, whereas diets rich in omega-3 fatty acids have no such enhancing effect. The mechanisms by which the high fat content of the diet promotes colon carcinogenesis may include the production of secondary bile acids in the colon and the modulation of colonic luminal bacterial 7 alpha-dehydroxylase that is involved in generating secondary bile acids, phosphatidylinositol-specific phospholipase C (PI-PLC), and mucosal PI-PLC, as well as diacylglycerol (DAG) kinase and protein kinase C (PKC). In the present study, we investigated the effect of high-fat diets that are rich in omega-3 and omega-6 fatty acids on cecal bacterial 7 alpha-dehydroxylase and PI-PLC, fecal secondary bile acids, and colonic mucosal DAG kinase and PKC activities during different stages of colon carcinogenesis in male F344 rats. At 5 weeks of age, groups of animals were fed a low-fat diet containing 5% corn oil (LFCO). Beginning at 7 weeks of age, all animals, except those intended as vehicle controls, received azoxymethane (AOM) s.c. once weekly for 2 weeks at a dose rate of 15 mg/kg body weight. Vehicle-treated groups received s.c. injections of normal saline. One day after the second AOM or saline treatment, the experimental groups of animals were transferred to a high-fat diet containing 23.5% corn oil (HFCO) or 20.5% fish oil + 3% corn oil (HFFO). One group continued on the LFCO diet. Animals were sacrificed at weeks 1, 12, and 36 after the AOM or saline treatment. Colonic mucosa were harvested at weeks 1, 12, or 36, and the colonic tumor tissues were examined for PKC and DAG kinase activities. Contents of the cecum were analyzed for bacterial 7 alpha-dehydroxylase and PI-PLC activities. Stool samples collected at week 12 were analyzed for bile acids. High corn oil content of the diet significantly increased the cecal bacterial 7 alpha-dehydroxylase and PI-PLC activities as compared to the diets with high fish oil or low corn oil content. Animals fed the HFCO diet excreted higher levels of secondary bile acids, such as deoxycholic acid and lithocholic acid, than those fed the LFCO or HFFO diets. Carcinogen treatment significantly enhanced the activities of DAG kinase and total membrane PKC activities in colonic mucosa compared to saline treatment in all dietary groups. Animals treated with saline or AOM and fed HFCO showed increased levels of DAG kinase and membrane PKC activities in the colonic mucosa when compared to LFCO and HFFO groups. DAG kinase and membrane PKC activities were higher in colon tumors than in the surrounding colonic mucosa, and also increased levels of these enzyme activities were found in the HFCO diet group. These results indicate that the modifying effect of dietary fat on colonic bacterial enzymes, secondary bile acids, colonic mucosal and tumor DAG kinase, and PKC that may play a role in colon carcinogenesis depends on the types and amount of fat given. The colon tumor-enhancing effect of a HFCO diet in contrast to the high dietary fish oil may be, in part, explained on the basis of its modulating effect on these bacterial and colonic mucosal enzymes and colonic secondary bile acids relevant to colon tumor promotion.
许多研究表明,膳食脂肪对结肠肿瘤促进作用的影响不仅取决于脂肪的量,尤其还取决于脂肪酸的组成。动物模型研究显示,富含ω-6脂肪酸的饮食会增加结肠肿瘤的促进作用,而富含ω-3脂肪酸的饮食则没有这种增强作用。饮食中高脂肪含量促进结肠癌变的机制可能包括结肠中次级胆汁酸的产生以及对参与生成次级胆汁酸的结肠腔细菌7α-脱羟基酶、磷脂酰肌醇特异性磷脂酶C(PI-PLC)、黏膜PI-PLC以及二酰基甘油(DAG)激酶和蛋白激酶C(PKC)的调节。在本研究中,我们调查了富含ω-3和ω-6脂肪酸的高脂肪饮食对雄性F344大鼠结肠癌变不同阶段盲肠细菌7α-脱羟基酶和PI-PLC、粪便次级胆汁酸以及结肠黏膜DAG激酶和PKC活性的影响。5周龄时,将动物分组喂食含5%玉米油的低脂饮食(LFCO)。从7周龄开始,除作为溶剂对照的动物外,所有动物每周皮下注射一次15mg/kg体重的偶氮甲烷(AOM),共注射2周。溶剂处理组皮下注射生理盐水。在第二次AOM或生理盐水处理后的一天,将实验组动物转移至含23.5%玉米油的高脂肪饮食(HFCO)或含20.5%鱼油+3%玉米油的高脂肪饮食(HFFO)中。一组继续喂食LFCO饮食。在AOM或生理盐水处理后的第1、12和36周处死动物。在第1、12或36周采集结肠黏膜,并检测结肠肿瘤组织中的PKC和DAG激酶活性。分析盲肠内容物中的细菌7α-脱羟基酶和PI-PLC活性。分析第12周收集的粪便样本中的胆汁酸。与高鱼油或低玉米油含量的饮食相比,饮食中高玉米油含量显著增加了盲肠细菌7α-脱羟基酶和PI-PLC活性。喂食HFCO饮食的动物排出的次级胆汁酸水平高于喂食LFCO或HFFO饮食的动物,如脱氧胆酸和石胆酸。与所有饮食组中的生理盐水处理相比,致癌物处理显著增强了结肠黏膜中DAG激酶和总膜PKC活性。与LFCO和HFFO组相比,用生理盐水或AOM处理并喂食HFCO的动物结肠黏膜中DAG激酶和膜PKC活性增加。结肠肿瘤中的DAG激酶和膜PKC活性高于周围结肠黏膜,并且在HFCO饮食组中也发现这些酶活性水平增加。这些结果表明,膳食脂肪对可能在结肠癌变中起作用的结肠细菌酶、次级胆汁酸、结肠黏膜和肿瘤DAG激酶以及PKC的调节作用取决于所给予脂肪的类型和量。与高膳食鱼油相比,HFCO饮食对结肠肿瘤的增强作用部分可能基于其对这些与结肠肿瘤促进相关的细菌和结肠黏膜酶以及结肠次级胆汁酸的调节作用来解释。
