高剂量富硒植物硒对胃癌模型大鼠的安全性研究

目的:对比研究长期摄入高剂量不同富硒植物硒对大鼠重要肝指标的影响,为安全合理利用不同植物硒源提供科学依据。方法:采用N-甲基-N’-硝基-N-亚硝基胍(MNNG)诱发大鼠胃癌模型,连续灌喂四种高剂量不同富硒植物硒17w,于18w末测定大鼠肝脏硒累积、丙二醛(MDA)含量和谷胱甘肽过氧化物酶(GPx)活性。结果:摄入富硒青花菜、富硒红羽、富硒绿羽的大鼠肝硒水平显著高于摄入富硒大蒜。补充植物硒显著降低了大鼠的肝MDA水平,提高了肝GPx活性。富硒大蒜高、低剂量组大鼠肝MDA含量差异显著,而GPx活性差异不显著。结论:长期摄入高剂量富硒大蒜后,动物肝组织低硒累积可作为富硒大蒜高安全性的重要依据。植物硒可通过GPx清除肝组织MDA,防止肝氧化损伤。

4种富硒植物预防MNNG诱发大鼠胃癌效果研究 二、不同源硒预防大鼠胃癌的安全性对比研究

目的对比研究长期摄入高剂量不同源硒的安全性。方法以亚硒酸钠为对照硒材料,采用N-甲基-N′-硝基-N-亚硝基胍(MNNG)诱发大鼠胃癌模型,连续灌以4种不同富硒植物(高剂量硒)17周,测定肝脏谷胱甘肽硫转移酶(GST)、血清谷草转氨酶(AST)和血清谷丙转氨酶(ALT)活性,并观察肝脏和肾脏的病理变化。结果各组大鼠肝GST活性均无显著性差异;75μg/kg bw(以Se计,下同)亚硒酸钠低剂量组大鼠血清AST和ALT活性不仅显著高于空白对照和MNNG组,而且显著高于150μg/kg bw和300μg/kg bw植物硒处理组(P<0.05)。病理分析发现75μg/kg bw亚硒酸钠低剂量组胆管周围有棕黄色颗粒,窦内枯否氏细胞轻度肥大、增生;其余各组未发现有意义的病变。结论亚硒酸钠毒性至少是实验用其它富硒植物的4倍。

4种富硒植物预防N-甲基-N’-硝基-N-亚硝基胍诱发大鼠胃癌效果研究 三、不同源硒预防实验性胃癌大鼠组织内硒累积分布研究

目的对比研究长期摄入高剂量不同富硒植物对大鼠体内硒累积分布的影响。方法采用N-甲基-N’-硝基-N-亚硝基胍(MNNG)诱发大鼠胃癌模型,连续灌以硒高剂量四种不同富硒植物17周,测定大鼠硒累积以及参与硒蛋白合成组织的含硒量。结果摄入富硒青花菜、富硒红羽、富硒绿羽的大鼠肝和肾硒水平显著高于摄入富硒大蒜的,摄入富硒大蒜的大鼠红血球和脾脏硒水平显著高于摄入富硒青花菜、富硒红羽和富硒绿羽的。结论初步认为长期摄入高剂量植物硒后,动物组织硒的累积和分布取决于摄入的硒种类;与其它源硒相比,长期摄入高剂量富硒大蒜后,动物肝组织的低硒累积可以作为富硒大蒜高安全性的重要依据之一。

Gastric cancer induced by N-methyl-N'-nitro-N-nitrosoguanidine in rat with ulcers and expressions of ras and c-erbB2 genes

Objective: To observe the series of pathological changes during the development of gastric adenocarcinoma in ulcerative rats induced by N-methyl-N′-nitro-N-nitrosoguanidine (MNNG), and the expression profile of related oncogenic protein.Methods: MNNG was administered in rats with ulcers due to acetic acid treatment to induce gastric cancer, and the protein expressions of ras and c-erbB2 genes in the ulcer were examined immunohistochemically along with pathological examination.Results: The incidence of gastric adenocarcinoma in the model group reaches 40% (6/15), while none of the rats developed cancer in the control group with ulcers.Positive expressions of the proteins of p21ras and c-erbB2 were observed in the tissues undergoing canceration in the 6 rats of model group, but were not observed in the 5 control rats; p53 protein expression, however, failed to be detected in both groups.Conclusion: A new animal model of gastric cancer has been established in rats with gastric ulcer after MNNG treatment, which may facilitate the pharmacological research of gastric cancer.