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首页> 外文期刊>Food and Chemical Toxicology: An International Journal Published for the British Industrial Biological Research >Evaluation of subchronic toxicity of dietary administered Cry1Ab protein from Bacillus thuringiensis var. Kurustaki HD-1 in F344 male rats with chemically induced gastrointestinal impairment.
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Evaluation of subchronic toxicity of dietary administered Cry1Ab protein from Bacillus thuringiensis var. Kurustaki HD-1 in F344 male rats with chemically induced gastrointestinal impairment.

机译:苏云金芽孢杆菌变种饮食中Cry1Ab饮食的亚慢性毒性评估化学性胃肠道损伤的F344雄性大鼠的Kurustaki HD-1。

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Bacillus thuringiensis (Bt) proteins are developed for genetically modified crops and the Bt proteins demonstrate no evidence of toxicity by the oral route in traditional animal models. However, the possible toxicity of Bt proteins under conditions of reduced gastric acid secretion and/or small intestinal damage has not been investigated. In the present study, we therefore evaluated following four F344 rat groups with a purified Bt protein Cry1Ab from B. thuringiensis var. Kurustaki HD-1. Gastrointestinal impairment (GI) alone and GI+Bt protein fed (GI+Bt) groups were given i.p. injections of famotidine to reduce gastric acid secretion twice a day at 30mg/kg body weight in weeks 2 and 4. GI and GI+Bt groups were additionally fed diets containing 80ppm indomethacin for induction of intestinal damage during weeks 1 and 3. Bt alone and GI+Bt groups were also fed diet containing Bt protein Cry1Ab at a concentration of 10ppm in weeks 2 and 4. A no treatment control group was also included. At the end of week 4, all animals were euthanized under ether anesthesia, blood samples were collected for hematology and serum biochemistry and a complete necropsy was performed. No significant changes indicative of toxicity of the Bt protein Cry1Ab used here were noted with any of the parameters investigated. In conclusion, no significant toxicological effects were detected in this subchronic gastrointestinal impairment rat model.
机译:苏云金芽孢杆菌(Btillus thuringiensis,Bt)蛋白是为转基因作物开发的,在传统动物模型中,Bt蛋白没有通过口服途径表现出毒性的证据。然而,尚未研究在降低的胃酸分泌和/或小肠损害的条件下Bt蛋白的可能毒性。因此,在本研究中,我们用来自苏云金芽孢杆菌var的纯化Bt蛋白Cry1Ab评估了四个F344大鼠组。 Kurustaki HD-1。腹膜内给予单独的胃肠道损伤(GI)和GI + Bt蛋白喂养(GI + Bt)组。在第2周和第4周,每天两次注射法莫替丁以减少30mg / kg体重的胃酸分泌,分别在第1和第3周向GI和GI + Bt组喂食含80ppm消炎痛的饮食,以诱导肠道损伤。在第2周和第4周,还给GI + Bt组喂食含Bt蛋白Cry1Ab的浓度为10ppm的饮食。也未包括对照组。在第4周结束时,将所有动物在乙醚麻醉下安乐死,收集血液样本进行血液学和血清生化检查,并进行完整的尸检。对于所研究的任何参数,未发现指示此处使用的Bt蛋白Cry1Ab毒性的显着变化。总之,在该亚慢性胃肠功能不全大鼠模型中未检测到明显的毒理作用。

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