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伞菌氨酸在lacI转基因小鼠突变试验中的遗传毒性:食用蘑菇的健康风险评估。

Genotoxicity of agaritine in the lacI transgenic mouse mutation assay: evaluation of the health risk of mushroom consumption.

作者信息

Shephard S E, Gunz D, Schlatter C

机构信息

Swiss Federal Institute of Technology, Schwerzenbach.

出版信息

Food Chem Toxicol. 1995 Apr;33(4):257-64. doi: 10.1016/0278-6915(94)00142-b.

Abstract

The mutagenic potency of the common mushroom Agaricus bisporus and crude agaritine extracted from mushrooms was determined in vivo using a new mutagenesis assay with lacI transgenic mice (Big Blue mice). Pairs of female lacI mice were fed one of three diets for 15 wk: (1) fresh mushrooms 3 days/wk followed by normal lab chow for 4 days/wk; (2) freeze-dried mushrooms mixed at 25% (w/w) into powdered chow; or (3) a mushroom extract containing 30% agaritine (w/w) mixed into powdered chow. The corresponding daily doses of agaritine were 30 (averaged over the whole week), 80 and 120 mg/kg body weight, respectively. Positive control animals received N-nitrosodimethylamine, N-nitrosomethylurea or urethane, mixed into powdered chow at concentrations corresponding to daily doses of 0.3, 3 and 130 mg/kg body weight, respectively. DNA of the forestomach, kidney, liver, lung and glandular stomach of the lacI mice was examined for increases in mutant frequency (MF). Control MFs ranged from 5 x 10(-5) to 10 x 10(-5). Positive control substances induced a two- to seven-fold increase in MF in their respective target organs. Of the mushroom diets, significant effects were seen only with the crude agaritine extract: it induced an increase in MF of 100% in the kidney and 50% in the forestomach. The other two A. bisporus diets, with lower agaritine doses, showed slightly but not significantly, raised MF values in the kidney alone. Thus, agaritine was weakly genotoxic in vivo; no genotoxic activity other than that attributable to agaritine was detected in A. bisporus. Substances or processes that might influence carcinogenicity by means of non-genotoxic mechanisms (e.g. increase in fibre, or decrease in calorie intake) are not detected in the lacI assay. Using a previously derived quantitative correlation between mutagenicity in the lacI test and carcinogenic potency, the carcinogenicity of agaritine in mushrooms was estimated: the average Swiss mushroom consumption of 4 g/day would be expected to contribute a lifetime cumulative cancer risk of about two cases per 100,000 lives.

摘要

利用一种针对lacI转基因小鼠(大蓝鼠)的新型诱变试验,在体内测定了普通蘑菇双孢蘑菇及其从蘑菇中提取的粗蘑菇氨酸的诱变效力。将成对的雌性lacI小鼠分为三组,每组喂食一种饮食,持续15周:(1)每周3天喂食新鲜蘑菇,随后4天喂食正常实验室饲料;(2)将冻干蘑菇按25%(w/w)混入粉状饲料中;或(3)将含有30%蘑菇氨酸(w/w)的蘑菇提取物混入粉状饲料中。相应的蘑菇氨酸每日剂量分别为30(整周平均)、80和120毫克/千克体重。阳性对照动物分别接受N-亚硝基二甲胺、N-亚硝基甲基脲或尿烷,按对应于每日剂量0.3、3和130毫克/千克体重的浓度混入粉状饲料中。检测lacI小鼠的前胃、肾脏、肝脏、肺和腺胃的DNA,以确定突变频率(MF)是否增加。对照MF范围为5×10⁻⁵至10×10⁻⁵。阳性对照物质在其各自的靶器官中诱导MF增加了2至7倍。在蘑菇饮食中,仅粗蘑菇氨酸提取物有显著影响:它在肾脏中诱导MF增加100%,在前胃中增加50%。另外两种双孢蘑菇饮食,蘑菇氨酸剂量较低,仅在肾脏中显示MF值略有升高,但不显著。因此,蘑菇氨酸在体内具有弱遗传毒性;在双孢蘑菇中未检测到除蘑菇氨酸以外的其他遗传毒性活性。在lacI试验中未检测到可能通过非遗传毒性机制影响致癌性的物质或过程(例如纤维增加或卡路里摄入减少)。利用先前得出的lacI试验中的诱变性与致癌效力之间的定量相关性,估计了蘑菇中蘑菇氨酸的致癌性:预计瑞士人平均每天食用4克蘑菇会导致每10万例生命中约有两例终身累积癌症风险。

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