共查询到17条相似文献,搜索用时 78 毫秒
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目的研究门冬氨酸钾的致突变作用。方法应用小鼠微核试验、哺乳动物培养细胞染色体试验 ,观察门冬氨酸钾对细胞的诱变性。结果门冬氨酸钾的小鼠体内微核试验、CHL细胞染色体畸变试验均呈阴性结果 ,门冬氨酸钾无诱变性。结论门冬氨酸钾无致突变作用 相似文献
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长春西汀的致突变研究 总被引:3,自引:0,他引:3
检测长春西汀是否有致突变作用。方法:要用Ames试验,小鼠微核试验及哺乳动物培养细胞染色体畸变试验观察长春西汀的诱导性。结果:Ames试验,微核试验及染色体畸变试验结果为阴性,结论:长春西汀在所试条件下未见致突变作用。 相似文献
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用氟芬那丁酯酸对4种鼠伤寒沙门氏菌营养缺陷型(TA)进行了回复突变试验和培养中国仓鼠肺细胞(CHL)的染色体畸变试验.结果在加代谢活化系统(S9)或不加的条件下,氟芬那酸丁酯(剂量为05~5000μg·皿-1)对4种TA菌的回复突变菌落数无明显影响;对培养CHL的50%细胞抑制浓度为40μg·mL-1,浓度为4~40μg·mL-1的氟芬那酸丁酯对CHL染色体无致畸变作用.提示本品无致突变作用. 相似文献
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目的评价9-[2-(膦酰甲氧基)乙基]腺苷-钠盐(PMEA-Na)的致突变性。方法采用组氨酸缺陷型鼠伤寒沙门氏菌回复突变试验(Am es试验)、中国仓鼠肺细胞(CHL)染色体畸变试验和小鼠骨髓微核试验,观察PMEA-Na的致突变性。结果PMEA-Na在50~5000μg.皿-1剂量范围内,加与不加S9活化系统条件下,对TA97、TA98、TA100、TA102四种菌株的回变菌落数均未超过自发对照的2倍,即Am es试验结果为阴性;染色体畸变试验中,当药物浓度为48、24、12、6 mg.L-1时,活化条件下各浓度细胞的染色体畸变率均低于5%。在非活化条件下,药物浓度为48 mg.L-1培养48 h时,染色体畸变率为10%,因此染色体畸变试验结果为阳性;小鼠静脉注射PMEA-Na剂量为1 000、500、250 mg.kg-1时,骨髓中含微核的嗜多染红细胞数明显增加,即微核试验结果为阳性。结论在本实验条件下,PMEA-Na具有潜在的致突变性。 相似文献
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目的对酸枣仁油进行毒理学试验,探讨酸枣仁油是否有致突变作用。方法①小鼠急性毒性试验:一次最大限量法。②Ames试验:选用经鉴定符合要求的鼠伤寒沙门氏组氨酸缺陷型TA97、TA98、TA100、TA102试验菌株,采用平板掺入法。③小鼠骨髓嗜多染红细胞微核试验。结果酸枣仁油对雌雄小鼠经口LD50均>10g/kg,为实际无毒级物质;骨髓嗜多染红细胞微核实验和Ames试验未发现破酸枣仁油对小鼠有致突变作用。结论从毒理学角度可以认为酸枣仁油作为保健食品用于人体是安全的。 相似文献
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目的检测爱宁的致突变性,以提供有关致突变的遗传毒性安全评价数据。方法设1.6,8,40,200和1000μg/皿5个剂量组,进行Am es试验;设0.3,1,3和9μg·mL-14个剂量组,进行仓鼠肺成纤维细胞染色体畸变试验;设15,100和250 mg·kg-13个剂量组,观察其对小鼠骨髓细胞微核的影响。结果Am es试验表明,爱宁在加和不加S9的条件下,对TA97,TA98,TA100和TA102菌株回复突变菌落结果为阴性。仓鼠肺成纤维细胞染色体畸变试验表明,爱宁对中国仓鼠肺成纤维细胞体外培养染色体无畸变作用。小鼠骨髓细胞微核试验表明,爱宁三个剂量组的微核出现率与阴性对照组比较无显著性差异。结论在本实验条件下,爱宁无致突变性。 相似文献
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目的 观察雷公藤的主要有效成分之一雷公藤内酯醇的遗传毒性。方法 采用鼠伤寒沙门氏菌回复突变试验(Ames试验)、体外培养CHO细胞染色体畸变试验和小鼠骨髓微核试验检测雷公藤内酯醇的遗传毒性。结果 Ames试验提示在每皿1.6~1000 μg受试剂量下,在加或不加S9代谢活化系统时,受试物对组氨酸缺陷型鼠伤寒沙门氏菌TA97、TA98、TA100、TA102及TA1535所诱发的回复突变菌落数均与溶媒对照的突变菌落数相近。体外培养CHO细胞染色体畸变试验结果显示0.01、0.02和0.04 μg/ml 3个剂量的受试物,对加与不加S9代谢活化系统培养的CHO细胞的染色体畸变率无明显影响。小鼠骨髓微核试验设180、360、720 μg/kg 3个剂量,在720 μg/kg剂量时,雷公藤内酯醇有诱发骨髓嗜多染红细胞微核率增高的效应。结论 在本实验条件下,雷公藤内酯醇对鼠伤寒沙门氏菌无致突变性,对哺乳动物培养细胞染色体无致畸变作用,720 μg/kg剂量下对ICR小鼠有诱发骨髓嗜多染红细胞微核率增高的效应。提示雷公藤内酯醇对人体可能具有潜在的遗传毒性。 相似文献
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目的:根据前期藿莲香Ⅰ号药效学研究结果,进一步研究该复方的急性毒性和致突变作用,为其进一步应用的安全性提供理论依据。方法应用急性毒性实验、小鼠骨髓嗜多染红细胞微核试验、小鼠骨髓细胞染色体畸变试验和Ames试验检测该组分配伍复方的急性毒性和致突变性。结果急性经口毒性试验:雌性、雄性小鼠经口MTD均大于10g·kg-1,属实际无毒。致突变实验:小鼠骨髓嗜多染红细胞微核试验、小鼠骨髓细胞染色体畸变试验和Ames试验结果均为阴性,显示在本实验条件下,该中药复方未见有致突变性作用。结论中药复方藿莲香Ⅰ号未见有明显的急性毒性和致突变作用,表明该药物安全性良好。 相似文献
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《Drug and chemical toxicology》2013,36(2):152-159
HM10760A is a recombinant human erythropoietin chemically conjugated to the N-terminus of human immunoglobulin Fc fragment through a polyethylene glycol linker. HM10760A was shown to have a relatively long half-life, compared with unconjugated recombinant erythropoietin. In this study, the genotoxicity of HM10760A was investigated by using a test battery of three different methods. In the Ames assay, five strains (TA100, TA1535, TA98, TA1537, and Escherichia coli WP2 uvrA) were tested at six concentrations of 3.13, 6.25, 12.5, 25, 50, and 100?μg/plate. HM10760A did not increase the number of revertant colonies in any tester strains with and without metabolic activation by rat-liver S9 mix. Subsequently, in vitro chromosomal aberration test, using Chinese hamster lung cells, were conducted at the concentrations of 25, 50, and 100?μg/mL. HM10760A did not induce chromosomal aberrations either in the short-period (6 hours) test with or without rat-liver S9 mix or in the continuous-treatment (24 hours) test. In the in vivo bone marrow micronucleus assay using the male ICR (imprinting control region) mouse, HM10760A was subcutaneously administered twice at 24-hour intervals at doses of 0, 150, 300, and 600?μg/kg. HM10760A produced a slight, but statistically significant, increase in the frequency of micronucleated polychromatic erythrocytes at 600?μg/kg. However, no biological significance was assumed, because this value was within the historical control range. From these findings obtained from the genotoxicity assays performed in this study, it appears unlikely that HM10760A acts as a genotoxic agent in vitro and in vivo. 相似文献
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Jacky Bhagat 《Journal of applied toxicology : JAT》2018,38(1):81-99
Many of the known human carcinogens are potent genotoxins that are efficiently detected as carcinogens in human populations but certain types of compounds such as immunosuppressants, sex hormones, etc. act via non‐genotoxic mechanism. The absence of genotoxicity and the diversity of modes of action of non‐genotoxic carcinogens make predicting their carcinogenic potential extremely challenging. There is evidence that combinations of different short‐term tests provide a better and efficient prediction of human genotoxic and non‐genotoxic carcinogens. The purpose of this study is to summarize the in vivo and in vitro comet assay (CMT) results of group 1 carcinogens selected from the International Agency for Research on Cancer and to discuss the utility of the comet assay along with other genotoxic assays such as Ames, in vivo micronucleus (MN), and in vivo chromosomal aberration (CA) test. Of the 62 agents for which valid genotoxic data were available, 38 of 61 (62.3%) were Ames test positive, 42 of 60 (70%) were in vivo MN test positive and 36 of 45 (80%) were positive for the in vivo CA test. Higher sensitivity was seen in in vivo CMT (90%) and in vitro CMT (86.9%) assay. Combination of two tests has greater sensitivity than individual tests: in vivo MN + in vivo CA (88.6%); in vivo MN + in vivo CMT (92.5%); and in vivo MN + in vitro CMT (95.6%). Combinations of in vivo or in vitro CMT with other tests provided better sensitivity. In vivo CMT in combination with in vivo CA provided the highest sensitivity (96.7%). 相似文献
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目的 检测Wentilactone A的遗传毒性。方法 应用经典遗传毒性检测组合(Ames试验、体外培养CHO细胞染色体畸变试验和小鼠骨髓微核试验)检测Wentilactone A的遗传毒性。结果 Ames试验结果提示,Wentilactone A在每皿5 000、500、50、5、0.5 μg 5个剂量下,在加和不加代谢活化系统(S9)时,对鼠伤寒沙门菌均无致突变性。CHO细胞染色体畸变试验结果提示,在终浓度23.74、47.48、94.96 μg/ml 3个剂量组,在加和不加S9中,于作用4 h和24 h的条件下培养的CHO细胞,均未诱发染色体畸变。小鼠骨髓微核试验在100、200、400 mg/kg 3个剂量下作用24 h以及400 mg/kg剂量下作用48 h对骨髓细胞的微核诱发率,与溶剂对照组比较均无显著差异(P>0.05)。结论 Wentilactone A对鼠伤寒沙门菌无致突变性,对CHO细胞的染色体无致畸变作用,对ICR小鼠无诱发骨髓细胞微核的效应。上述结果提示Wentilactone A不具有遗传毒性和潜在致癌性。 相似文献
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Context: Black tea has been reported to have significant antimutagenic and anticarcinogenic properties associated with its polyphenols theaflavins (TF) and thearubigins (TR). Similarly, Turkish black tea (TBT) also contains a considerable amount of TF and TR.Objective: This study investigated the mutagenic, antimutagenic and anticlastogenic properties of TBT.Materials and methods: The mutagenic and antimutagenic effects of TBT (10 to 40000?μg/plate) were investigated in vitro on Salmonella strains TA98 and TA100 with and without S9 fraction. Anticlastogenic effect was studied at concentrations of 300–1200?mg/kg TBT extract by chromosomal aberrations (CA) assay from bone marrow of mice.Results: The results of this study did not reveal any mutagenic properties of TBT. On the contrary, TBT extract exhibited antimutagenic activity at >1000?μg/plate concentrations in TA98 strain with and without S9 activation (40% inhibition with S9 and 27% without S9). In TA100 strain, the antimutagenic activity was observed at?>20,000?μg/plate TBT extracts without S9 activation (28% inhibition) and at >1000?μg/plate with S9 activation (59% inhibition). A significant decrease in the percentage of aberrant cells (12.33%?±?1.27) was observed in dimethylbenz(a)anthracene (DMBA) plus highest concentration (1200?mg/kg) of TBT extract-treated group when compared to only DMBA-treated group (17.00%?±?2.28).Discussion and conclusion: Results indicated that TBT can be considered as genotoxically safe, because it did not exert any mutagenic and clastogenic effects. As a result, TBT exhibited antimutagenic effects more apparently after metabolic activation in bacterial test system and had an anticlastogenic effect in mice. 相似文献
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二乙基二硫代氨基甲酸钠抑制顺铂的致突变作用 总被引:1,自引:1,他引:0
王青定周玉宁张培棪 《中国药理学与毒理学杂志》1996,3(3):207-210
二乙基二硫代氨基甲酸钠(DDTC)能明显抑制顺铂诱导鼠伤寒沙门氏菌TA100,TA98回变,有S9代谢活化系统时抑制作用增强,160.74μg/plateDDTC对0.25~2.00μg/plate顺铂抑制率为87.4%~95.7%(TA100)和89.4%~105.5%(TA98).小鼠ip顺铂1.5mg·kg-1,24h重复ip1次,每次给顺铂后1hipDDTC400~800mg·kg-1或同时igDDTC750~1500mg·kg-1.可显著降低顺铂诱发小鼠骨髓多染红细胞微核的形成.体内外实验结果表明DDTC可降低顺铂的致突变作用 相似文献