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A critical review of the genetic toxicity of steviol and steviol glycosides.

机译:甜菊糖和甜菊糖苷遗传毒性的严格综述。

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摘要

Extracts of the leaves of the stevia plant (Stevia rebaudiana Bertoni) are used to sweeten food and beverages in South America, Japan and China. The components responsible for the sweet properties of the plant are glycosides of steviol, primary stevioside (ent-13-hydroxykaur-16-en-18-oic acid), which is 250-300 times sweeter than sucrose and rebaudiosides A and C. Stevioside and steviol have been subjected to extensive genetic testing. The majority of the findings show no evidence of genotoxic activity. Neither stevioside nor its aglycone steviol have been shown to react directly with DNA or demonstrate genotoxic damage in assays relevant to human risk. The mutagenic activity of steviol and some of its derivatives, exhibited in strain TM677, was not reproduced in the same bacteria having normal DNA repair processes. The single positive in vivo study measuring single-strand DNA breaks in Wistar rat tissues by stevioside, was not confirmed in experiments in mice and appears to be measuring processes other than direct DNA damage. Neither stevioside nor steviol-induced clastogenic effects at extremely high dose levels in vivo. Application of a Weight-of-Evidence approach to assess the genetic toxicology database concludes that these substances do not pose a risk of genetic damage following human consumption.
机译:甜菊植物(Stevia rebaudiana Bertoni)叶子的提取物在南美,日本和中国用于增甜食品和饮料。负责植物甜味特性的成分是甜菊醇的糖苷,主要的甜菊糖苷(ent-13-hydroxykaur-16-en-18-oic acid),其甜度比蔗糖和莱鲍迪苷A和C的甜度高250-300倍。和甜菊醇已经过广泛的基因测试。大多数发现没有显示出遗传毒性活性的证据。在与人类风险相关的测定中,甜菊糖苷或其糖苷甜菊醇均未显示直接与DNA反应或显示出遗传毒性损害。在TM677菌株中显示的甜菊醇及其某些衍生物的诱变活性未在具有正常DNA修复过程的同一细菌中重现。甜菊糖测定Wistar大鼠组织中单链DNA断裂的单项阳性体内研究尚未在小鼠实验中得到证实,并且似乎是在测量直接DNA损伤以外的过程。甜菊糖甙和甜菊醇在体内的极高剂量水平下均不产生致胶剂作用。证据权重方法用于评估遗传毒理学数据库的结论是,这些物质在人类食用后不会造成遗传损害的风险。

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