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评估非洲爪蟾胚胎致畸试验(FETAX)的预测效度。

Assessing the predictive validity of frog embryo teratogenesis assay-Xenopus (FETAX).

作者信息

Fort D J, Stover E L, Farmer D R, Lemen J K

机构信息

The Stover Group, Stillwater, OK 74074, USA.

出版信息

Teratog Carcinog Mutagen. 2000;20(2):87-98.

Abstract

The ability of frog embryo teratogenesis assay - Xenopus (FETAX) to identify the potential developmental toxicity of a group of diverse chemicals was evaluated by comparison with results from in vivo studies in rats. A total of 12 chemicals, three of which were shown to be teratogenic in vivo, four of which were embryolethal (but not teratogenic) in vivo, and five which did not produce any developmental toxicity in vivo in the rat were evaluated using FETAX. Results of the FETAX test with these 12 blind-coded compounds correctly predicted that three chemicals had strong teratogenic potential, four had low teratogenic hazard potential but were embryolethal, and five posed little if any developmental toxicity hazard. In addition, this study concluded that within a family of chemistry analogs could be ranked according to relative teratogenic hazard and that for the teratogenic compounds the types of malformations induced in Xenopus mimicked the abnormalities induced in vivo in rats. In summary, these results confirmed that the FETAX assay is predictive and can be useful in an integrated biological hazard assessment for the preliminary screening of chemicals. Teratogenesis Carcinog. Mutagen. 20:87-98, 2000.

摘要

通过与大鼠体内研究结果进行比较,评估了非洲爪蟾胚胎致畸试验(FETAX)识别一组不同化学品潜在发育毒性的能力。使用FETAX评估了总共12种化学品,其中3种在体内显示具有致畸性,4种在体内具有胚胎致死性(但无致畸性),5种在大鼠体内未产生任何发育毒性。对这12种盲编码化合物进行FETAX试验的结果正确预测出,3种化学品具有很强的致畸潜力,4种具有低致畸风险潜力但具有胚胎致死性,5种几乎不具有任何发育毒性风险。此外,本研究得出结论,在化学类似物家族中,可以根据相对致畸风险进行排序,并且对于致畸化合物,非洲爪蟾中诱导的畸形类型与大鼠体内诱导的异常情况相似。总之,这些结果证实FETAX试验具有预测性,可用于化学品初步筛选的综合生物危害评估。《致畸、致癌、致突变》20:87 - 98,2000年。

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