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Metabolic Toxicity Screening Using Electrochemiluminescence Arrays Coupled with Enzyme-DNA Biocolloid Reactors and Liquid Chromatography-Mass Spectrometry

机译:使用电化学发光阵列与酶-DNA生物胶体反应器和液相色谱-质谱联用筛选代谢毒性

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摘要

New chemicals or drugs must be guaranteed safe before they can be marketed. Despite widespread use of bioassay panels for toxicity prediction, products that are toxic to a subset of the population often are not identified until clinical trials. This article reviews new array methodologies based on enzyme/DNA films that form and identify DNA-reactive metabolites that are indicators of potentially genotoxic species. This molecularly based methodology is designed in a rapid screening array that utilizes electro-chemiluminescence (ECL) to detect metabolite-DNA reactions, as well as biocolloid reactors that provide the DNA adducts and metabolites for liquid chromatography-mass spectrometry (LC-MS) analysis. ECL arrays provide rapid toxicity screening, and the biocolloid reactor LC-MS approach provides a valuable follow-up on structure, identification, and formation rates of DNA adducts for toxicity hits from the ECL array screening. Specific examples using this strategy are discussed. Integration of high-throughput versions of these toxicity-screening methods with existing drug toxicity bioassays should allow for better human toxicity prediction as well as more informed decision making regarding new chemical and drug candidates.
机译:必须保证新化学药品或药物在销售之前是安全的。尽管生物测定法广泛用于毒性预测,但是直到临床试验通常才鉴定出对一部分人群有毒的产品。本文回顾了基于酶/ DNA膜的新阵列方法,这些膜形成并鉴定了DNA反应性代谢物,这些代谢物是潜在遗传毒性物种的指标。这种基于分子的方法学是在快速筛选阵列中设计的,该阵列利用电化学发光(ECL)来检测代谢物-DNA反应,以及为液相色谱-质谱(LC-MS)分析提供DNA加合物和代谢物的生物胶体反应器。 。 ECL阵列可提供快速的毒性筛查,而生物胶体反应器LC-MS方法可为ECL阵列筛查的毒性命中提供关于DNA加合物的结构,鉴定和形成速率的有价值的后续信息。讨论了使用该策略的特定示例。这些毒性筛选方法的高通量版本与现有药物毒性生物测定法的集成应该可以更好地预测人类的毒性,并就新的化学和药物候选者做出更明智的决策。

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