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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The use of the in vitro micronucleus assay to detect and assess the aneugenic activity of chemicals.
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The use of the in vitro micronucleus assay to detect and assess the aneugenic activity of chemicals.

机译:使用体外微核检测来检测和评估化学物质的气生成活性。

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摘要

The successful validation of the in vitro micronucleus assay by the SFTG now provides the opportunity for this highly cost effective assay to be used to screen chemicals for their ability to induce both structural (clastogenic) and numerical (aneugenic) chromosome changes using interphase cells. The use of interphase cells and a relatively simple experimental protocol provides the opportunity to greatly increase the statistical power of cytogenetic studies on chemical interactions. The application of molecular probes capable of detecting kinetochores and centromeres provides the opportunity to classify mechanisms of micronucleus induction into those which are primarily due to chromosome loss or breakage. When a predominant mechanism of micronucleus induction has been shown to be based upon chromosome loss then further investigation can involve the determination of the role of non-disjunction in the induction of aneuploidy. The binucleate cell modification of the in vitro micronucleus assay can be combined with the use of chromosome specific centromere probes to determine the segregation of individual chromosomes into daughter nuclei. The combination of these methods provides us with powerful tools for the investigation of mechanisms of genotoxicity particularly in the low dose regions.
机译:SFTG对体外微核测定的成功验证现在提供了这种高成本效益的测定方法的机会,该测定法可用于使用相间细胞筛选化学物质诱导结构性(破灭性)和数字性(成神经性)染色体变化的能力。相间细胞的使用和相对简单的实验方案提供了极大地提高细胞遗传学研究化学相互作用的统计能力的机会。能够检测动植物和着丝粒的分子探针的应用提供了将微核诱导机制分类为主要归因于染色体丢失或断裂的机制的机会。当显示微核诱导的主要机理是基于染色体丢失时,则进一步的研究可能涉及确定非分离在非整倍性诱导中的作用。体外微核分析的双核细胞修饰可以与染色体特异性着丝粒探针结合使用,以确定单个染色体向子核的分离。这些方法的组合为我们提供了研究遗传毒性机制的强大工具,尤其是在低剂量区域。

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