首页> 外文期刊>Nucleic Acids Research >MULTIPLEX FLUORESCENCE-BASED PRIMER EXTENSION METHOD FOR QUANTITATIVE MUTATION ANALYSIS OF MITOCHONDRIAL DNA AND ITS DIAGNOSTIC APPLICATION FOR ALZHEIMERS DISEASE
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MULTIPLEX FLUORESCENCE-BASED PRIMER EXTENSION METHOD FOR QUANTITATIVE MUTATION ANALYSIS OF MITOCHONDRIAL DNA AND ITS DIAGNOSTIC APPLICATION FOR ALZHEIMERS DISEASE

机译:基于多重荧光的引物扩展方法用于线粒体DNA定量突变分析及其在阿尔茨海默氏病的诊断中的应用

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摘要

A sensitive and highly reproducible multiplexed primer extension assay is described for quantitative mutation analysis of heterogeneous DNA populations. Wild-type and mutant target DNA are simultaneously probed in competitive primer extension reactions using fluorophor-labeled primers and high fidelity thermostable DNA polymerases in the presence of defined mixtures of deoxy- and dideoxynucleotides, Primers are differentially extended and the resulting products are distinguished by size and dye label. Wild-type:mutant DNA ratios are determined from the fluorescence intensities associated with electrophoretically resolved reaction products, Multiple nucleotide sites can be simultaneously interrogated with uniquely labeled primers of different lengths, The application of this quantitative technique is shown in the analysis of heteroplasmic point mutations in mitochondrial DNA that are associated with Alzheimer's disease.
机译:描述了一种灵敏且高度可重复的多重引物延伸测定法,用于异种DNA群体的定量突变分析。在脱氧核苷酸和双脱氧核苷酸定义的混合物存在下,使用荧光团标记的引物和高保真热稳定的DNA聚合酶,在竞争性引物延伸反应中同时探测野生型和突变目标DNA,对引物进行差异延伸,并按大小区分所得产物和染料标签。野生型:突变DNA的比例由电泳分离的反应产物的荧光强度确定,多个核苷酸位点可同时用独特标记的不同长度的引物进行询问,该定量技术在异质点突变分析中的应用与阿尔茨海默氏病有关的线粒体DNA中

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