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运用焦磷酸测序技术通过多重实时DNA测序进行细胞色素P450基因分型。

Cytochrome p450 genotyping by multiplexed real-time dna sequencing with pyrosequencing technology.

作者信息

Eriksson Solveig, Berg Lars M, Wadelius Mia, Alderborn Anders

机构信息

Pyrosequencing AB, Uppsala, Sweden.

出版信息

Assay Drug Dev Technol. 2002 Nov;1(1 Pt 1):49-59. doi: 10.1089/154065802761001301.

DOI:10.1089/154065802761001301
PMID:15090156
Abstract

Individual differences in xenobiotic metabolism influence the therapeutic value of many drugs and are of major concern during the development of new drug candidates. A number of polymorphic cytochrome p450 enzymes account for a significant part of this variation. A better understanding of these genetic factors would be of value for drug development, as well as clinical practice. To fulfill the goal of a personalized medicine, methods for simple and accurate assessment of cytochrome p450 genes are required. We report on the development of multiplex assays for genotyping of the cytochrome p450 drug-metabolizing enzymes CYP2D6, CYP2C9, and CYP2C19 with Pyrosequencing technology. Eleven variable positions, representing 12 of the most frequent alleles, were scored: CYP2D6 alleles *2, *3, *4, *6, *7, *8, and *14, CYP2C19 alleles *2, *3, and *4, and CYP2C9 alleles *2 and *3. Four multiplex Pyrosequencing reactions per patient sample were performed to cover these positions, using either simplex or multiplex PCR for amplification of target DNA sequences. Unequivocal genotypes were obtained for all patient samples, and the results were validated by comparing with results obtained using PCR-RFLP. For positions addressed with both methods, the results were in complete agreement. Pyrosequencing technology offers a highly automated, rapid, and accurate method for identification of cytochrome p450 alleles, which is suitable for pharmacogenomic research, as well as for routine assessment of patient genotypes.

摘要

外源性物质代谢的个体差异影响许多药物的治疗价值,并且在新药候选物的研发过程中是主要关注的问题。多种多态性细胞色素P450酶在这种变异中占很大一部分。更好地理解这些遗传因素对于药物研发以及临床实践都将具有价值。为了实现个性化医疗的目标,需要简单且准确地评估细胞色素P450基因的方法。我们报道了利用焦磷酸测序技术对细胞色素P450药物代谢酶CYP2D6、CYP2C9和CYP2C19进行基因分型的多重检测方法的开发。对代表12个最常见等位基因的11个可变位点进行了评分:CYP2D6等位基因*2、*3、4、6、7、8和14,CYP2C19等位基因2、3和4,以及CYP2C9等位基因2和3。对每个患者样本进行四次多重焦磷酸测序反应以覆盖这些位点,使用单重或多重PCR扩增目标DNA序列。所有患者样本均获得了明确的基因型,并且通过与使用PCR-RFLP获得的结果进行比较来验证结果。对于两种方法都检测的位点,结果完全一致。焦磷酸测序技术为细胞色素P450等位基因的鉴定提供了一种高度自动化、快速且准确的方法,适用于药物基因组学研究以及患者基因型的常规评估。

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