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A multiplex single nucleotide polymorphism genotyping method using ligase-based mismatch discrimination and CE-SSCP

Authors
Choi, WoongShin, Gi WonHwang, Hee SungPack, Seung PilJung, Gyu YongJung, Gyoo Yeol
Issue Date
Apr-2014
Publisher
WILEY
Keywords
CE-SSCP; Diagnostic assay; Ligase-based genotyping assay; Multiplex analysis; SNP
Citation
ELECTROPHORESIS, v.35, no.8, pp.1196 - 1203
Indexed
SCIE
SCOPUS
Journal Title
ELECTROPHORESIS
Volume
35
Number
8
Start Page
1196
End Page
1203
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/98820
DOI
10.1002/elps.201300486
ISSN
0173-0835
Abstract
Accuracy, simplicity, and cost-effectiveness are the most important criteria for a genotyping method for SNPs compatible with clinical use. One method developed for SNP genotyping, ligase-based discrimination, is considered the simplest for clinical diagnosis. However, multiplex assays using this method are limited by the detection method. Although CE has been introduced as an alternative to error prone microarray-based detection, the design process and multiplex assay procedure are complicated because of the DNA size-dependent separation principle. In this study, we developed a simple and accurate multiplex genotyping method using reaction condition-optimized ligation and high-resolution CE-based SSCP. With this high-resolution CE-SSCP system, we are able to use similar-sized probes, thereby eliminating the complex probe design step and simplifying the optimization process. We found that this method could accurately discriminate single-base mismatches in SNPs of the tp53 gene, used as targets for multiplex detection.
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