Detection of the four sequence variations of MDR1 gene using TaqMan MGB probe based real-time PCR and haplotype analysis in healthy Japanese subjects |
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Authors: | Saito Katsuhiko Miyake Sachie Moriya Hiroyuki Yamazaki Miyuki Itoh Fumio Imai Kohzoh Kurosawa Nahoko Owada Eiji Miyamoto Atsushi |
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Affiliation: | Division of Pharmaceutical Health Care and Sciences, Sapporo Medical University, South 1, West 16, Chuo-ku, Sapporo, 060-8543 Japan. ksaitoh@sapmed.ac.jp |
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Abstract: | OBJECTIVES: P-glycoprotein (P-gp) is significant from the viewpoint of pharmacokinetics/pharmacodynamics (PK/PD). MDR1 gene encodes P-gp and has a wide variety of SNPs. As the SNPs may be one of the factors that induce pharmacogenetic individual difference, haplotype analysis is necessary to evaluate the PK/PD. DESIGN AND METHODS: The SNPs of the detected MDR1 were -129T>C, 325G>A, 2677G>T/A, and 3435C>T. For the analysis of linkage disequilibrium (LD) and haplotype analysis, and for the reconstruction of the haplotype pair, ARLEQUIN and PHASE were employed. RESULTS: The result of the chi(2) test detected significant LD between -129 and 2677, -129 and 3435, and 2677 and 3435. There were 9 haplotypes: T-G-C, T-T-C, C-T-C, T-A-C, C-A-C, T-G-T, T-T-T, C-G-T, and C-T-T. CONCLUSIONS: LD was found among the positions -129, 2677 and 3435. As a result, 9 haplotypes exists in the Japanese population. These results suggest that it would be necessary to give consideration to haplotype for the purpose of evaluating the PK/PD of the drugs transported by P-gp. |
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Keywords: | MDR1 gene Multi-drug resistance P-glycoprotein Single nucleotide polymorphisms SNPs Linkage disequilibrium Haplotype analysis Expectation-Maximization (EM) algorithm Real-time PCR |
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