Ethnic Differences of two Non-synonymous Single Nucleotide Polymorphisms in CDA Gene

Emiko SUGIYAMA; Su-Jun LEE; Sang Seop LEE; Woo-Young KIM; Su-Ryang KIM; Masahiro TOHKIN; Ryuichi HASEGAWA; Haruhiro OKUDA; Manabu KAWAMOTO; Naoyuki KAMATANI; Jun-ichi SAWADA; Nahoko KANIWA; Yoshiro SAITO; Jae-Gook SHIN

doi:10.2133/dmpk.24.553

SNP Communications

Ethnic Differences of two Non-synonymous Single Nucleotide Polymorphisms in CDA Gene

Emiko SUGIYAMA, Su-Jun LEE, Sang Seop LEE, Woo-Young KIM, Su-Ryang KIM, Masahiro TOHKIN, Ryuichi HASEGAWA, Haruhiro OKUDA, Manabu KAWAMOTO, Naoyuki KAMATANI, Jun-ichi SAWADA, Nahoko KANIWA, Yoshiro SAITO, Jae-Gook SHIN

Author information

Emiko SUGIYAMA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Science, National Institute of Health Sciences
Su-Jun LEE
Department of Pharmacology and Pharmacogenomics Research Center, Inje University College of Medicine, Inje University
Sang Seop LEE
Department of Pharmacology and Pharmacogenomics Research Center, Inje University College of Medicine, Inje University
Woo-Young KIM
Department of Pharmacology and Pharmacogenomics Research Center, Inje University College of Medicine, Inje University
Su-Ryang KIM
Project Team for Pharmacogenetics, National Institute of Health Sciences
Masahiro TOHKIN
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Science, National Institute of Health Sciences
Ryuichi HASEGAWA
Division of Medicinal Safety Science, National Institute of Health Sciences
Haruhiro OKUDA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Organic Chemistry, National Institute of Health Sciences
Manabu KAWAMOTO
Division of Genomic Medicine, Department of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University
Naoyuki KAMATANI
Division of Genomic Medicine, Department of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University
Jun-ichi SAWADA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Nahoko KANIWA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Science, National Institute of Health Sciences
Yoshiro SAITO
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Science, National Institute of Health Sciences
Jae-Gook SHIN
Department of Pharmacology and Pharmacogenomics Research Center, Inje University College of Medicine, Inje University

Keywords: CDA, allele frequency, non-synonymous single nucleotide polymorphisms, ethnic-difference

JOURNAL FREE ACCESS

2009 Volume 24 Issue 6 Pages 553-556

DOI https://doi.org/10.2133/dmpk.24.553

Details

Abstract

Cytidine deaminase, encoded by the CDA gene, catalyzes anti-cancer drugs gemcitabine and ara-C into their respective inactive metabolites. In CDA, two functionally significant non-synonymous polymorphisms, 79A>C (Lys27Gln) and 208G>A (Ala70Thr), have been found and their minor allele frequencies (MAFs) were reported in Japanese and Chinese patients and a relatively small numbers of healthy volunteers in Caucasians and Africans. In this study, we determined the MAFs of both polymorphisms in 200 healthy volunteers of Koreans, along with 206 Japanese, 200 Chinese-Americans, 150 Caucasian-Americans and 150 African-Americans to reveal ethnic differences. MAFs of 79A>C (Lys27Gln) were 0.153 in Koreans and 0.327 in Caucasian-Americans, 0.204 in Japanese, 0.155 in Chinese-Americans and 0.087 in African-Americans. MAFs of 208G>A (Ala70Thr) were 0.005 in Koreans and 0.022 in Japanese and the minor allele was not detected in Chinese-Americans, Caucasian-Americans or African-Americans. Thus possibly, MAF of 208G>A in Japanese is likely to be somewhat higher than in Koreans and Chinese-Americans. These data would provide fundamental and useful information for pharmacogenetic studies on cytidine deaminase-catalyzing drugs.

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