Twenty Novel Genetic Variations and Haplotype Structures of the DCK Gene Encoding Human Deoxycytidine Kinase (dCK)

Su-Ryang KIM; Yoshiro SAITO; Keiko MAEKAWA; Emiko SUGIYAMA; Nahoko KANIWA; Hideki UENO; Takuji OKUSAKA; Masafumi IKEDA; Chigusa MORIZANE; Noboru YAMAMOTO; Teruhiko YOSHIDA; Naoyuki KAMATANI; Junji FURUSE; Hiroshi ISHII; Nagahiro SAIJO; Shogo OZAWA; Jun-ichi SAWADA

doi:10.2133/dmpk.23.379

SNP Communications

Twenty Novel Genetic Variations and Haplotype Structures of the DCK Gene Encoding Human Deoxycytidine Kinase (dCK)

Su-Ryang KIM, Yoshiro SAITO, Keiko MAEKAWA, Emiko SUGIYAMA, Nahoko KANIWA, Hideki UENO, Takuji OKUSAKA, Masafumi IKEDA, Chigusa MORIZANE, Noboru YAMAMOTO, Teruhiko YOSHIDA, Naoyuki KAMATANI, Junji FURUSE, Hiroshi ISHII, Nagahiro SAIJO, Shogo OZAWA, Jun-ichi SAWADA

著者情報

Su-Ryang KIM
Project Team for Pharmacogenetics, National Institute of Health Sciences
Yoshiro SAITO
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Functional Biochemistry and Genomics, National Institute of Health Sciences
Keiko MAEKAWA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Functional Biochemistry and Genomics, National Institute of Health Sciences
Emiko SUGIYAMA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Sciences, National Institute of Health Sciences
Nahoko KANIWA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Medicinal Safety Sciences, National Institute of Health Sciences
Hideki UENO
Hepatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital
Takuji OKUSAKA
Hepatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital
Masafumi IKEDA
Hepatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital
Chigusa MORIZANE
Hepatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital
Noboru YAMAMOTO
Thoracic Oncology Division, National Cancer Center Hospital
Teruhiko YOSHIDA
Genetics Division, National Cancer Center Research Institute
Naoyuki KAMATANI
Division of Genomic Medicine, Department of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University
Junji FURUSE
Hapatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital East
Hiroshi ISHII
Hapatobiliary and Pancreatic Oncology Division, National Cancer Center Hospital East
Nagahiro SAIJO
Deputy Director, National Cancer Center Hospital East
Shogo OZAWA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Pharmacology, National Institute of Health Sciences
Jun-ichi SAWADA
Project Team for Pharmacogenetics, National Institute of Health Sciences
Division of Functional Biochemistry and Genomics, National Institute of Health Sciences

キーワード: DCK, genetic variation, haplotype, gemcitabine, ethnic differences

ジャーナルフリー

2008 年 23 巻 5 号 p. 379-384

DOI https://doi.org/10.2133/dmpk.23.379

詳細

抄録

Deoxycytidine kinase (dCK) is a rate-limiting enzyme in the activation of nucleoside anticancer drugs, such as gemcitabine and cytarabine (Ara-C), to their active metabolites. In this study, the 5′-flanking region, 7 exons and their flanking introns of DCK were comprehensively screened for genetic variations in 256 Japanese cancer patients administered gemcitabine. Twenty-nine genetic variations, including twenty novel ones, were found: 11 in the 5′-flanking region, 1 in the 5′-untranslated region (UTR), 1 in the coding exon, 9 in the 3′-UTR, and 7 in the introns. The novel variations included -1110C>T, -757G>A, -639C>T, -465G>A, -402T>C, -224C>A, -199C>G, IVS1+38G>T, IVS2+78_+83delTTTTTC, IVS3-9C>T, IVS4+12T>C, IVS5+39T>C, 1357A>G, 1545A>T, 1572delA, 1736G>A, 1749G>A, 1838T>C, 1889G>A, and 2048A>T. The frequencies were 0.01 for IVS2+78_ +83delTTTTTC, 0.008 for -402T>C, 0.006 for -639C>T and IVS4+12T>C, 0.004 for -757G>A and 1572delA, and 0.002 for the other 14 variations. A known nonsynonymous SNP 364C>T (Pro122Ser) was detected at a 0.061 frequency. Using the detected polymorphisms, linkage disequilibrium analysis was performed, and 24 haplotypes were identified or inferred. Our findings suggest considerable ethnic differences in genetic variations of DCK and provide fundamental and useful information for genotyping DCK in the Japanese and probably other Asian populations.

責任著者(Corresponding author)

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