Your search keyword '"Jieh-Yuan Liou"' showing total 6 results

1. Phosphorylation of Pyrimidine l-Deoxynucleoside Analog Diphosphates

Author

Preethi Krishnan, Jieh-Yuan Liou, and Yung-Chi Cheng

Subjects

chemistry.chemical_classification, biology, Kinase, Active site, Cell Biology, Biochemistry, Nucleoside-diphosphate kinase, Amino acid, Dephosphorylation, Enzyme, chemistry, biology.protein, Phosphorylation, Molecular Biology, Nucleoside

Abstract

Anticancer and antivirald- and l-nucleoside analogs are phosphorylated stepwise in the cells to the pharmacologically active triphosphate metabolites. We recently reported that in the last step,l-deoxynucleoside analog diphosphates are phosphorylated by 3-phosphoglycerate kinase (PGK). To explain the preference of PGK forl- over d-deoxynucleoside analog diphosphates, the kinetics of their phosphorylation were compared with the dephosphorylation of the respective triphosphates using recombinant human PGK. The results attributed favorable phosphorylation ofl-deoxynucleoside analog diphosphates by PGK to differences in k cat, which were consequences of varied orientations of the sugar and diphosphates in the catalytic site of PGK. The amino acids involved in the catalytic reaction of PGK (including Glu344, Lys220, and Asn337) were therefore mutated. The impact of mutations on the phosphorylation of l- and d-deoxynucleoside analog diphosphates was different from those on dephosphorylation of the respective triphosphates. This suggested that the interactions of the nucleoside analogs with amino acids during the transition state are different in the phosphorylation and dephosphorylation reactions. Thus, reversible action of the enzyme may not involve the same configuration of the active site. Furthermore, the amino acid determinants of the action of PGK for l-deoxynucleotides were not the same as for the d-deoxynucleotides. This study also suggests the potential impact of nucleoside analog diphosphates and triphosphates on the multiple cellular functions of PGK, which may contribute to the action of the analogs.

Published

2002

2. Phosphorylation of Pyrimidine Deoxynucleoside Analog Diphosphates

Author

Yung-Chi Cheng, Ginger E. Dutschman, Wing Lam, Qin Fu, Preethi Krishnan, and Jieh-Yuan Liou

Subjects

chemistry.chemical_classification, biology, Pyrimidine, Chemistry, Kinase, Stereochemistry, Cell Biology, Biochemistry, Nucleoside-diphosphate kinase, chemistry.chemical_compound, Enzyme, biology.protein, Phosphorylation, Creatine kinase, Molecular Biology, Nucleoside, Pyruvate kinase

Abstract

D-Nucleoside analogs, which are in the natural configuration, as well as the L-nucleoside analogs, are clinically relevant antiviral and anticancer agents. Metabolism of L-nucleoside analog diphosphates to the triphosphates, however, remains unexplored. Studies with recombinant nm23-H1 and -H2 isoforms indicated that L-nucleoside analog diphosphates were not phosphorylated by their nucleoside diphosphate kinase (NDPK) activity. Therefore, roles of creatine kinase, 3-phosphoglycerate kinase, and pyruvate kinase were evaluated using preparations from commercial sources and human HepG2 cells. Phosphorylation of L-OddC, L-SddC, L-Fd4C, L-FMAU, and L-ddC were compared with D-deoxynucleoside analogs, AraC, dFdC, and D-FMAU, and D-dideoxynucleoside analogs, ddC and d4T. Results based on preparations from HepG2 cells showed that L-nucleoside analog diphosphates were selectively phosphorylated by 3-phosphoglycerate kinase, whereas, D-deoxynucleoside analog diphosphates were phosphorylated by NDPK. Interestingly, ddCDP and d4TDP were substrates for creatine kinase, but were not phosphorylated by NDPK. In conclusion, it is proposed that specificity of the phosphorylating enzymes toward the nucleoside analog diphosphates is dependent on the configuration of the analog (L or D) and the presence or absence of 3'-hydroxyl group in the sugar moiety. The enzymatic process of phosphorylation of L- and D-nucleoside analog diphosphates is different in cells.

Published

2002

3. Modulation of human UMP/CMP kinase affects activation and cellular sensitivity of deoxycytidine analogs

Author

Wei-Ling Chang, Yung-Chi Cheng, Yu-Chun Huang, Mei-Ju Hsieh, Hui-Ru Lai, Chih-Hung Hsu, and Jieh-Yuan Liou

Subjects

Down-Regulation, Antineoplastic Agents, Biology, Biochemistry, Deoxycytidine, Cell Line, Pyrimidine analogue, Cell Line, Tumor, Humans, RNA, Messenger, Phosphorylation, Pharmacology, chemistry.chemical_classification, Dose-Response Relationship, Drug, Cell growth, Kinase, Deoxycytidine Monophosphate, Enzyme Activation, Enzyme, chemistry, Cell culture, Pyrimidine metabolism, Nucleoside-Phosphate Kinase, Cytidylate kinase, HeLa Cells

Abstract

Deoxycytidine analogs are an important class of clinically active antiviral and anticancer agents. The stepwise phosphorylation of these analogs to triphosphate metabolites is crucial for biological action. Human UMP/CMP kinase (UMP/CMPK; cytidylate kinase; EC 2.7.4.14) is thought to be responsible for phosphorylation of UMP, CMP, and dCMP and may also play an important role in the activation of pyrimidine analogs. However, no evidence has verified this notion in intact cells. In this study we explored the functional roles of UMP/CMPK in natural pyrimidine synthesis and metabolism of deoxycytidine analogs, as well as 5-FU in HeLa S3 and HCT8 cells. The amounts of UMP/CMPK protein in different cell lines correlated with UMP, CMP, and dCMP kinase activities and amounts of UMP/CMPK RNA. Modulation of UMP/CMPK by overexpression or down-regulation had no impact on natural pyrimidine nucleotides and cell growth. However, down-regulating UMP/CMPK expression by siRNA led to a decrease in the formation of the triphosphate metabolites, resulting in cellular resistance to these analogs. More diphosphate and triphosphate metabolites of deoxycytidine analogs were detected and cellular sensitivity to these agents was increased in the UMP/CMPK-overexpressing cells. This study indicates that the second step enzyme (UMP/CMPK) is responsible for the phosphorylation of pyrimidine analogs and also has an impact on cellular sensitivity to these analogs in those cell lines.

Published

2009

4. Phosphorylation of Cytidine, Deoxycytidine, and Their Analog Monophosphates by Human UMP/CMP Kinase Is Differentially Regulated by ATP and Magnesium

Author

Chih-Hung Hsu, Jieh-Yuan Liou, Yung-Chi Cheng, and Ginger E. Dutschman

Subjects

Cytidine, Deoxycytidine, Substrate Specificity, chemistry.chemical_compound, Pyrimidine analogue, Adenosine Triphosphate, Cytidine Monophosphate, Humans, Phosphorylation, Pharmacology, chemistry.chemical_classification, Kinase, DCMP phosphorylation, Deoxycytidine monophosphate, Deoxycytidine Monophosphate, Molecular biology, carbohydrates (lipids), Kinetics, Enzyme, chemistry, Biochemistry, Molecular Medicine, Nucleoside-Phosphate Kinase, Cytidylate kinase

Abstract

Human UMP/CMP kinase (cytidylate kinase; EC 2.7.4.14) is responsible for phosphorylation of CMP, UMP, and deoxycytidine monophosphate (dCMP) and also plays an important role in the activation of pyrimidine analogs, some of which are clinically useful anticancer or antiviral drugs. Previous kinetic data using recombinant or highly purified human UMP/CMP kinase showed that dCMP, as well as pyrimidine analog monophosphates, were much poorer substrates than CMP or UMP for this enzyme. This implies that other unidentified mechanisms must be involved to make phosphorylation of dCMP or pyrimidine analog monophosphates inside cells by this enzyme possible. Here, we reevaluated the optimal reaction conditions for human recombinant human UMP/CMP kinase to phosphorylate dCMP and CMP (referred as dCMPK and CMPK activities). We found that ATP and magnesium were important regulators of the kinase activities of this enzyme. Free magnesium enhanced dCMPK activity but inhibited CMPK activity. Free ATP or excess ATP/magnesium, on the other hand, inhibited dCMPK but not CMPK reactions. The differential regulation of dCMPK versus CMPK activities by ATP or magnesium was also seen in other 2'-deoxypyrimidine analog monophosphates (deoxyuridine monophosphate, 5-fluorodeoxyuridine monophosphate, 1-beta-D-arabinofuranosylcytosine monophosphate, and gemcitabine monophosphate) versus their ribose-counterparts (UMP and 5-fluorouridine monophosphate), in a similar manner. The data suggest that the active sites of human UMP/CMP kinase for dCMP and for CMP cannot be identical. Furthermore, enzyme inhibition studies demonstrated that CMP could inhibit dCMP phosphorylation in a noncompetitive manner, with Ki values much higher than its own Km values. We thus propose novel models for the phosphorylation action of human UMP/CMP kinase.

Published

2004

5. Phosphorylation of pyrimidine L-deoxynucleoside analog diphosphates. Kinetics of phosphorylation and dephosphorylation of nucleoside analog diphosphates and triphosphates by 3-phosphoglycerate kinase

Author

Preethi, Krishnan, Jieh-Yuan, Liou, and Yung-Chi, Cheng

Subjects

Carcinoma, Hepatocellular, Base Sequence, Liver Neoplasms, Molecular Conformation, Antineoplastic Agents, Purine Nucleosides, Antiviral Agents, Recombinant Proteins, Substrate Specificity, Models, Structural, Kinetics, Phosphoglycerate Kinase, Amino Acid Substitution, Mutagenesis, Site-Directed, Tumor Cells, Cultured, Humans, Phosphorylation, Purine Nucleotides, DNA Primers

Abstract

Anticancer and antiviral D- and L-nucleoside analogs are phosphorylated stepwise in the cells to the pharmacologically active triphosphate metabolites. We recently reported that in the last step, L-deoxynucleoside analog diphosphates are phosphorylated by 3-phosphoglycerate kinase (PGK). To explain the preference of PGK for L- over D-deoxynucleoside analog diphosphates, the kinetics of their phosphorylation were compared with the dephosphorylation of the respective triphosphates using recombinant human PGK. The results attributed favorable phosphorylation of L-deoxynucleoside analog diphosphates by PGK to differences in k(cat), which were consequences of varied orientations of the sugar and diphosphates in the catalytic site of PGK. The amino acids involved in the catalytic reaction of PGK (including Glu(344), Lys(220), and Asn(337)) were therefore mutated. The impact of mutations on the phosphorylation of L- and D-deoxynucleoside analog diphosphates was different from those on dephosphorylation of the respective triphosphates. This suggested that the interactions of the nucleoside analogs with amino acids during the transition state are different in the phosphorylation and dephosphorylation reactions. Thus, reversible action of the enzyme may not involve the same configuration of the active site. Furthermore, the amino acid determinants of the action of PGK for L-deoxynucleotides were not the same as for the D-deoxynucleotides. This study also suggests the potential impact of nucleoside analog diphosphates and triphosphates on the multiple cellular functions of PGK, which may contribute to the action of the analogs.

Published

2002

6. Characterization of human UMP/CMP kinase and its phosphorylation of D- and L-form deoxycytidine analogue monophosphates

Author

Jieh-Yuan, Liou, Ginger E, Dutschman, Wing, Lam, Zaoli, Jiang, and Yung-Chi, Cheng

Subjects

Gene Expression, Stereoisomerism, Deoxycytidine, KB Cells, Recombinant Proteins, Pyrimidines, Antibody Specificity, Cytidine Monophosphate, Escherichia coli, Humans, Cloning, Molecular, Phosphorylation, Nucleoside-Phosphate Kinase, HeLa Cells, Subcellular Fractions

Abstract

Pyrimidine nucleoside monophosphate kinase [UMP/CMP kinase (UMP/CMPK);EC 2.7.4.14] plays a crucial role in the formation of UDP, CDP, and dCDP, which are required for cellular nucleic acid synthesis. Several cytidine and deoxycytidine analogues are important anticancer and antiviral drugs. These drugs require stepwise phosphorylation to their triphosphate forms to exert their therapeutic effects. The role of UMP/CMPK for the phosphorylation of nucleoside analogues has been indicated. Thus, we cloned the human UMP/CMPK gene, expressed it in Escherichia coli, and purified it to homogeneity. Its kinetic properties were determined. UMP and CMP proved to be far better substrates than dCMP. UMP/CMPK used all of the nucleoside triphosphates as phosphate donors, with ATP and dATP being the best donors and CTP being the poorest. Furthermore, UMP/CMPK was able to phosphorylate all of the deoxycytidine analogue monophosphates that we tested. The relative efficiency was as follows: arabinofuranosyl-CMPdCMPbeta-L-2',3'-dideoxy-3'-thia-CMPGemcitabine monophosphatebeta-D-2',3'-dideoxy-CMP; beta-L-2',3'-dideoxy-2',3'-didehydro-5-fluoro-CMP; beta-L-2',3'-dideoxy-5-fluoro-3'-thia-CMPbeta-L-2',3'-dideoxy-CMPbeta-L-dioxolane-CMP. By comparing the relative V(max)/K(m) values of D- and L-form dideoxy-CMP, we showed that this kinase lacked stereoselectivity. Reducing agents, such as DTT, 2-mercaptoethanol, and thioredoxin, were able to activate this enzyme, suggesting that its activity may be regulated by redox potential in vivo. UMP/CMPK localized predominantly to the cytoplasm. In addition, 196-amino acid UMP/CMPK was the actual form of UMP/CMPK, rather than the 228-amino acid form as suggested before.

Published

2002