Your search keyword '"Jae Yong Chung"' showing total 300 results

101. CYP3A5*3 Genotype Associated With Intrasubject Pharmacokinetic Variation Toward Tacrolimus in Bioequivalence Study

Author

Min Soo Park, Jae Yong Chung, Lay Ahyoung Lim, Seong Bok Jang, Yoon Jung Lee, and Kyung Hwan Kim

Subjects

Male, Genotype, Cmax, Biology, Pharmacology, Bioequivalence, Tacrolimus, Asian People, Pharmacokinetics, medicine, Cytochrome P-450 CYP3A, Humans, Pharmacology (medical), Randomized Controlled Trials as Topic, Cross-Over Studies, Korea, medicine.diagnostic_test, Genetic Variation, Crossover study, Calcineurin, Therapeutic Equivalency, Sample size determination, Therapeutic drug monitoring, Area Under Curve, Female, Immunosuppressive Agents

Abstract

Tacrolimus is metabolized by CYP3A and has highly variable pharmacokinetics. To study the factors contributing to this high variability in pharmacokinetics and to investigate the possibility of genotype-specific clinical applications, the effect of differing CYP3A5 genotypes on the intrasubject coefficients of variation for tacrolimus was investigated. Genotyping for CYP3A5*3 was performed in healthy volunteers who had previously participated in the pharmacokinetic study of 2 tacrolimus formulations with a 2 x 2 cross-over design. Intrasubject coefficients of variation calculated from analysis of variation in CYP3A5*1/*1+*1/*3 (n = 16) and CYP3A5*3/*3 (n = 13) groups were compared. The intrasubject CVs of AUClast and Cmax in the CYP3A5*3/*3 group were about 41.1% and 52.4% greater than those in the CYP3A5*1*1+*1/*3 group. The estimated total sample size for the bioequivalence study of tacrolimus with a 2 x 2 cross-over design was increased by 93.3% for AUClast (n = 30 versus 58) and 121.4% for Cmax (n = 28 versus 62) in the CYP3A5*3/*3 group compared with the CYP3A5*1/*1+*1/*3 group. The intraindividual variability of tacrolimus PK parameters may be associated with the CYP3A5 genotype. We propose that genotyping for CYP3A5 will provide a more efficient approach for bioequivalence designs and therapeutic drug monitoring.

Published

2010

102. Effects of SLCO1B1 and ABCB1 genotypes on the pharmacokinetics of atorvastatin and 2-hydroxyatorvastatin in healthy Korean subjects

Author

Youngjoo Lee, Lim La, Seong Bok Jang, Myung Gull Lee, and Jae Yong Chung

Subjects

Adult, Male, ATP Binding Cassette Transporter, Subfamily B, Genotype, Atorvastatin, Organic Anion Transporters, Pharmacology, Single oral dose, Lactones, Young Adult, Asian People, Pharmacokinetics, Polymorphism (computer science), Cytochrome P-450 CYP3A, Humans, Medicine, Pyrroles, Pharmacology (medical), ATP Binding Cassette Transporter, Subfamily B, Member 1, Allele, CYP3A5, Alleles, Korea, biology, Liver-Specific Organic Anion Transporter 1, business.industry, Heptanoic Acids, Area Under Curve, biology.protein, Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors, SLCO1B1, business, Half-Life, medicine.drug

Abstract

OBJECTIVE This study aimed to evaluate the effect of genetic polymorphisms of SLCO1B1 and ABCB1 on the pharmacokinetics of atorvastatin and its metabolites. METHODS 290 Koreans were genotyped for SLCO1B1, ABCB1 and CYP3A5, and 28 subjects were selected for the pharmacokinetic study. Each subject received a single oral dose of 20 mg atorvastatin and blood samples were collected up to 48 hr after dosing. The relationship between the genotypes and atorvastatin pharmacokinetics was examined. RESULTS For SLCO1B1 genotypes, the mean area under the concentration-time curve from time 0 to infinity (AUC0-infinity) of atorvastatin was 148.2 ng x hr/ml for *15/*15 subjects (n = 3), which was significantly larger than for 1a/*15 and *1b/*15 (n = 8) (80.7 ng x hr/ml, p = 0.0121) and also larger than for *1a/*1a, *1a/*1b and *1b/*1b (n = 17) (66.3 ng x hr/ml, p = 0.0018). The mean AUC0-infinity of 2-hydroxyatorvastatin for *15/*15 was also larger than in *1a/*1a, *1a/*1b and *1b/*1b (p = 0.012). In lactone forms, no significant pharmacokinetic difference was found among the genotypes. For ABCB1 genotypes, the half-lives of atorvastatin, atorvastatin lactone, 2-hydroxyatorvastatin and 2-hydroxyatorvastatin lactone were significantly longer in c.2677TT-c.3435TT (n = 3) vs. c.2677GG-c.3435CC and c.2677GT-c.3435CT (n = 10), yielding p = 0.049, 0.007, 0.007 and 0.007, respectively. CONCLUSION This study shows that the SLCO1B1*15 allele may be associated with the individual difference in the AUC0-infinity of atorvastatin whereas the ABCB1 TT-TT diplotype may affect the elimination half-life of the drug in the Korean population.

Published

2010

103. Safety, tolerability and pharmacokinetics of udenafil, a novel PDE-5 inhibitor, in healthy young Korean subjects

Author

Kyung Sang Yu, In Jin Jang, Dong-Ryul Sohn, Jung-Ryul Kim, Jae-Seung Paick, Hyeong-Seok Lim, Kyoung Soo Lim, Joo Youn Cho, Sang-Goo Shin, Bo-Hyung Kim, and Jae Yong Chung

Subjects

Adult, Male, medicine.drug_mechanism_of_action, Phosphodiesterase Inhibitors, Cmax, Administration, Oral, Pharmacology, Double-Blind Method, Erectile Dysfunction, Pharmacokinetics, Oral administration, medicine, Humans, Pharmacology (medical), Dosing, Adverse effect, Sulfonamides, Udenafil, Korea, Dose-Response Relationship, Drug, business.industry, Penile Erection, Pyrimidines, Pharmacodynamics, Tolerability, Area Under Curve, business, Phosphodiesterase 5 inhibitor, medicine.drug

Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • The phosphodiesterase (PDE) type 5 inhibitor is a widely used agent that facilitates penile erection. • Udenafil is newly developed as a PDE-5 inhibitor. WHAT THIS STUDY ADDS • This is the first study to determine the safety, tolerability and pharmacokinetics of udenafil in healthy subjects. • Udenafil was safe and well tolerated in healthy Korean subjects. • The AUC and Cmax of udenafil increased supraproportionally with increasing dose upon single administration, but there was no significant drug accumulation upon multiple administrations. AIM To evaluate the safety, tolerability and pharmacokinetics (PK) of udenafil, a novel phosphodiesterase type 5 inhibitor. METHODS A double-blind, randomized, placebo-controlled, dose-rising, parallel-group, single- and multiple-dose study was conducted in healthy Korean subjects. The subjects were allocated to single-dose groups of 25, 50, 100, 200 or 300 mg (eight subjects in each dose group, including two placebos), or to multiple-dose groups of 100 or 200 mg (once-daily dosing for 7 days; nine subjects in each dose group, including three placebos). Serial samples of blood and urine were collected after oral administration and the drug concentrations in plasma and urine were determined by high-performance liquid chromatography. Safety and tolerability were evaluated by monitoring clinical laboratory parameters and adverse events. RESULTS Udenafil reached peak plasma concentrations at 0.8–1.3 h, and then declined mono-exponentially with a terminal half-life of 7.3–12.1 h in the single-dose study. The area under the time–concentration curves (AUC) and maximum plasma concentrations (Cmax) increased supraproportionally with increasing dose in the single-dose study. During multiple dosing, a steady state was reached at 5 days and little accumulation occurred after repeated dosing for 7 days. Udenafil was generally well tolerated in these healthy subjects, and no serious adverse events occurred. CONCLUSIONS Udenafil was safe and well tolerated in healthy volunteers. The AUC and Cmax of udenafil increased supraproportionally with increasing dose upon single administration, but there was no significant drug accumulation upon multiple administrations.

Published

2008

104. An analysis of QTc prolongation with atypical antipsychotic medications and selective serotonin reuptake inhibitors using a large ECG record database

Author

Anhye Kim, Kyung Sang Yu, Sang In Park, Hyungmi An, Jae Yong Chung, and In-Jin Jang

Subjects

QTC PROLONGATION, Drug, Adult, Adolescent, Databases, Factual, medicine.drug_class, media_common.quotation_subject, Atypical antipsychotic, Tetrazoles, computer.software_genre, QT interval, 03 medical and health sciences, Electrocardiography, Electrolytes, Young Adult, 0302 clinical medicine, Sex Factors, Risk Factors, medicine, Humans, Pharmacology (medical), 030212 general & internal medicine, cardiovascular diseases, media_common, Aged, Retrospective Studies, Diazepam, Database, business.industry, Age Factors, General Medicine, Odds ratio, Middle Aged, Confidence interval, Cilostazol, Long QT Syndrome, Case-Control Studies, business, computer, 030217 neurology & neurosurgery, Selective Serotonin Reuptake Inhibitors, medicine.drug, Antipsychotic Agents

Abstract

Background: This study evaluated the effects of atypical antipsychotic drugs and selective serotonin reuptake inhibitors (SSRIs) on the corrected QT (QTc) interval using a large database obtained from clinical settings. Additionally, the effects of factors including age on QTc intervals were estimated. Methods: Using an open-access QT database (ECG-ViEW), QTc-lengthening effects of 14 selected atypical antipsychotics and SSRIs were compared to those of a positive control drug, cilostazol, and a negative control drug, diazepam. We also evaluated effects of age, sexgender, and select electrolyte levels on observed QTc intervals. Results: The frequency of QTc prolongation with the pooled data of the 14 study drugs was lower than that with cilostazol (age-adjusted odds ratio (OR) = 0.43, 95% confidence interval (CI) = 0.27-0.69), but no significant difference was found relative to when compared with that with diazepam (age-adjusted OR = 0.89, 95% CI = 0.55-1.47). Furthermore, administration of the 14 study drugs significantly increased the QTc interval by 2.89 ms after each 10-year age increment (p-value < 0.0001). Conclusions: This study suggests that atypical antipsychotic drugs and SSRIs are less likely to be associated with QTc prolongation in clinical settings. In addition, age showed a significant association with the QTc interval. Further studies with well-characterized cohorts are warranted.

Published

2016

105. Pharmacokinetics, Safety, and Tolerability of Metformin in Healthy Elderly Subjects

Author

Kyungho, Jang, Hyewon, Chung, Jang-Soo, Yoon, Seol-Joo, Moon, Seo Hyun, Yoon, Kyung-Sang, Yu, Kwangil, Kim, and Jae-Yong, Chung

Subjects

Adult, Aged, 80 and over, Blood Glucose, Male, Young Adult, Administration, Oral, Humans, Hypoglycemic Agents, Healthy Volunteers, Metformin, Aged

Abstract

Age-related physiological changes are known to alter the pharmacokinetics (PK) and pharmacodynamics (PD) of drugs. Metformin is commonly used as first-line medication for management of diabetes in elderly patients. However, the PK and PD of metformin have not been sufficiently studied in elderly subjects. Here, 12 elderly subjects, aged 65 to 85 years, and 20 younger healthy volunteers were orally administered 750 mg of metformin 2 hours after dinner, followed by administration of a second dose (500 mg) 12 hours later. An oral glucose tolerance test (OGTT) was performed 2 hours after the second dose, with 75 g of glucose administered. Blood samples were collected at specific time points after the second metformin dose for the assessment of PK and the glucose-lowering effect of metformin. Elderly subjects exhibited 1.7 and 2.0 times higher average Cmax and AUC∞ than the younger subjects, respectively (P = .007 and .001, respectively), and t1/2 was comparable between the elderly and younger subjects. However, relative glucose level changes from baseline after metformin administration tended to be lower in elderly subjects. Systemic exposure to metformin was elevated by 50% or more in elderly subjects, whereas the glucose-lowering effect was similar compared to younger subjects after 2 doses of metformin.

Published

2015

106. Development of a physiologically-based pharmacokinetic model for cyclosporine in Asian children with renal impairment.

Author

Sumin Yoon, Sojeong Yi, Su-jin Rhee, Hyun A Lee, Yun Kim, Kyung-Sang Yu, and Jae-Yong Chung

Subjects

JUVENILE diseases, DISABILITIES, ADULT-child relationships, PARAMETERS (Statistics), PHARMACOKINETICS

Abstract

This study aimed to assess the pharmacokinetics of cyclosporine A (CsA) in Asian children with renal impairment (RI) by developing a physiologically-based pharmacokinetic (PBPK) model with Simcyp Simulator. The PBPK model of Asian children with RI was developed by modifying the physiological parameters of the built-in population libraries in Simcyp Simulator. The ratio of healthy and RI populations was obtained for each parameter showing a difference between the populations. Each ratio was multiplied by the corresponding parameter in healthy Asian children. The model verification was performed with published data of Korean children with kidney disease given multiple CsA administrations. Simulations were performed with different combinations of ethnicity, age, and renal function to identify the net impact of each factor. The simulated results suggested that the effect of RI was higher in children than adults for both Caucasian and Asian. In conclusion, the constructed model adequately characterized CsA pharmacokinetics in Korean children with RI. Simulations with populations categorized by ethnicity, age, and renal function enabled to assess the net impact of each factor on specific populations. [ABSTRACT FROM AUTHOR]

Published

2019

107. Effect of () variant alleles on the pharmacokinetics of pitavastatin in healthy volunteers

Author

Joo Youn Cho, Sang-Goo Shin, Jae Yong Chung, Ki-Ho Moon, Jung-Ryul Kim, Kyung Sang Yu, In-Jin Jang, Hye-Ryung Jung, Dal-Seok Oh, and Kyoung-Soo Lim

Subjects

Pharmacology, Organic anion transporter 1, Cmax, Half-life, Biology, medicine.disease, Dose–response relationship, Pharmacokinetics, Hyperlipidemia, biology.protein, medicine, Pharmacology (medical), SLCO1B1, Pitavastatin, medicine.drug

Abstract

Background Pitavastatin is a potent, newly developed 3-hydroxy-3-methylglutaryl–coenzyme A reductase inhibitor for the treatment of hyperlipidemia. We characterized the effects of organic anion transporting polypeptide 1B1 (OATP1B1) alleles *1a, *1b, and *15 on the pharmacokinetics of pitavastatin. Methods Twenty–four healthy Korean volunteers who had previously participated in a pharmacokinetic study of pitavastatin (single oral dose, 1–8 mg) were further investigated. Subjects were grouped according to OATP1B1 genotype. Dose–normalized area under the plasma concentration–time curve (AUC) and peak plasma concentration (Cmax) values were analyzed, because different dosages were administered to subjects, whereas the pharmacokinetics showed linear characteristics. Results Dose-normalized pitavastatin AUCs for *1b/*1b (group 1), *1a/*1a or *1a/*1b (group 2), and *1a/*15 or *1b/*15 (group 3) were 38.8 ± 13.3, 54.4 ± 12.4, and 68.1 ± 16.3 ng · h · mL−1 · mg−1 (mean ± SD), respectively, with significant differences between all 3 groups (P = .008) and between subjects carrying and those not carrying the *15 allele (P = .004). Dose-normalized pitavastatin Cmax values were 13.2 ± 3.3, 18.2 ± 5.7, and 29.4 ± 9.6 ng · mL−1 · mg−1 in groups 1, 2, and 3, respectively, and also showed significant differences (P = .003) in a manner similar to that shown by AUC. No significant differences were found between the genotype groups in terms of dose-normalized AUC or Cmax values of pitavastatin lactone. Conclusion OATP1B1 variant haplotypes were found to have a significant effect on the pharmacokinetics of pitavastatin. These results suggest that the *15 allele is associated with decreased pitavastatin uptake from blood into hepatocytes and that OATP1B1 genetic polymorphisms have no effect on the pharmacokinetics of pitavastatin lactone. Clinical Pharmacology & Therapeutics (2005) 78, 342–350; doi: 10.1016/j.clpt.2005.07.003

Published

2005

108. Experimental studies on seismic behavior of steel coupling beams

Author

Yong-Chul Kim, Wan-Shin Park, Hyun-Do Yun, and Jae-Yong Chung

Subjects

Materials science, business.industry, Mechanical Engineering, Connection (vector bundle), Structural system, Seismic loading, Building and Construction, Structural engineering, Physics::Fluid Dynamics, Coupling (physics), Coupling beam, Resist, Mechanics of Materials, Shear strength, Shear wall, business, Civil and Structural Engineering

Abstract

Hybrid coupled shear walls in tall buildings are known as efficient structural systems to provide lateral resistance to wind and seismic loads. Multiple hybrid coupled shear walls throughout a tall building should be joined to provide additional coupling action to resist overturning moments caused by the lateral loading. This can be done using a coupling beam which connects two shear walls. In this study, experimental studies on the hybrid coupled shear wall were carried out. The main test variables were the ratios of coupling beam strength to connection strength. Finally, this paper provides background for rational design guidelines that include a design model to behave efficiently hybrid coupled shear walls.

Published

2005

109. Effect of the genotype on the pharmacokinetics, pharmacodynamics, and drug interactions of intravenous lorazepam in healthy volunteers

Author

In-Jin Jang, Kyoung-Soo Lim, Sang-Goo Shin, Hye-Ryung Jung, Jung-Ryul Kim, Kyung Sang Yu, Jae Yong Chung, and Joo Youn Cho

Subjects

Pharmacology, business.industry, medicine.drug_class, Lorazepam, Drug interaction, Confidence interval, Hypnotic, Pharmacokinetics, Pharmacodynamics, Sedative, Medicine, Pharmacology (medical), business, Rifampicin, medicine.drug

Abstract

Objective Our objective was to investigate the effect of the uridine 5′-diphosphate-glucuronosyltransferase (UGT) 2B15 genetic polymorphism on the pharmacokinetics and pharmacodynamics of lorazepam in basal, inhibited, and induced metabolic states in healthy normal volunteers. Methods Twenty-four healthy subjects were enrolled and grouped into UGT2B15*1/*1 or UGT2B15*2/*2 genotype groups. The pharmacokinetic and pharmacodynamic profiles of intravenous lorazepam were characterized before and after inhibition with 600 mg valproate once daily for 4 days and after induction with rifampin (INN, rifampicin) pretreatment (600 mg once daily for 10 days), with a washout period of 10 days between. The plasma concentrations of lorazepam and lorazepam glucuronide were analyzed before and at 0.25, 0.5, 1, 1.5, 2, 4, 6, 8, 12, 24, and 48 hours after lorazepam administration by liquid chromatography-tandem mass spectrometry. Visual analog scale assessments and psychomotor coordination tests were administered before and up to 12 hours after drug administration. Results The UGT2B15*2/*2 group showed 0.58-fold (95% confidence interval, 0.43–0.72; P

Published

2005

110. A variant 2677A allele of the gene affects fexofenadine disposition

Author

Jae Yong Chung, Sang-Goo Shin, Jung-Ryul Kim, So-Young Yi, Hyeong-Seok Lim, Kyung Sang Yu, In-Jin Jang, Hye-Ryung Jung, Joo Youn Cho, Kyoung-Sup Hong, and Dal-Seok Oh

Subjects

Pharmacology, medicine.medical_specialty, Fexofenadine, business.industry, Haplotype, Single-nucleotide polymorphism, Fexofenadine Hydrochloride, Endocrinology, Polymorphism (computer science), Internal medicine, Genotype, medicine, Pharmacology (medical), business, Allele frequency, Pharmacogenetics, medicine.drug

Abstract

Background and Objectives There have been considerable disagreements regarding the influence of MDR1 (ABCB1) polymorphisms on the disposition of P-glycoprotein (P-gp) substrates. We speculated that the unknown function of the A allele of exon 21 G2677T/A (Ala893Ser/Thr) provides one of the reasons for the contradictory results. This study was performed to clarify the effects of major MDR1 gene polymorphisms, including a variant A allele in exon 21, on fexofenadine pharmacokinetics. Methods We investigated the occurrence of 3 high-frequency single-nucleotide polymorphisms (SNPs) in exons 12 (C1236T), 21 (G2677T/A), and 26 (C3435T) of the MDR1 gene in 232 healthy Koreans, using a polymerase chain reaction-restriction fragment length polymorphism method, and performed haplotype analysis on these 3 SNPs. A single oral dose of 180 mg fexofenadine hydrochloride was administered to 33 healthy Korean male volunteers, who were divided into 6 groups based on the MDR1 genotype for the G2677T/A polymorphism in exon 21 and the C3435T polymorphism in exon 26. Results A strong linkage disequilibrium was observed among the 3 SNPs. The frequencies of the 4 major haplotypes, 1236C-2677A-3435C, C-G-C, T-G-C, and T-T-T, were 16.4%, 18.6%, 21.6%, and 32.2%, respectively. Fexofenadine disposition varied considerably among the groups. In the 2677AA/3435CC genotype group (n = 3), the values of area under the concentration-time curve from time 0 to 24 hours [AUC(0–24)] were significantly lower (P = .014) than those of the other 5 genotype groups (GG/CC, GT/CT, TT/TT, GA/CC, and TA/CT). As compared with the 2677GG/3435CC subjects, the AUC(0–24) values were 17% lower in the 2677AA/3435CC subjects and 47% higher in the 2677TT/3435TT subjects (GG/CC versus AA/CC versus TT/TT, 4017 ± 1137 ng · h/mL versus 3315 ± 958 ng · h/mL versus 5934 ± 2,064 ng · h/mL; P = .018). By stratification for genotypes at position 3435, homozygous 3435TT subjects were found to have significantly higher AUC(0–24) (P = .024) and maximum plasma concentration (P = .040) values than CC subjects [AUC(0–24), 5934 ± 2064 ng · h/mL versus 3998 ± 1241 ng · h/mL; maximum plasma concentration, 958 ± 408 ng/mL versus 673 ± 242 ng/mL]. Conclusions The plasma concentrations of fexofenadine after a single oral administration were lower in 2677AA/3435CC subjects than in subjects with the other 5 genotype combinations of the SNPs of G2677T/A and C3435T. These findings confirm the importance of analyzing MDR1 haplotypes and provide a plausible explanation for the conflicting results regarding the effect of MDR1 polymorphisms on the disposition of P-gp substrates. Clinical Pharmacology & Therapeutics (2004) 76, 418–427; doi: 10.1016/j.clpt.2004.08.002

Published

2004

111. Effect of the CYP3A5 genotype on the pharmacokinetics of intravenous midazolam during inhibited and induced metabolic states*1

Author

Sang-Goo Shin, Joo Youn Cho, Hyeong-Seok Lim, Kyung Sang Yu, Jung-Ryul Kim, In-Jin Jang, Jae Yong Chung, Jae-Gook Shin, So-Young Yi, Kwang-Hyeon Liu, Kyoung-Seop Hong, and Dal-Seok Oh

Subjects

Pharmacology, medicine.drug_class, Itraconazole, business.industry, Hypnotic, Pharmacokinetics, Sedative, Cytochrome P-450 CYP3A, medicine, Midazolam, Pharmacology (medical), business, Volunteer, Pharmacogenetics, medicine.drug

Abstract

Objective Our objective was to investigate the effect of the CYP3A5 genotype on the systemic clearance of midazolam in constitutive, inhibited, and induced metabolic conditions. Methods Nineteen healthy volunteers were grouped with regard to the CYP3A5*3 allele, into homozygous wild-type (CYP3A5*1/*1, n = 6), heterozygous (CYP3A5*1/*3, n = 6), and homozygous variant-type (CYP3A5*3/*3, n = 7) subject groups. The pharmacokinetic profile of intravenous midazolam was characterized before and after itraconazole administration (200 mg once daily for 4 days) and also after rifampin (INN, rifampicin) pretreatment (600 mg once daily for 10 days), with a washout period of 2 weeks in between. Results The pharmacokinetic profiles of midazolam and of its hydroxy metabolites did not show differences between the genotype groups under basal and induced metabolic conditions. However, during the inhibited metabolic state, the CYP3A5*3/*3 group showed a greater decrease in systemic clearance than was seen in the CYP3A5*1/*1 group (8.5 ± 3.8 L · h−1 · 70 kg−1 versus 13.5 ± 2.7 L · h−1 · 70 kg−1, P = .027). The 1′-hydroxymidazolam–to–midazolam area under the plasma concentration–time curve ratio was also significantly lower in the CYP3A5*3/*3 group (0.58 ± 0.35 versus 1.09 ± 0.37 for the homozygous wild-type group, P = .026). Conclusions The CYP3A5 genotype did not affect the pharmacokinetics of intravenous midazolam in the basal or induced states. However, during cytochrome P450 (CYP) 3A inhibition by itraconazole, individuals carrying the CYP3A5*1 allele were found to be less susceptible to changes in systemic clearance and showed higher 1′-hydroxymidazolam–to–midazolam area under the plasma concentration–time curve ratios, probably resulting from the relatively CYP3A4-specific inhibition caused by itraconazole. Clinical Pharmacology & Therapeutics (2004) 76, 104–112; doi: 10.1016/j.clpt.2004.03.009

Published

2004

112. Phase I and Pharmacokinetic Study of Genexol-PM, a Cremophor-Free, Polymeric Micelle-Formulated Paclitaxel, in Patients with Advanced Malignancies

Author

Dae Seog Heo, Sung-Chul Kim, Dong Wan Kim, Sang Goo Shin, Yung-Jue Bang, Tae-You Kim, Jae-Yong Chung, and Noe Kyeong Kim

Subjects

Adult, Male, myalgia, Cancer Research, Time Factors, Paclitaxel, Polymers, Phases of clinical research, Antineoplastic Agents, Neutropenia, Pharmacology, Polyethylene Glycols, chemistry.chemical_compound, Pharmacokinetics, Neoplasms, medicine, Humans, Micelles, Taxane, Dose-Response Relationship, Drug, business.industry, Area under the curve, Middle Aged, medicine.disease, Antineoplastic Agents, Phytogenic, Oncology, chemistry, Area Under Curve, Female, Premedication, medicine.symptom, business

Abstract

Purpose: The rationale for developing an alternative paclitaxel formulation concerns Cremophor EL-related side effects, and a novel paclitaxel delivery system might augment its therapeutic efficacy. Genexol-PM is a polymeric micelle formulated paclitaxel free of Cremophor EL. A phase I study was performed to determine the maximum tolerated dosage, dose-limiting toxicities, and the pharmacokinetic profile of Genexol-PM in patients with advanced, refractory malignancies. Experimental Design: Twenty-one patients were entered into the study. Genexol-PM was i.v. administered over 3 h every 3 weeks without premedication. The Genexol-PM dose was escalated from 135 mg/m2 to 390 mg/m2. Results: All of the patients were evaluable for toxicity and response. Acute hypersensitivity reactions were not observed. Neuropathy and myalgia were the most common toxicities. During cycle 1, grade 3 myalgia occurred in 1 patient at 230 and 300 mg/m2, respectively. At 390 mg/m2, 2 of 3 patients developed grade 4 neutropenia or grade 3 polyneuropathy. Therefore, the maximum tolerated dosage was determined to be 390 mg/m2. There were 3 partial responses (14%) among the 21 patients. Of the 3 responders, 2 were refractory to prior taxane therapy. The paclitaxel area under the curve from time 0 to infinity and peak or maximum paclitaxel concentration seemed to increase with escalating dose, except at 230 mg/m2, which suggests that Genexol-PM has linear pharmacokinetics. Conclusion: The main dose-limiting toxicities were neuropathy, myalgia, and neutropenia, and the recommended dosage for a phase II study is 300 mg/m2. Genexol-PM is believed to be superior to conventional paclitaxel in terms of the obviation of premedication and the delivery of higher paclitaxel doses without additional toxicity.

Published

2004

113. Effect of the CYP2D6 genotype on the pharmacokinetics of tropisetron in healthy Korean subjects

Author

Kyun-Seop Bae, Hyeong-Seok Lim, Kyoung-Seop Hong, In-Jin Jang, Dong Ho Lee, Joo Youn Cho, Jae Yong Chung, Myo-Kyoung Kim, Dal-Seok Oh, Sang-Goo Shin, Bumchan Min, and Sanghun Lee

Subjects

Adult, Male, Heterozygote, CYP2D6, medicine.medical_specialty, Indoles, Time Factors, Genotype, Tropisetron, Cmax, digestive system, Asian People, Pharmacokinetics, Internal medicine, medicine, Humans, Pharmacology (medical), Allele, skin and connective tissue diseases, Chromatography, High Pressure Liquid, Pharmacology, Korea, Polymorphism, Genetic, business.industry, Wild type, General Medicine, Endocrinology, Cytochrome P-450 CYP2D6, Area Under Curve, Serotonin Antagonists, business, Pharmacogenetics, Half-Life, medicine.drug

Abstract

To evaluate the effect of the CYP2D6 genotype on the pharmacokinetics of tropisetron in healthy Korean subjects. A single 5-mg capsule of tropisetron was administered orally to 13 healthy subjects. Plasma concentrations were determined by validated HPLC procedures and data were analyzed by using noncompartmental linear PK methods. Four alleles, CYP2D6*1, CYP2D6*2 ×2, CYP2D6*5, and CYP2D6*10, were identified by PCR. Thirteen subjects, consisting of two homozygous carriers of the wild type allele (*1/*1), four heterozygous carriers of poor metabolizer (PM)-associated allele (*1/*10), six homozygous carriers of PM-associated alleles (four with *10/*10 and two with *5/*10), and one carrier of a duplicated allele *1/*2 ×2. All tested pharmacokinetic parameters (AUCinf, AUCinf NL70, Cmax, CmaxNL70, T1/2, and Tec) were significantly different among four different genotypic groups. The mean AUCs of carriers with the heterozygous PM-associated allele and the homozygous PM-associated allele were 1.9- and 6.8-higher than those of carriers with the wild type allele, respectively. In contrast, the mean AUC of carriers with a duplicated allele was 0.5-fold lower than that of those carriers with the wild type allele. The presence of CYP2D6*5, CYP2D6*10, and CYP2D6*2 ×2 has an important impact on the pharmacokinetics of tropisetron, which may influence clinical response to tropisetron therapy.

Published

2003

114. A non-linear pharmacokinetic-pharmacodynamic relationship of metformin in healthy volunteers: An open-label, parallel group, randomized clinical study

Author

Hye Won Chung, Joo Youn Cho, Seo Hyun Yoon, Jae Yong Chung, Kyung Sang Yu, and Jaeseong Oh

Subjects

Blood Glucose, Male, Pharmacogenomic Variants, endocrine system diseases, Physiology, Oral Glucose Suppression Test, lcsh:Medicine, Urine, Pharmacology, 030226 pharmacology & pharmacy, law.invention, 0302 clinical medicine, Randomized controlled trial, law, Blood plasma, Medicine and Health Sciences, 030212 general & internal medicine, lcsh:Science, Glucose tolerance test, Multidisciplinary, medicine.diagnostic_test, Pharmaceutics, Organic Cation Transporter 2, Adjustment of Dosage at Steady State, Healthy Volunteers, Metformin, Body Fluids, Dose–response relationship, Blood, Anatomy, Research Article, medicine.drug, Adult, Drug Administration, Organic Cation Transport Proteins, Models, Biological, Polymorphism, Single Nucleotide, Blood Plasma, Young Adult, 03 medical and health sciences, Dose Prediction Methods, Drug Therapy, Pharmacokinetics, Genetics, medicine, Humans, Hypoglycemic Agents, Dosing, Evolutionary Biology, Dose-Response Relationship, Drug, Population Biology, business.industry, lcsh:R, Biology and Life Sciences, nutritional and metabolic diseases, Glucose Tolerance Test, Pharmacologic-Based Diagnostics, Nonlinear Dynamics, Pharmacodynamics, Genetic Polymorphism, lcsh:Q, business, Population Genetics

Abstract

Background The aim of this study was to explore the pharmacokinetic-pharmacodynamic (PK-PD) relationship of metformin on glucose levels after the administration of 250 mg and 1000 mg of metformin in healthy volunteers. Methods A total of 20 healthy male volunteers were randomized to receive two doses of either a low dose (375 mg followed by 250 mg) or a high dose (1000 mg followed by 1000 mg) of metformin at 12-h intervals. The pharmacodynamics of metformin was assessed using oral glucose tolerance tests before and after metformin administration. The PK parameters after the second dose were evaluated through noncompartmental analyses. Four single nucleotide polymorphisms in MATE1, MATE2-K, and OCT2 were genotyped, and their effects on PK characteristics were additionally evaluated. Results The plasma exposure of metformin increased as the metformin dose increased. The mean values for the area under the concentration-time curve from dosing to 12 hours post-dose (AUC0-12h) were 3160.4 and 8808.2 h·μg/L for the low- and high-dose groups, respectively. Non-linear relationships were found between the glucose-lowering effect and PK parameters with a significant inverse trend at high metformin exposure. The PK parameters were comparable among subjects with the genetic polymorphisms. Conclusions This study showed a non-linear PK-PD relationship on plasma glucose levels after the administration of metformin. The inverse relationship between systemic exposure and the glucose-lowering effect at a high exposure indicates a possible role for the intestines as an action site for metformin. Trial registration ClinicalTrials.gov NCT02712619.

Published

2018

115. Antihyperglycemic mechanism of metformin occurs via the AMPK/LXRα/POMC pathway

Author

In-Jin Jang, Hyun Woo Shin, Jae Yong Chung, Jong Wan Park, Sung Kweon Cho, Joo Youn Cho, Kyung Sang Yu, and K.H. Cho

Subjects

Adult, Blood Glucose, Male, medicine.medical_specialty, Pro-Opiomelanocortin, endocrine system diseases, Hydrocortisone, Metabolite, Type 2 diabetes, Adrenocorticotropic hormone, Biology, AMP-Activated Protein Kinases, Models, Biological, Article, Mass Spectrometry, chemistry.chemical_compound, Young Adult, Adrenocorticotropic Hormone, Internal medicine, Cell Line, Tumor, medicine, Animals, Humans, Hypoglycemic Agents, Metabolomics, Phosphorylation, Protein kinase A, Liver X receptor, Chromatography, High Pressure Liquid, Liver X Receptors, Principal Component Analysis, Multidisciplinary, digestive, oral, and skin physiology, AMPK, nutritional and metabolic diseases, medicine.disease, Orphan Nuclear Receptors, Immunohistochemistry, Metformin, Rats, Endocrinology, chemistry, Gluconeogenesis, medicine.drug, Signal Transduction

Abstract

Metformin is a first-line drug for treating type 2 diabetes. Although metformin is known to phosphorylate AMP-activated protein kinase (AMPK), it is unclear how the glucose-lowering effect of metformin is related to AMPK activation. The aim of this study was to identify the urinary endogenous metabolites affected by metformin and to identify the novel underlying molecular mechanisms related to its anti-diabetic effect. Fourteen healthy male subjects were orally administered metformin (1000 mg) once. First morning urine samples were taken before and after administration to obtain metabolomic data. We then further investigated the anti-diabetic mechanism of metformin in vitro and in vivo. The fluctuation of the metabolite cortisol indicated that the neuroendocrine system was involved in the anti-diabetic effect of metformin. Actually we found that metformin induced AMPK/liver X receptor α (LXRα) phosphorylation, followed by pro-opiomelanocortin (POMC) suppression in rat pituitary cells. We confirmed this result by administering metformin in an animal study. Given that cortisol stimulates gluconeogenesis, we propose the anti-hyperglycemic effect of metformin is attributed to reduced POMC/adrenocorticotropic hormone (ACTH)/cortisol levels following AMPK/LXRα phosphorylation in the pituitaries.

Published

2015

116. EAU recommended preparations (antibiotic prophylaxis and cleansing enema) are important to prevent febrile complications in transrectal ultrasonography guided prostate biopsy

Author

Luck Hee Sung, Jae Yong Chung, Dae Yeon Cho, and J. Yu

Subjects

medicine.medical_specialty, Prostate biopsy, medicine.diagnostic_test, business.industry, Urology, medicine.medical_treatment, medicine, Transrectal ultrasonography, Enema, Antibiotic prophylaxis, business, Surgery

Published

2017

117. Role of the Fc Region in the Vitreous Half-Life of Anti-VEGF Drugs

Author

Kwangsic Joo, Se Joon Woo, Jung Eun Lee, Kyu Hyung Park, Young Mi Na, Ho Min Kim, Jae Yong Chung, Hye Kyoung Hong, Sang Jun Park, and Yewon Choi

Subjects

0301 basic medicine, medicine.medical_specialty, Retina, genetic structures, Fc receptor, Half-life, Biology, Fragment crystallizable region, eye diseases, Vascular endothelial growth factor B, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, Pharmacokinetics, Internal medicine, 030221 ophthalmology & optometry, medicine, biology.protein, sense organs, Choroid, Receptor

Abstract

Purpose To identify the role of the fragment crystallizable (Fc) region in determining intraocular protein drug pharmacokinetics. Methods We generated a new VEGF-Trap lacking the Fc region (FcfVEGF-Trap, MWt = 100 kDa) by replacing the Fc region of native VEGF-Trap (MWt = 145 kDa) with a dimerized coiled-coil domain. Forty-two rabbits were injected intravitreally with VEGF-Trap or FcfVEGF-Trap (n = 21 each) in one of the eyes, harvested at six time points (1 hour and 1, 2, 4, 14, and 30 days after injections). VEGF-Trap and FcfVEGF-Trap concentrations in the vitreous, aqueous humor, and retina/choroid were measured, and drug pharmacokinetic properties were analyzed. Results In all three ocular compartments, the maximal concentrations for both FcfVEGF-Trap and VEGF-Trap were observed at 1 hour after injection. Half-lives of FcfVEGF-Trap in the vitreous and retina/choroid (145.02 and 102.12 hours, respectively) were 1.39 and 2.30 times longer than those of VEGF-Trap (103.99 and 44.42 hours, respectively). Total exposure of the aqueous humor and retina/choroid to FcfVEGF-Trap was 13.2% and 39% of the vitreous exposure, respectively, whereas VEGF-Trap concentrations were 25.2% and 26.2%, indicating that FcfVEGF-Trap shows a preference for posterior distribution and elimination. Conclusions FcfVEGF-Trap, despite its lower molecular weight, showed longer half-lives in vitreous and retina/choroid than VEGF-Trap did, suggesting that Fc receptors in ocular tissues contribute to anti-VEGF drug elimination. Truncation or mutation of the Fc region can prolong the intraocular residence time of VEGF-Trap and possibly reduce the number of VEGF-Trap injections required in clinical practice.

Published

2017

118. Pharmacokinetics and tolerability of the new second-generation nonnucleoside reverse- transcriptase inhibitor KM-023 in healthy subjects

Author

Yu Jung Cha, Min Kyu Park, Brian L. Bray, Stephen E. Schneider, Seo Hyun Yoon, Jae Yong Chung, Myung Chol Kang, Kyung Sang Yu, Joo Youn Cho, and Kyoung Soo Lim

Subjects

Adult, Male, Maximum Tolerated Dose, Pyridones, Cmax, Pharmaceutical Science, Phases of clinical research, Urine, Pharmacology, Biology, Placebo, Imides, Young Adult, Pharmacokinetics, Double-Blind Method, Tandem Mass Spectrometry, Drug Discovery, medicine, Humans, tolerability, Adverse effect, Original Research, Drug Design, Development and Therapy, Reverse-transcriptase inhibitor, Dose-Response Relationship, Drug, KM-023, Middle Aged, Healthy Volunteers, Tolerability, healthy subjects, HIV-1, Reverse Transcriptase Inhibitors, nonnucleoside reverse-transcriptase inhibitor, pharmacokinetics, medicine.drug, Chromatography, Liquid

Abstract

Yu-Jung Cha,1,* Kyoung Soo Lim,2,* Min-Kyu Park,1 Stephen Schneider,3 Brian Bray,3 Myung-Chol Kang,3 Jae-Yong Chung,1 Seo Hyun Yoon,1 Joo-Youn Cho,1 Kyung-Sang Yu11Department of Clinical Pharmacology and Therapeutics, Seoul National University College of Medicine and Hospital, Seoul, South Korea; 2Department of Clinical Pharmacology and Therapeutics, CHA University School of Medicine and CHA Bundang Medical Center, Seongnam, South Korea; 3Kainos Medicine USA Inc., Morrisville, NC, USA *These authors contributed equally to this workBackground: KM-023 is a new second-generation nonnucleoside reverse-transcriptase inhibitor that is under development for the treatment of human immunodeficiency virus (HIV) type 1 infection. Objective: This study determined KM-023 tolerability and pharmacokinetic characteristics in healthy subjects. Materials and methods: A randomized, double-blinded, placebo-controlled, dose-escalation study was conducted in 80 healthy South Korean male volunteers. The subjects were allocated to single- or multiple-dose (once daily for 7 days) groups that received 75, 150, 300, or 600 mg drug or placebo in a 4:1 ratio. Safety and pharmacokinetic assessments were performed during the study. Plasma and urine concentrations were quantified using liquid chromatography–tandem mass spectrometry. Results: The average maximum concentration (Cmax) and area under the concentration–time curve from time 0 to infinity (AUC∞) values of KM-023 for the 75–600 mg doses in the single-dose study ranged from 440.2 ng/mL to 1,245.4 ng/mL and 11,142.4 ng • h/mL to 33,705.6 ng • h/mL, respectively. Values of the mean Cmax at a steady state and AUC within the dosing interval ranged from 385.1 ng/mL to 1,096.7 ng/mL and 3,698.9 ng • h/mL to 10,232.6 ng • h/mL, respectively, following 75–600 mg doses in the multiple-dose study. Dose proportionality was not observed for KM-023. KM-023 showed a 0.6-fold accumulation after multiple doses in the 600 mg dose group. The mean half-life values ranged between 20.7 and 31.2 hours. KM-023 was generally well tolerated without serious adverse events. Conclusion: KM-023 demonstrated dose- and time-dependent nonlinear pharmacokinetic characteristics after single or multiple doses over a dose range (75–600 mg) in healthy subjects. KM-023 showed favorable tolerability in this study. This Phase I clinical trial information can be used to design further clinical studies appropriately to evaluate KM-023 in patients with HIV-1 infection. Keywords: KM-023, HIV-1, nonnucleoside reverse-transcriptase inhibitor, pharmacokinetics, tolerability, healthy subjects

Published

2014

119. Korean, Japanese, and Chinese populations featured similar genes encoding drug-metabolizing enzymes and transporters: a DMET Plus microarray assessment

Author

Kenji Yoshida, In Jin Jang, Joo Youn Cho, Ichiro Ieiri, Howard Lee, Yuichi Sugiyama, Shinichiro Nagatsuka, Kyung-Sang Yu, Masato Fukae, Kyoung Soo Lim, Hyungmi An, Youngjo Lee, Sangin Lee, Dong Wan Shin, Sojeong Yi, Miyuki Kimura, Jae Yong Chung, Takeshi Hirota, and Shin Irie

Subjects

Male, Microarray, Biology, Polymorphism, Single Nucleotide, Asian People, Gene Frequency, Polymorphism (computer science), Genetics, Humans, General Pharmacology, Toxicology and Pharmaceutics, Molecular Biology, Allele frequency, Gene, Genetics (clinical), Oligonucleotide Array Sequence Analysis, chemistry.chemical_classification, Principal Component Analysis, Transporter, Healthy Volunteers, Enzymes, Drug metabolizing enzymes, Enzyme, chemistry, Pharmaceutical Preparations, Pharmacogenetics, Molecular Medicine, Female, Carrier Proteins, Drug metabolism

Abstract

Interethnic differences in genetic polymorphism in genes encoding drug-metabolizing enzymes and transporters are one of the major factors that cause ethnic differences in drug response. This study aimed to investigate genetic polymorphisms in genes involved in drug metabolism, transport, and excretion among Korean, Japanese, and Chinese populations, the three major East Asian ethnic groups.The frequencies of 1936 variants representing 225 genes encoding drug-metabolizing enzymes and transporters were determined from 786 healthy participants (448 Korean, 208 Japanese, and 130 Chinese) using the Affymetrix Drug-Metabolizing Enzymes and Transporters Plus microarray. To compare allele or genotype frequencies in the high-dimensional data among the three East Asian ethnic groups, multiple testing, principal component analysis (PCA), and regularized multinomial logit model through least absolute shrinkage and selection operator were used.On microarray analysis, 1071 of 1936 variants (50% of markers) were found to be monomorphic. In a large number of genetic variants, the fixation index and Pearson's correlation coefficient of minor allele frequencies were less than 0.034 and greater than 0.95, respectively, among the three ethnic groups. PCA identified 47 genetic variants with multiple testing, but was unable to discriminate ethnic groups by the first three components. Multinomial least absolute shrinkage and selection operator analysis identified 269 genetic variants that showed different frequencies among the three ethnic groups. However, none of those variants distinguished between the three ethnic groups during subsequent PCA.Korean, Japanese, and Chinese populations are not pharmacogenetically distant from one another, at least with regard to drug disposition, metabolism, and elimination.

Published

2014

120. Effects of proton pump inhibitors on metformin pharmacokinetics and pharmacodynamics

Author

Kyoung Soo Lim, Anhye Kim, Howard Lee, Jae Yong Chung, Seo Hyun Yoon, In-Jin Jang, Joo Youn Cho, Kyung Sang Yu, and Inbum Chung

Subjects

Blood Glucose, medicine.medical_specialty, endocrine system diseases, Rabeprazole, Cmax, Pharmaceutical Science, Pharmacology, Pharmacokinetics, Internal medicine, medicine, Humans, Hypoglycemic Agents, Drug Interactions, Pantoprazole, Organic cation transport proteins, Cross-Over Studies, biology, business.industry, digestive, oral, and skin physiology, nutritional and metabolic diseases, Proton Pump Inhibitors, Crossover study, Metformin, Endocrinology, Concomitant, Area Under Curve, biology.protein, business, medicine.drug

Abstract

As inhibitors of organic cation transporters (OCTs), proton pump inhibitors (PPIs) may affect the plasma levels of metformin, an OCT substrate. We investigated the effects of two PPIs, pantoprazole and rabeprazole, on metformin pharmacokinetics and glucose levels in healthy subjects. In this open, randomized, six-sequence, three-period crossover study, 24 participants were administered metformin, either alone or in combination with pantoprazole or rabeprazole. The plasma concentrations of metformin and serum concentrations of glucose after a 75-g oral glucose tolerance test (OGTT) were determined. The area under the concentration-time curve (AUC) for metformin was 15% and 16% greater following coadministration with pantoprazole and rabeprazole, respectively. The maximum plasma metformin concentrations (Cmax) also increased by 15% and 22%, respectively, compared with when it was administered without the PPIs. The percentage change in the AUC for glucose concentration versus time for metformin plus rabeprazole was significantly lower than that for metformin plus pantoprazole [geometric mean ratio: 0.96 (90% confidence interval: 0.92-0.99) and 0.77 (0.63-0.93), respectively]. There was no significant difference in the maximum glucose concentration. In conclusion, concomitant administration of PPIs with metformin significantly increased plasma metformin exposure, but the effects on glucose disposition were minor and varied depending on the PPI administered.

Published

2014

121. Eosinophilic myositis in a slaughtered Korean native cattle

Author

Jae-Yong Chung, Jin-Kyu Park, Kyu-Shik Jeong, Hai Jie Yang, Da Hee Jeong, Sun Hee Do, and Dong Wei Yuan

Subjects

Pathology, medicine.medical_specialty, Necrosis, Short Communication, Cattle Diseases, myofiber, Biology, Muscular Diseases, eosinophilic myositis, Eosinophilic, Eosinophilia, medicine, Animals, granuloma, Muscle, Skeletal, Myositis, General Veterinary, Anatomy, Eosinophil, medicine.disease, medicine.anatomical_structure, Korean native cow, Giant cell, Granuloma, Cattle, Female, medicine.symptom, Infiltration (medical)

Abstract

Histopathological findings of eosinophilic myositis in the carcass of a slaughtered Korean native cow are presented. Lesions contained massive fibrous septae with vacuolar changes in some lesions, and the hypercontraction and rupturing of muscle bundles, with replacement by eosinophils. Necrosis and severe eosinophil infiltration were observed. Sarcoplasmic fragmentation and atrophy developed. Typical of granuloma, calcified myofibers were focally surrounded by macrophages and numerous inflammatory cells, and multinucleated giant cell formation was evident.

Published

2008

122. Verapamil decreases the glucose-lowering effect of metformin in healthy volunteers

Author

Sung Kweon, Cho, Choon Ok, Kim, Eun Seok, Park, and Jae-Yong, Chung

Subjects

Adult, Blood Glucose, Male, Organic Cation Transport Proteins, Verapamil, Organic Cation Transporter 1, Humans, Hypoglycemic Agents, Drug Interactions, Metformin

Abstract

The organic cation transporter 1 (OCT1) plays a key role in the cellular transport of metformin and its subsequent glucose-lowering effect. A recent non-clinical study reported that metformin uptake into hepatocytes is regulated via OCT1, and that uptake was strongly inhibited by verapamil. Therefore, we investigated the effects of verapamil co-administration on the pharmacokinetics and pharmacodynamics of metformin in humans.We evaluated the pharmacokinetics and the anti-hyperglycaemic effects of metformin using an oral glucose tolerance test (OGTT) in 12 healthy participants, before (day 1) and after metformin treatment (day 2), and again on days 15 and 16 after co-administration with verapamil.Verapamil inhibited the ability of metformin to reduce maximum blood glucose concentrations (ΔGmax ) by 62.5% (P = 0.008) and decreased the area under the glucose concentration-time curve (ΔAUCgluc ) by 238% (P = 0.015). However, verapamil did not significantly alter the Cmax and the AUC of metformin, nor its renal clearance.Our results suggest that verapamil remarkably decreases the glucose-lowering effect of metformin, possibly by acting as a competitive inhibitor of OCT1.

Published

2014

123. Pharmacokinetics, safety and tolerability of DA-6034, an anti-inflammatory agent, after single and multiple oral administrations in healthy volunteers

Author

Jae Yong Chung, Jung-Ryul Kim, Jieon Lee, In-Jin Jang, Kyoung Soo Lim, and Kwang-Hee Shin

Subjects

Drug, Adult, Male, medicine.drug_class, media_common.quotation_subject, Anti-Inflammatory Agents, Administration, Oral, Pharmacology, Inflammatory bowel disease, Anti-inflammatory, law.invention, Young Adult, Pharmacotherapy, Pharmacokinetics, Randomized controlled trial, Double-Blind Method, law, medicine, Humans, Pharmacology (medical), media_common, Flavonoids, Gastrointestinal tract, Dose-Response Relationship, Drug, business.industry, General Medicine, Middle Aged, medicine.disease, digestive system diseases, Healthy Volunteers, Tolerability, business

Abstract

Inflammatory bowel disease (IBD) is a chronic inflammatory disorder of the gastrointestinal tract. DA-6034 has been shown to be effective in an IBD model and has demonstrated a good toxicological profile in preclinical studies. This study evaluated the tolerability, safety and pharmacokinetics of DA-6034 in healthy volunteers.A double-blind, randomized, placebo-controlled, ascending-dose study was conducted in 67 healthy volunteers. In the single-ascending-dose study, 10, 20, 50, 100 or 200 mg of DA-6034 was administered orally to 40 subjects; in the multiple-ascending-dose study, 40, 100 or 200 mg/day of DA-6034 was administered orally to 27 subjects for 7 days. Serial blood and urine samples were taken for pharmacokinetic analysis. Plasma drug concentrations were determined by high-performance liquid chromatography. Safety and tolerability were assessed throughout the study.DA-6034 had minimal absorption, and the pharmacokinetic parameters were highly variable among subjects. For both the single- and multiple-dose administrations, the coefficients of variation of the area under the plasma concentration-time curve to the last observation (AUClast) and the area under the plasma concentration-time curve over the dosing interval at steady state (AUCss,τ) ranged from 16.0 to 125.0 %. At doses of up to 200 mg of DA-6034, the mean maximum plasma concentration (C max) was3 ng/mL, and the urine recovery ratio was 0.3 % of the dose, indicating a lack of absorption. Twenty-two mild adverse events were reported in 14 subjects. There were no serious adverse events and no significant changes in the safety assessment.DA-6034 was well tolerated and minimally absorbed in healthy volunteers. The non-systemic, local exposure of the gastrointestinal tract to DA-6034 may be advantageous for IBD treatment.

Published

2013

124. SIU/ICUD Consultation On Urethral Strictures: Epidemiology, etiology, anatomy, and nomenclature of urethral stenoses, strictures, and pelvic fracture urethral disruption injuries

Author

Daniel I. Rosenstein, Steven B. Brandes, Jae Yong Chung, Jack W. McAninch, and Jerilyn M. Latini

Subjects

Male, medicine.medical_specialty, Urology, MEDLINE, Constriction, Pathologic, Fractures, Bone, Urethra, Terminology as Topic, Epidemiology, Medicine, Humans, Pelvic Bones, Urethral Stricture, business.industry, Urological Diseases, Evidence-based medicine, Anatomy, medicine.disease, Surgery, Standardized terminology, medicine.anatomical_structure, Etiology, Pelvic fracture, Female, business

Abstract

This committee reviewed and evaluated published data, and recommended standardized terminology relating to the epidemiology, etiology, anatomy, and nomenclature of urethral stenoses, urethral strictures, and pelvic fracture urethral disruption injuries, as well as their surgical management. A literature search using Medline, PubMed (U.S. National Library of Medicine and the National Institutes of Health), Embase, online acronym databases, and abstracts from scientific meetings was performed from 1980-2010. Articles were evaluated using the Levels of Evidence adapted by the International Consultation on Urological Diseases (ICUD) from the Oxford Centre for Evidence-Based Medicine. Recommendations were based on the level of evidence and discussed among the committee to reach a consensus. There is expert opinion to support standards regarding the epidemiology, anatomy, and nomenclature of urethral stenoses, urethral strictures, and pelvic fracture urethral disruption injuries. There is level 3 evidence regarding the epidemiology and etiology of urethral stenoses, urethral strictures, and pelvic fracture urethral injuries. The literature regarding the epidemiology, anatomy, and nomenclature of urethral stenoses, urethral strictures, and pelvic fracture urethral disruption injuries are sparse and generally of a low level of evidence. The proposed ICUD system does not readily apply to these areas. Further research is needed so that stronger levels of evidence can be developed leading to recommendations regarding the accuracy of the data. To improve future research and promote effective scientific progress and communication, a standardized nomenclature and anatomy regarding the urethra and urethral surgery is detailed herein.

Published

2013

125. Sustained Increase in the Oral Bioavailability of Loperamide after a Single Oral Dose of HM30181, a P-glycoprotein Inhibitor, in Healthy Male Participants

Author

Joo Youn Cho, Yu Jung Cha, Kyung Sang Yu, Sang-Goo Shin, Seo Hyun Yoon, In-Jin Jang, Kyoung Soo Lim, Tae Eun Kim, Howard Lee, Jae Yong Chung, and Namyi Gu

Subjects

Adult, Male, Loperamide, Population, Administration, Oral, Biological Availability, Tetrazoles, Pharmacology, Toxicology, Young Adult, Pharmacokinetics, Oral administration, Medicine, Humans, Benzopyrans, ATP Binding Cassette Transporter, Subfamily B, Member 1, education, Adverse effect, education.field_of_study, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Drug Synergism, General Medicine, Middle Aged, Isoquinolines, Crossover study, Bioavailability, Tolerability, business, medicine.drug

Abstract

HM30181 is a new P-glycoprotein (P-gp) inhibitor. This study was conducted to investigate the effect of HM30181 and its duration of action on P-gp inhibition using loperamide as a probe drug. An open-label, five-period, fixed-sequence, cross-over study was conducted in 25 healthy Korean participants, who received a single oral dose of loperamide at 16 mg in five periods lasting for 17 days. In period II, participants also randomly received a single oral dose of HM30181 at 1, 5, 10, 15 mg simultaneously with loperamide. Serial pharmacokinetic blood samples were obtained up to 72 and 336 hr after loperamide and HM30181 administration, respectively. A mixed-effects analysis was performed to compare the area under the plasma concentration versus time curve from time 0 to 72 hr (AUC0-72 hr ) between periods and HM30181 dose groups. Tolerability was also assessed. The AUC0-72 hr of repeatedly administered loperamide was significantly increased 1.18-1.62 times for up to 14 days after a single oral administration of HM30181, particularly at doses ≥10 mg although the between-group difference failed to reach statistical significance. Plasma HM30181 was not detected in many participants including none at any sampling points beyond 48 hr after administration. Most adverse events (AEs) were mild to moderate and resolved spontaneously. The oral bioavailability of loperamide was significantly enhanced by a single oral administration of HM30181, which was sustained for up to 14 days. HM30181 was well tolerated in this selected population.

Published

2013

126. 736 RCC GRADE PREDICTION USING CONTRASTED COMPUTED TOMOGRAPHY

Author

Luck Hee Sung, Ji Hyung Yu, Choong Hee Noh, and Jae Yong Chung

Subjects

medicine.medical_specialty, medicine.diagnostic_test, business.industry, Urology, medicine, Computed tomography, Radiology, Nuclear medicine, business

Published

2013

127. Effect of plasma membrane monoamine transporter genetic variants on pharmacokinetics of metformin in humans.

Author

Seol Ju Moon, Jaeseong Oh, Seung Hwan Lee, Yewon Choi, Kyung-Sang Yu, and Jae-Yong Chung

Subjects

CELL membranes, METFORMIN, PHARMACOKINETICS

Abstract

Metformin, an oral hypoglycemic agent belonging to biguanide class, is widely used to treat type 2 diabetes mellitus, and several drug transporters such as organic cation transporters (OCTs), multidrug and toxin extrusion transporter (MATE), and plasma membrane monoamine transporter (PMAT) are thought to affect its disposition. We evaluated the role of PMAT genetic variations on the pharmacokinetic characteristics of metformin in a Korean population. In this retrospective study, 91 healthy subjects from four different metformin pharmacokinetic studies were analyzed; in each study, the subjects were administered two oral doses of metformin at intervals of 12 hours and dose-normalized pharmacokinetic parameters were compared between the subjects' genotypes. Subjects who had more than one allele of c.883-144A>G single nucleotide polymorphism (SNP) in PMAT gene (rs3889348) showed increased renal clearance of metformin compared to wild-type subjects (814.79 ± 391.73 vs. 619.90 ± 195.43 mL/min, p=0.003), whereas no differences in metformin exposure were observed between the PMAT variant subjects and wild-type subjects. Similarly, subjects with variant rs316019 SNP in OCT2 showed decreased renal clearance of metformin compared to wild-type subjects (586.01 ± 160.54 vs. 699.13 ± 291.40 mL/min, p=0.048). Other SNPs in PMAT and MATE1/2-K genes did not significantly affect metformin pharmacokinetics. In conclusion, the genetic variation of c.883-144A>G SNP in PMAT significantly affects the renal clearance of metformin in healthy Korean male subjects. [ABSTRACT FROM AUTHOR]

Published

2018

128. A post hoc analysis of intra-subject coefficients of variation in pharmacokinetic measures to calculate optimal sample sizes for bioequivalence studies

Author

Seung-Hwan Lee, Youngjo Lee, Inbum Chung, Jaeseong Oh, Jae Yong Chung, and In-Jin Jang

Subjects

bioequivalence, Coefficient of variation, Cmax, Bioequivalence, 030226 pharmacology & pharmacy, Crossover study, sample size, coefficient of variation, power, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Sample size determination, 030220 oncology & carcinogenesis, Retraction and Republication, Post-hoc analysis, Statistics, Original Article, Pharmacology (medical), Christian ministry, generic drugs, Mathematics

Abstract

Because bioequivalence studies are performed using a crossover design, information on the intra-subject coefficient of variation (intra-CV) for pharmacokinetic measures is needed when determining the sample size. However, calculated intra-CVs based on bioequivalence results of identical generic drugs produce different estimates. In this study, we collected bioequivalence results using public resources from the Ministry of Food and Drug Safety (MFDS) and calculated the intra-CVs of various generics. For the generics with multiple bioequivalence results, pooled intra-CVs were calculated. The estimated intra-CVs of 142 bioequivalence studies were 14.7±8.2% for AUC and 21.7±8.8% for Cmax. Intra-CVs of Cmax were larger than those of area under the concentration-time curve (AUC) in 129 studies (90.8%). For the 26 generics with multiple bioequivalence results, the coefficients of variation of intra-CVs between identical generics (mean±sd (min ~ max)) were 38.0±24.4% (1.9 ~ 105.3%) for AUC and 27.9±18.2% (4.0 ~ 70.1%) for Cmax. These results suggest that substantial variation exists among the bioequivalence results of identical generics. In this study, we presented the intra-CVs of various generics with their pooled intra-CVs. The estimated intra-CVs calculated in this study will provide useful information for planning future bioequivalence studies. (This is republication of the article 'Transl Clin Pharmacol 2017;25:179-182' retracted from critical typographic errors. See the 'Retraction and Republication section of this issue for further information).

Published

2017

129. Fetal Bladder Outlet Obstruction in a Stillborn Bovine Fetus

Author

Mi-Young An, Jae-Yong Chung, Cha-Soo Lee, Bruce H. Williams, Da-Hee Jeong, Sang-Joon Park, Kyu-Shik Jeong, Won-Il Jeong, Dong-Hyung Noh, and Sun Hee Do

Subjects

Male, Urinary Bladder, Hydronephrosis, Abdominal wall, Bladder outlet obstruction, Fetus, Meconium, Animals, Medicine, Abnormalities, Multiple, Fetal Death, reproductive and urinary physiology, Arthrogryposis, Korea, General Veterinary, business.industry, Megacystis, Anatomy, medicine.disease, Anus, female genital diseases and pregnancy complications, Urinary Bladder Neck Obstruction, Fetal Diseases, medicine.anatomical_structure, Cattle, medicine.symptom, business

Abstract

A stillborn bovine male fetus with abdominal distention, arthrogryposis and atresia ani was presented for diagnostic evaluation. At necropsy, this fetus had a large amount of ascites, urachal obstruction and marked bladder distention. The ventral surface of the bladder had ruptured and attached to the abdominal wall by fibrinous adhesions. There was bilateral hydronephrosis with moderate pelvic dilatation and cortical attenuation. The rectum was filled with meconium but the anus was imperforate. The right forelimb was contracted. The cause(s) of these abnormalities could not be determined; however, we believe that developmental abnormalities during embryogenesis may be the result of chromosomal abnormalities.

Published

2003

130. Modeling of the LDL cholesterol-lowering effect of atorvastatin in Korean dyslipidemic patients and non-patient volunteers

Author

Sang Hak Lee, Min Soo Park, Jae Yong Chung, Kyungsoo Park, and Eun Sil Oh

Subjects

Adult, Male, medicine.medical_specialty, Atorvastatin, Population, Down-Regulation, Gastroenterology, Models, Biological, Drug Administration Schedule, law.invention, Decision Support Techniques, chemistry.chemical_compound, Young Adult, Randomized controlled trial, Asian People, law, Internal medicine, Republic of Korea, medicine, Humans, Pharmacology (medical), Computer Simulation, Drug Dosage Calculations, Pyrroles, education, Dyslipidemias, Pharmacology, Ldl cholesterol, education.field_of_study, business.industry, Cholesterol, Cholesterol, LDL, Middle Aged, Treatment period, NONMEM, Treatment Outcome, chemistry, Heptanoic Acids, Pharmacodynamics, lipids (amino acids, peptides, and proteins), Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, Biomarkers, medicine.drug

Abstract

Objective The aim of this study was to develop a longitudinal pharmacodynamic model describing the time-courses of low-density lipoprotein cholesterol (LDL) profiles during and after atorvastatin treatment in Korean dyslipidemic patients and non-patient volunteers. Methods 15 dyslipidemic patients and 11 non-patient volunteers with no prior therapy participated in a parallel, 2-step dose escalation study. Subjects received atorvastatin doses ranging from 10 to 80 mg for 42 days (dyslipidemic patients) or 10 mg for 21 days (non-patient volunteers). Plasma samples were collected before and during the treatment period and up to 2 weeks after the last administration. A population pharmacodynamic model was built using the NONMEM software package. An indirect response model consisting of production in hepatocyte and elimination from plasma stimulated by atorvastatin described the LDL time-course. Results The typical population value of the estimated dose producing 50% of maximal stimulation on LDL elimination (SD50) for dyslipidemic patients was 11.9 mg, which was about 6 times higher than that of non-patient volunteers (2.0 mg). Conclusion A longitudinal population pharmacodynamic model for the LDL-lowering effect of atorvastatin in both dyslipidemic patients and non-patient volunteers was developed. This could help guide optimal therapies according to the target population.

Published

2012

131. Serum cystatin C is a major predictor of vancomycin clearance in a population pharmacokinetic analysis of patients with normal serum creatinine concentrations

Author

Ji Hyun Yoon, Young Goo Song, Jae Yong Chung, and Sung Joon Jin

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Population, TDM, chemistry.chemical_compound, Young Adult, Sex Factors, Pharmacokinetics, Serum cystatin, Vancomycin, Internal medicine, medicine, Humans, Cystatin C, education, NONMEM, Aged, Demography, Volume of distribution, Aged, 80 and over, education.field_of_study, Creatinine, Models, Statistical, biology, business.industry, Body Weight, Age Factors, General Medicine, Middle Aged, Infectious Diseases, Microbiology & Parasitology, Anti-Bacterial Agents, Endocrinology, chemistry, biology.protein, Female, Original Article, business, Biomarkers, Software, medicine.drug

Abstract

We developed a population pharmacokinetic model of vancomycin by integrating the effects of cystatin C and other demographic factors in a large population of Korean patients with normal serum creatinine concentrations to elucidate the precise role of serum cystatin C concentrations in the prediction of vancomycin clearance. A population pharmacokinetic model of vancomycin was developed using NONMEM software from a total of 1,373 vancomycin concentration measurements in 678 patients whose serum creatinine concentrations were lower than 1.2 mg/dL. Covariate selection revealed that cystatin C was the most influential factor and had negative influence ((-0.78)) in the relationship. Total body weight, sex, age, and serum creatinine were also significantly correlated with the clearance. The estimated intersubject variabilities of clearance and volume of distribution were 24.7% and 25.1%, respectively. A 14-fold difference in predicted trough concentrations was observed according to only cystatin C concentrations in a population of simulated individuals with median demographic characteristics. The use of serum cystatin C as marker of vancomycin clearance for more accurate predictions of serum vancomycin concentrations could be useful, particularly among patients with normal serum creatinine concentrations.

Published

2012

132. Pharmacokinetic comparison of sustained- and immediate-release oral formulations of cilostazol in healthy Korean subjects: a randomized, open-label, 3-part, sequential, 2-period, crossover, single-dose, food-effect, and multiple-dose study

Author

Jin Woo Park, Kiyoon Kim, Yoon Jung Lee, Min Soo Park, Seong Bok Jang, Donghwan Lee, Lay Ahyoung Lim, Jae Yong Lee, Hosang Yoon, Jae Yong Chung, Kyungsoo Park, and Jong Rak Choi

Subjects

Adult, Male, Metabolic Clearance Rate, Chemistry, Pharmaceutical, Administration, Oral, Tetrazoles, Bioequivalence, Pharmacology, Models, Biological, law.invention, Food-Drug Interactions, Young Adult, Randomized controlled trial, Pharmacokinetics, Asian People, law, Republic of Korea, Medicine, Humans, Pharmacology (medical), Adverse effect, FOOD EFFECT, Cross-Over Studies, business.industry, Cardiovascular Agents, Middle Aged, Crossover study, Cilostazol, Bioavailability, Therapeutic Equivalency, Area Under Curve, Delayed-Action Preparations, Female, business, medicine.drug

Abstract

A sustained-release (SR) formulation of cilostazol was recently developed in Korea and was expected to yield a lower C(max) and a similar AUC to the immediate-release (IR) formulation.The goal of the present study was to compare the pharmacokinetic profiles of a newly developed SR formulation and an IR formulation of cilostazol after single- and multiple-dose administration and to evaluate the influence of food in healthy Korean subjects. This study was developed as part of a product development project at the request of the Korean regulatory agency.This was a randomized, 3-part, sequential, open-label, 2-period crossover study. Each part consisted of different subjects between the ages of 19 and 55 years. In part 1, each subject received a single dose of SR (200 mg × 1 tablet, once daily) and IR (100 mg × 2 tablets, BID) formulations of cilostazol orally 7 days apart in a fasted state. In part 2, each subject received a single dose of the SR (200 mg × 1 tablet, once daily) formulation of cilostazol 7 days apart in a fasted and a fed state. In part 3, each subject received multiple doses of the 2 formulations for 8 consecutive days 21 days apart. Blood samples were taken for 72 hours after the dose. Cilostazol pharmacokinetics were determined for both the parent drug and its metabolites (OPC-13015 and OPC-13213). Adverse events were evaluated through interviews and physical examinations.Among the 92 enrolled subjects (66 men, 26 women; part 1, n = 26; part 2, n = 26; part 3, n = 40), 87 completed the study. In part 1, all the primary pharmacokinetic parameters satisfied the criterion for assumed bioequivalence both in cilostazol and its metabolites, yielding 90% CI ratios of 0.9624 to 1.2323, 0.8873 to 1.1208, and 0.8919 to 1.1283 for C(max) and 0.8370 to 1.0134, 0.8204 to 0.9807, and 0.8134 to 0.9699 for AUC(0-last) of cilostazol, OPC-13015, and OPC-13213, respectively. In part 2, food intake increased C(max) and AUC significantly (P0.0001), yielding geometric mean ratios of 3.2879, 2.9894, and 3.0592 for C(max) and 1.7001, 1.7689, and 1.6976 for AUC(0-last) of cilostazol, OPC-13015, and OPC-13213. In part 3, only the C(ssmax) of clilostazol in the reference formulation did not satisfy the criterion for assumed bioequivalence, yielding 90% CI ratios of 1.2693 to 1.4238 and 1.2038 to 1.3441, respectively. When each dose was normalized, the C(max) for the SR formulation was significantly lower (P0.005 for cilostazol). Headache was the most frequently noted adverse effect (part 1, a total of 14 subjects with the IR formulation and 14 with the SR formulation; part 2, a total of 10 without food and 23 with a high-fat meal; part 3, a total of 10 with the IR formulation and 24 with the SR formulation), followed by nausea (part 1, none; part 2, only 1 without food and 3 with a high-fat meal; part 3, a total of 3 with the IR formulation and 3 with the SR formulation), and then dizziness (parts 1 and 2, none; part 3, a total of 4 with the IR formulation and 5 with the SR formulation). All other AEs, including fever, cough, vomiting, palpitation, diarrhea, and epigastric pain, occurred in3 subjects.These findings suggest that in this select group of healthy Korean volunteers, the SR formulation of cilostazol was not significantly different in AUC compared with that of the IR formulation, although it did display a significantly lower C(max) per dose in both the single- and multiple-dose groups. Food significantly increased the bioavailability of the SR formulation. The cilostazol SR and IR formulations were well tolerated in all parts of the study, with no serious adverse events reported. ClinicalTrials.gov identifier: NCT01455558.

Published

2011

133. 1572 RENAL FUNCTION IS ONE OF THE PREDICTIVE FACTORS FOR STONE-FREE RATE AFTER SWL IN PROXIMAL URETERAL CALCULI

Author

Ji Hyeong Yu, Choong Hee Noh, Luck Hee Sung, June Hyun Han, Jae Yong Chung, and Yong Il Park

Subjects

medicine.medical_specialty, business.industry, Urology, Stone free, medicine, Renal function, business

Published

2010

134. 801 PROSTATE VOLUME AND PROSTATITIS: EFFECTS ON LOWER URINARY TRACT SYMPTOMS

Author

Luck Hee Sung, Choong Hee Noh, Ji Hyeong Yu, C one Cho, and Jae Yong Chung

Subjects

medicine.medical_specialty, Neck of urinary bladder, medicine.anatomical_structure, business.industry, Lower urinary tract symptoms, Prostate, Urology, Medicine, Prostatitis, business, medicine.disease, Volume (compression)

Published

2010

135. Effect of CYP2B6 genotype on the pharmacokinetics of sibutramine and active metabolites in healthy subjects

Author

Jae Yong Chung, Min Soo Park, Kyungsoo Park, Seong Bok Jang, and Yoon Jung Lee

Subjects

Adult, Male, CYP2B6, Genotype, Metabolite, Administration, Oral, Pharmacology, chemistry.chemical_compound, Young Adult, Pharmacokinetics, Appetite Depressants, Medicine, Humans, Pharmacology (medical), Dosing, Active metabolite, Alleles, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Oxidoreductases, N-Demethylating, Cytochrome P-450 CYP2B6, chemistry, Area Under Curve, Female, Aryl Hydrocarbon Hydroxylases, business, Drug metabolism, Pharmacogenetics, Cyclobutanes, Sibutramine, medicine.drug, Half-Life

Abstract

Sibutramine is a pharmacologic intervention for the treatment of obesity. The effect of CYP2B6 genotypes on the pharmacokinetics of sibutramine and its active metabolites (desmethylsibutramine [M1] and didesmethylsibutramine [M2]) was evaluated in 57 healthy subjects. Each subject received a single oral dose of 10 or 15 mg sibutramine, and blood samples were collected up to 72 hours after dosing. The relationship between the genotypes and the pharmacokinetics of sibutramine, M1, and M2 was examined. A statistically significant difference in the elimination half-life (t 1/2 ) of sibutramine M1 was found among the 3 genotype groups (P = .0006), between the *1/*1 and * 1/ * 6 groups (P = .0001), and between the *1/*4 and *1/*6 groups (P = .012). The mean value of M1 t 1/2 in *1/*6 (33.3 ± 10.5 hours) was about 58% and 61% greater than that of the *1/*1 group (21.0 ± 7.4 hours) and the *1/*4 group (20.7 ± 9.8 hours), respectively. No significant differences in area under the concentration-time curve or maximum plasma drug concentration were observed between thegroups. The CYP2B6* 6 allele may be associated with a lower metabolic clearance of the M1 metabolite of sibutramine in human subjects.

Published

2010

136. Bone-protecting effect of Rubus coreanus by dual regulation of osteoblasts and osteoclasts

Author

Sun Hee Do, Ji-Won Lee, Sang-Kyung Jeon, Il-Hwa Hong, In-Seon Lee, Jae-Yong Chung, Kyu-Shik Jeong, Sang-Joon Park, and Wong-Il Jeong

Subjects

medicine.medical_specialty, medicine.drug_class, Ovariectomy, Osteoporosis, Osteoclasts, Apoptosis, Bone remodeling, Osteoclast, In vivo, Internal medicine, medicine, Animals, Humans, Femur, Bone Resorption, Rats, Wistar, Rosaceae, Osteoporosis, Postmenopausal, Osteoblasts, Bone Density Conservation Agents, Dose-Response Relationship, Drug, business.industry, Caspase 3, Plant Extracts, Obstetrics and Gynecology, Osteoblast, Cell Differentiation, medicine.disease, Alkaline Phosphatase, Rats, Dose–response relationship, Endocrinology, medicine.anatomical_structure, Estrogen, Fruit, Ovariectomized rat, Female, business, Phytotherapy

Abstract

Objective Bone loss occurs with increasing age and/or as a secondary occurrence to chronic metabolic disease. Certain nutritional and pharmacological, as well as nonpharmacologic interventions such as weight-bearing exercise and muscle strengthening help prevent bone loss. We examined the effect of the methanol extract from the fruit of Rubus coreanus (RCM) on postmenopausal osteoporosis. Design Ovariectomized rats were assigned to sham (negative control), vehicle control, positive control, safflower seed 200 mg/kg, RCM 100 mg/kg (RCM 100), RCM 200 mg/kg (RCM 200), and RCM 400 mg/kg (RCM 400) groups for 10 weeks after the operation. Serum biochemistry, histochemistry, immunohistochemistry, and other related biomarkers of bone metabolism were investigated. Results We observed that RCM could prevent bone loss by increasing the femur trabecular bone area in a dose-dependent manner in ovariectomized rats. The mineral composition of RCM contains many more valuable elements, especially potassium, magnesium, and vitamins D and B2, than safflower seed. The effect of RCM increased not only osteoblast differentiation but also osteoclast apoptosis. In addition, the extract of RCM contained in quercetin suggests that the extract of RCM resulted in improved aging-related bone loss through an antioxidant effect. Conclusions The present data provide the first direct in vivo evidence that RCM has a bone-protecting effect caused by estrogen deficiency, without undesirable side effects on the uterus and other solid organs. The beneficial effect of RCM may be mediated, at least in part, by dual regulation of the enhancement of osteoblast function and induction of osteoclast apoptosis.

Published

2008

137. Erratum: Pharmacokinetics and bioequivalence of two different 20 mg olmesartan tablets: A randomized, single-dose, two-period crossover study in healthy Korean male volunteers

Author

Jieon Lee, AnHye Kim, Kyung-Sang Yu, Jae-Yong Chung, Sung-Vin Yim, and Bo-Hyung Kim

Subjects

Pharmacology (medical)

Published

2016

138. Evaluation of factors associated with drug-induced liver injury using electronic medical records

Author

Kyung Sang Yu, Jaeseong Oh, Jieon Lee, Jae Yong Chung, Hyungmi An, and Hye Won Chung

Subjects

Drug, Clinical pharmacology, business.industry, Medical record, media_common.quotation_subject, medicine.disease, humanities, eye diseases, law.invention, law, Medicine, Pharmacology (medical), Medical emergency, business, media_common

Abstract

Hyewon Chung, Hyungmi An, Jieon Lee, Jaeseong Oh, Kyung-Sang Yu and Jae-Yong Chung* Department of Clinical Pharmacology and Therapeutics, Seoul National University College of Medicine and Hospital, Seoul 03080, Korea, Department of Clinical Pharmacology and Therapeutics, Seoul National University College of Medicine and Bundang Hospital, Seongnam 13620, Korea *Correspondence: J. Y. Chung; Tel: +82-31-787-3955, Fax: +82-31-787-4045, E-mail: jychung@snubh.org These authors have contributed equally to the work.

Published

2016

139. Pharmacokinetic and pharmacodynamic interaction of lorazepam and valproic acid in relation to UGT2B7 genetic polymorphism in healthy subjects

Author

Sang-Goo Shin, Jae Yong Chung, Jung-Ryul Kim, Kyung Sang Yu, Dong-Ryul Sohn, Kyoung-Soo Lim, In Jin Jang, and Joo Youn Cho

Subjects

Adult, Male, Psychometrics, medicine.drug_class, medicine.medical_treatment, Pharmacology, Lorazepam, Hypnotic, Pharmacokinetics, Genotype, medicine, Humans, Pharmacology (medical), Glucuronosyltransferase, Valproic Acid, Polymorphism, Genetic, business.industry, Anticonvulsant, Sedative, Pharmacodynamics, Area Under Curve, Anticonvulsants, Female, business, Psychomotor Performance, medicine.drug

Abstract

Pharmacokinetic and pharmacodynamic profiles of lorazepam and valproate were analyzed according to uridine 5'-diphosphate-glucuronosyltransferase (UGT)2B7 genotype in 14 healthy subjects with UGT2B15*2/*2 genotype. Systemic clearance of lorazepam (2 mg intravenously) and area under the concentration-time curve (AUC) of valproate (600 mg once daily for 4 days) were analyzed as pharmacokinetic parameters, and area under the effect-time curve (AUEC) of psychomotor coordination tests (Vienna) was used for pharmacodynamic parameter. No significant differences were found in systemic clearances of lorazepam by UGT2B7 genotype. AUCs of valproate showed an increasing tendency as the number of UGT2B7*2 alleles increased, but the difference was insignificant. Psychometric results were significant among the UGT2B7 genotype group (AUEC_tracking 261.5+/-298.9 in *1/*1, and 3,396.8+/-947 in *2/*2, P=0.047) when the two drugs were coadministered. Our study suggests that the UGT2B7 genotype probably affects lorazepam-valproate pharmacodynamic interaction, especially in subjects who have homovariant genotypes of UGT2B7 and UGT2B15, although the effects on the pharmacokinetics are less significant.

Published

2007

140. Discovery of URAT1 SNPs and association between serum uric acid levels and URAT1

Author

Jae Yong Chung, Sung Kweon Cho, Soriul Kim, and Sun Ha Jee

Subjects

Adult, Male, Candidate gene, medicine.medical_specialty, Genotype, Organic Cation Transport Proteins, GENETICS, Organic Anion Transporters, Single-nucleotide polymorphism, Hyperuricemia, Bioinformatics, Polymorphism, Single Nucleotide, Young Adult, chemistry.chemical_compound, Asian People, CLINICAL PHARMACOLOGY, Internal medicine, Republic of Korea, Odds Ratio, medicine, Humans, Genetic Predisposition to Disease, Alleles, biology, business.industry, Research, Case-control study, nutritional and metabolic diseases, General Medicine, medicine.disease, Pharmacology and Therapeutics, Uric Acid, Phenotype, Endocrinology, chemistry, Case-Control Studies, Mutation, biology.protein, Uric acid, SLC22A12, Metabolic syndrome, business, Body mass index

Abstract

Objectives Human urate transporter 1 (URAT1) is a member of the organic anion transporter family (SLC22A12) that primarily regulates the renal tubular reabsorption of uric acid. This case–control study was designed to analyse whether hURAT1 might also be a candidate gene for hyperuricaemia or hypouricaemia. Setting We recruited 68 healthy volunteers and divided them into two groups: a normal uric acid group and a hyperuricaemia group. We analysed the sequence of the URAT1 gene and found five significant single nucleotide polymorphisms (SNPs). We then selected 900 male subjects from the 262 200 enrolled in the Korean Cancer Prevention Study-II (KCPS-II) cohort for further genetic analysis. Participants DNA samples from 36 individuals with normal uric acid (8.5 mg/dL) were sequenced. Five significant SNPs (rs7929627, rs75786299, rs3825017, rs11602903 and rs121907892) were identified. We then chose 900 subjects from the KCPS-II cohort consisting of 450 subjects with normal uric acid (UA 8.7 mg/dL). The groups were matched by age, body mass index, metabolic syndrome and use of anti-hypertensive medication. Primary outcome measures We compared the OR of the incidence of hyperuricaemia by URAT1 genotype. Results The strongest association with hyperuricaemia was observed for rs75786299 (IVS3+11A/G) with an OR of 32.05. rs7929627 (IVS7-103A/G) and rs3825017 (N82N) showed an association with hyperuricaemia with ORs of 2.56 and 2.29, respectively. rs11602903 (788A/T) and rs121907892 (W258X) were negatively correlated with hyperuricaemia with ORs of 0.350 and 0.447, respectively. Individuals carrying the GATAG haplotype (n=32)—a relatively common variant consisting of rs7929627, rs75786299 and rs3825017—showed the highest risk for hyperuricaemia with an OR of 92.23 (p=9.55×10−3). Conclusions These results indicate that five newly described SNPs in the hURAT1 gene are significantly associated with uric acid level (4-2008-0318 and 4-2011-0277).

Published

2015

141. Joint bio-equivalence tests with multivariate Gaussian random effects

Author

Kyung Sang Yu, Jae Yong Chung, H. An, and In-Jin Jang

Subjects

Pharmacology, Multivariate statistics, Multivariate analysis, business.industry, BIO-EQUIVALENCE, Multivariate normal distribution, Random effects model, symbols.namesake, Statistics, symbols, Medicine, Pharmacology (medical), Multivariate t-distribution, business, Joint (geology), Gaussian process

Published

2015

142. Effects of bio-active ceramic resources in cutaneous wound healing and the role of TGF-beta signaling

Author

Soon-Bok Kim, Myung-Sook Choi, Sun Hee Do, Mi-Ran Ki, Kyu-Shik Jeong, Jae-Yong Chung, Da-Hee Jeong, Won-Il Jeong, Sang-Joon Park, and Dongmi Kwak

Subjects

Male, medicine.medical_specialty, Ceramics, Clinical Biochemistry, Inflammation, SMAD, Smad2 Protein, Pharmacology, Epithelium, Ointments, Rats, Sprague-Dawley, Tgf β signaling, Transforming Growth Factor beta, medicine, Animals, Ceramic, Smad3 Protein, Molecular Biology, Skin, Wound Healing, integumentary system, Chemistry, Granulation tissue, Cell Biology, General Medicine, Phosphoproteins, Immunohistochemistry, Surgery, Rats, medicine.anatomical_structure, visual_art, visual_art.visual_art_medium, medicine.symptom, Cutaneous wound, Signal transduction, Wound healing, Signal Transduction

Abstract

The wound healing process is a highly orchestrated process, which includes inflammation, re-epithelialization, granulation tissue formation, matrix formation and re-modeling. In this paper, we attempt to determine if bio-active ceramic resource powder particles had an effect on cutaneous wound healing. Furthermore, we investigated its related mechanism and the expression of Smads of cutaneous wound healing, which can be accelerated by bio-active ceramic ointment. Topically applied lesions of 5%, 10% and 15% bio-active ceramic ointment (AO) showed accelerated wound closure, re-epithelialization, and the related immediate down stream of TGF-beta (p-Smad2/3 and Smad3) was suppressed. In particular, 10% and 15% AO lesions became closed faster at Days 3 and 4 of post-wound and p-Smad2/3 was also suppressed. All AO lesions showed accelerated mild wound closure at Day 6, but there were no significant difference. Several papers reported that Smad3 may mediate the signaling pathways that is inhibitory to wound healing, as the deletion of Smad3 leads to enhanced re-epithelialization and contraction of the wound area. This study showed that topical, bio-active ceramic ointment applications accelerated wound closure, re-epithelialization and the suppression of Smad proteins (p-Smad2/3, Smad3). The data revealed that the suppression of Smad3, which was induced by bio-active ceramic resources powder particles affected re-epithelialization and cutaneous wound closure. At the end of this paper, we concluded that bio-active ceramic resources affect cutaneous wound healing by accelerating the re-epithelialization of keratinocytes and that is mediated by the suppression of related protein, Smad3.

Published

2006

143. Up-regulation of Metabotropic glutamate receptor 3 (mGluR3) in rat fibrosis and cirrhosis model of persistent hypoxic condition

Author

Soon-Bok Kim, Mi-Ran Ki, Sun Hee Do, Kyu-Shik Jeong, Da-Hee Jeong, Won-Il Jeong, Hae-Sun Yun, Sang-Joon Park, and Jae-Yong Chung

Subjects

Male, medicine.medical_specialty, Clinical Biochemistry, Biology, Liver Cirrhosis, Experimental, Receptors, Metabotropic Glutamate, Neuroprotection, Glutamatergic, Internal medicine, medicine, Animals, Rats, Wistar, Receptor, Hypoxia, Molecular Biology, Carbon Tetrachloride, Glutamate receptor, Cell Biology, General Medicine, Fibrosis, Immunohistochemistry, Rats, Up-Regulation, Disease Models, Animal, Endocrinology, Metabotropic glutamate receptor, Metabotropic glutamate receptor 3, Signal transduction, Metabotropic glutamate receptor 2

Abstract

Glutamate is the major excitatory neurotransmitter in the central nervous system, and evidence for peripheral glutamatergic fibers in mammals is still lacking. However, glutamate receptors have been identified in peripheral organs, including taste buds, myenteric plexus, and pancreatic islet cell. Protection against anoxic damage could also be explained by mechanisms mediated by postsynaptic mGluR2 or mGluR3, such as the inhibition of membrane excitability resulting from a reduction of cAMP formation by a G-protein-dependent modulation of ion channels. In addition, activation of mGluR3 present in glial cells may contribute to neuroprotection by enhancing the production of death. Thus, mGluR2/3 behaves potentially as a major defensive mechanism anoxia-tolerant species. There are a few reports for the regional pattern of hypoxic damage, which was inversely related to the expression of mGluR2/3. The aim of this study was to characterize the expression of mGluR3 in hypoxic liver in experimental model of rat liver. Proteomic analysis of protein extracts from CCl4–induced cirrhotic liver revealed the presence of the mGluR3. The presence of mGluR3 in the cirrhotic liver was confirmed by immunohistochemical analysis. There were a number of macrophages expressing mGluR3 mainly in the fibrous septa. After 2 weeks recovery, however, most of mGluR3 positive macrophages disappeared with collagen fibers. These results demonstrate that mGluR3 involved in the liver in response to persistent hypoxic status such as fibrotic/cirrhotic condition, and suggest that the expression of mGluR3 may be a key role functional metabolism and viability in the liver by interacting with the glutamate receptors in vivo.

Published

2006

144. Safety, tolerability and pharmacokinetics of 21 day multiple oral administration of a new oxazolidinone antibiotic, LCB01-0371, in healthy male subjects.

Author

Yewon Choi, Sang Won Lee, Anhye Kim, Kyungho Jang, Heesook Nam, Young Lag Cho, Kyung-Sang Yu, In-Jin Jang, Jae-Yong Chung, Choi, Yewon, Lee, Sang Won, Kim, Anhye, Jang, Kyungho, Nam, Heesook, Cho, Young Lag, Yu, Kyung-Sang, Jang, In-Jin, and Chung, Jae-Yong

Subjects

GRAM-positive bacterial infections, OXAZOLIDINONES, PHARMACOKINETICS, DRUG tolerance, ORAL medication, HEMATOLOGY, BACTERIAL disease treatment, THERAPEUTICS, ERYTHROCYTES, ANTIBIOTICS, COMPARATIVE studies, GRAM-positive bacteria, HETEROCYCLIC compounds, RESEARCH methodology, MEDICAL cooperation, ORAL drug administration, RESEARCH, EVALUATION research, RANDOMIZED controlled trials, HUMAN research subjects, BLIND experiment, PHARMACODYNAMICS

Abstract

Background: LCB01-0371 is a new oxazolidinone antibiotic, which targets most Gram-positive organisms. High rates of adverse reactions including myelosuppression have been reported for existing oxazolidinones, limiting their long-term use.Objectives: The safety, tolerability and pharmacokinetics (PK) of 21 day multiple oral administrations of LCB01-0371 in healthy male subjects (clinicaltrials.gov: NCT02540460) were investigated.Methods: In this randomized, double-blind, placebo-controlled study, subjects received 800 mg of LCB01-0371 once or twice daily or 1200 mg of LCB01-0371 twice-daily for 21 days in a fasting state. Safety and tolerability profiles including laboratory tests were evaluated during the study and on a post-study visit and the results were analysed using repeated-measures analysis of variance (RM-ANOVA). Serial blood samples for PK analysis were collected up to 12 h after dosing on day 21.Results: A total of 40 subjects were enrolled and 34 subjects completed the study. Two subjects dropped out according to stopping rules. In the 1200 mg twice-daily dose group, the absolute value of red blood cell count, haematocrit and haemoglobin decreased by 500 × 106/L (6.5%), 4.5% (6.8%) and 1.6 g/dL (6.9%), respectively, after 21 day administrations of LCB01-0371. However, mean relative changes from baseline of all haematology values were not significantly different among doses, including placebo (all, P < 0.05). PK profiles of LCB01-0371 in the dose range of 800 mg once daily to 1200 mg twice daily were consistent with previous studies.Conclusions: LCB01-0371 is well tolerated in healthy male subjects with comparable haematology profiles to placebo, after multiple doses of up to 1200 mg twice daily for 21 days. [ABSTRACT FROM AUTHOR]

Published

2018

145. A post hoc analysis of intra-subject coefficients of variation in pharmacokinetic measures to calculate optimal sample sizes for bioequivalence studies.

Author

Inbum Chung, Jaeseong Oh, SeungHwan Lee, In-Jin Jang, Youngjo Lee, and Jae-Yong Chung

Subjects

PHARMACOKINETICS, THERAPEUTIC equivalency in drugs, DRUG design

Abstract

Because bioequivalence studies are performed using a crossover design, information on the intrasubject coefficient of variation (intra-CV) for pharmacokinetic measures is needed when determining the sample size. However, calculated intra-CVs based on bioequivalence results of identical generic drugs produce different estimates. In this study, we collected bioequivalence results using public resources from the Ministry of Food and Drug Safety (MFDS) and calculated the intra-CVs of various generics. For the generics with multiple bioequivalence results, pooled intra-CVs were calculated. The estimated intra-CVs of 142 bioequivalence studies were 14.7±8.2% for AUC and 21.7±8.8% for Cmax. Intra-CVs of Cmax were larger than those of area under the concentrationtime curve (AUC) in 129 studies (90.8%). For the 26 generics with multiple bioequivalence results, the coefficients of variation of intra-CVs between identical generics (mean±sd (min ~ max)) were 38.0±24.4% (1.9 ~ 105.3%) for AUC and 27.9±18.2% (4.0 ~ 70.1%) for Cmax. These results suggest that substantial variation exists among the bioequivalence results of identical generics. In this study, we presented the intra-CVs of various generics with their pooled intra-CVs. The estimated intra-CVs calculated in this study will provide useful information for planning future bioequivalence studies. (This is republication of the article 'Transl Clin Pharmacol 2017;25:179-182' retracted from critical typographic errors. See the 'Retraction and Republication section of this issue for further information). [ABSTRACT FROM AUTHOR]

Published

2018

146. S-1-Induced Lacrimal Drainage Obstruction and Its Association with Ingredients/Metabolites of S-1 in Tears and Plasma: A Prospective Multi-institutional Study.

Author

Namju Kim, Jin Won Kim, Je-Hyun Baek, Jin-Soo Kim, Ho-Kyung Choung, Tae-Yong Kim, Kyung-Hun Lee, Yung-Jue Bang, Sang In Khwarg, Sang-Hoon Ahn, Do Joong Park, Hyung-Ho Kim, Jae-Yong Chung, Soyeon Ahn, and Keun-Wook Lee

Subjects

METABOLITES, CANCER chemotherapy, FLUOROURACIL, UNIVARIATE analysis, ADVERSE health care events

Abstract

Purpose This prospective study was conducted to determine the incidence of lacrimal drainage obstruction (LDO) during S-1 chemotherapy and evaluate the association between the development of LDO and the concentrations of ingredients/metabolites of S-1 in tears and plasma. Materials and Methods A total of 145 patients with gastric cancer who received adjuvant S-1 therapy were enrolled. Ophthalmologic examinations were performed regularly during S-1 chemotherapy. Concentrations of tegafur, 5-chloro-2,4-dihydroxypyridine (CDHP), and 5-fluorouracil at steady-state trough level were measured in both tears and plasma. Results Fifty-three patients (37%) developed LDO. The median time to the onset of LDO was 10.9 weeks, and LDO developed most frequently in the nasolacrimal duct. Univariable analyses revealed that an older age (≥ 70 years), creatinine clearance rate (Ccr) < 80 mL/min, 5-fluorouracil concentration in plasma ≥ 22.3 ng/mL (median), CDHP concentration in plasma ≥ 42.0 ng/mL (median), and tegafur concentration in tears ≥ 479.2 ng/mL (median) were related to increased development of LDO. Multivariable analysis indicated that a high plasma 5-fluorouracil concentration was predictive of increased development of LDO (hazard ratio, 2.02; p=0.040), along with older age and decreased Ccr. Patients with LDO also developed S-1-related non-hematologic toxicity more frequently than those without LDO (p=0.016). Conclusion LDO is a frequent adverse event during S-1 chemotherapy. An older age, decreased Ccr, and high plasma 5-fluorouracil concentration were found to be independent risk factors for LDO. The high incidence of LDO warrants regular ophthalmologic examination and early intervention in patients receiving S-1 therapy. [ABSTRACT FROM AUTHOR]

Published

2018

147. The Political Economy of Development and Environment in Korea

Author

Jae-Yong Chung and Richard J. Kirkby

Published

2005

148. Effect of the UGT2B15 genotype on the pharmacokinetics, pharmacodynamics, and drug interactions of intravenous lorazepam in healthy volunteers

Author

Jae-Yong, Chung, Joo-Youn, Cho, Kyung-Sang, Yu, Jung-Ryul, Kim, Hye-Ryung, Jung, Kyoung-Soo, Lim, In-Jin, Jang, and Sang-Goo, Shin

Subjects

Adult, Male, Polymorphism, Genetic, Genotype, Valproic Acid, Lorazepam, Humans, Hypnotics and Sedatives, Drug Interactions, Female, Enzyme Inhibitors, Glucuronosyltransferase, Rifampin, Infusions, Intravenous

Abstract

Our objective was to investigate the effect of the uridine 5'-diphosphate-glucuronosyltransferase (UGT) 2B15 genetic polymorphism on the pharmacokinetics and pharmacodynamics of lorazepam in basal, inhibited, and induced metabolic states in healthy normal volunteers.Twenty-four healthy subjects were enrolled and grouped into UGT2B15*1/*1 or UGT2B15*2/*2 genotype groups. The pharmacokinetic and pharmacodynamic profiles of intravenous lorazepam were characterized before and after inhibition with 600 mg valproate once daily for 4 days and after induction with rifampin (INN, rifampicin) pretreatment (600 mg once daily for 10 days), with a washout period of 10 days between. The plasma concentrations of lorazepam and lorazepam glucuronide were analyzed before and at 0.25, 0.5, 1, 1.5, 2, 4, 6, 8, 12, 24, and 48 hours after lorazepam administration by liquid chromatography-tandem mass spectrometry. Visual analog scale assessments and psychomotor coordination tests were administered before and up to 12 hours after drug administration.The UGT2B15*2/*2 group showed 0.58-fold (95% confidence interval, 0.43-0.72; P.0001) lower systemic clearance during the basal state and 1.37-fold (95% confidence interval, 1.05-1.88; P = .037) higher area under the visual analog scale-time curve during the induced state compared with the UGT2B15*1/*1 group. The mean systemic clearance of lorazepam decreased by 20% in the inhibited state and increased by 140% in the induced state. During the inhibited or induced state, absolute values of clearance were consistently lower in the *2/*2 group, but the percent changes from baseline did not differ significantly by genotype.Our results suggest that the UGT2B15*2 polymorphism is a major determinant of interindividual variability with respect to the pharmacokinetics and pharmacodynamics of lorazepam.

Published

2005

149. Effect of OATP1B1 (SLCO1B1) variant alleles on the pharmacokinetics of pitavastatin in healthy volunteers

Author

Jae-Yong, Chung, Joo-Youn, Cho, Kyung-Sang, Yu, Jung-Ryul, Kim, Dal-Seok, Oh, Hye-Ryung, Jung, Kyoung-Soo, Lim, Ki-Ho, Moon, Sang-Goo, Shin, and In-Jin, Jang

Subjects

Adult, Male, Korea, Dose-Response Relationship, Drug, Genotype, Liver-Specific Organic Anion Transporter 1, Organic Anion Transporters, Asian People, Area Under Curve, Quinolines, Humans, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Alleles, Half-Life

Abstract

Pitavastatin is a potent, newly developed 3-hydroxy-3-methylglutaryl-coenzyme A reductase inhibitor for the treatment of hyperlipidemia. We characterized the effects of organic anion transporting polypeptide 1 B 1 (OATP 1 B 1) alleles *1a, *1b, and *15 on the pharmacokinetics of pitavastatin.Twenty-four healthy Korean volunteers who had previously participated in a pharmacokinetic study of pitavastatin (single oral dose, 1--8 mg) were further investigated. Subjects were grouped according to OATP 1 B 1 genotype. Dose-normalized area under the plasma concentration-time curve (AUC) and peak plasma concentration (C(max)) values were analyzed, because different dosages were administered to subjects, whereas the pharmacokinetics showed linear characteristics.Dose-normalized pitavastatin AUCs for *1b/*1b (group 1), *1a/*1a or *1a/*1b (group 2), and *1a/*15 or *1b/*15 (group 3) were 38.8+/-13.3, 54.4 +/-12.4, and 68.1+/-6.3 ng.h.mL(-1).mg(-1) (mean+/-SD), respectively, with significant differences between all 3 groups (P=.008) and between subjects carrying and those not carrying the *15 allele (P = .004). Dose-normalized pitavastatin C(max) values were 13.2+/- 3.3, 18.2+/-5.7, and 29.4+/- 9.6 ng.mL(-1).mg(-1) in groups 1, 2, and 3, respectively, and also showed significant differences (P=.003) in a manner similar to that shown by AUC. No significant differences were found between the genotype groups in terms of dose-normalized AUC or C(max) values of pitavastatin lactone.OATP 1 B 1 variant haplotypes were found to have a significant effect on the pharmacokinetics of pitavastatin. These results suggest that the *15 allele is associated with decreased pitavastatin uptake from blood into hepatocytes and that OATP 1 B 1 genetic polymorphisms have no effect on the pharmacokinetics of pitavastatin lactone.

Published

2005

150. A variant 2677A allele of the MDR1 gene affects fexofenadine disposition

Author

So-Young, Yi, Kyoung-Sup, Hong, Hyeong-Seok, Lim, Jae-Yong, Chung, Dal-Seok, Oh, Jung-Ryul, Kim, Hye-Ryung, Jung, Joo-Youn, Cho, Kyung-Sang, Yu, In-Jin, Jang, and Sang-Goo, Shin

Subjects

Adult, Male, Korea, Polymorphism, Genetic, Genotype, Genetic Variation, Exons, Gene Frequency, Haplotypes, Area Under Curve, Histamine H1 Antagonists, Humans, Female, Terfenadine, Genes, MDR, Alleles

Abstract

There have been considerable disagreements regarding the influence of MDR1 (ABCB1) polymorphisms on the disposition of P-glycoprotein (P-gp) substrates. We speculated that the unknown function of the A allele of exon 21 G2677T/A (Ala893Ser/Thr) provides one of the reasons for the contradictory results. This study was performed to clarify the effects of major MDR1 gene polymorphisms, including a variant A allele in exon 21, on fexofenadine pharmacokinetics.We investigated the occurrence of 3 high-frequency single-nucleotide polymorphisms (SNPs) in exons 12 (C1236T), 21 (G2677T/A), and 26 (C3435T) of the MDR1 gene in 232 healthy Koreans, using a polymerase chain reaction-restriction fragment length polymorphism method, and performed haplotype analysis on these 3 SNPs. A single oral dose of 180 mg fexofenadine hydrochloride was administered to 33 healthy Korean male volunteers, who were divided into 6 groups based on the MDR1 genotype for the G2677T/A polymorphism in exon 21 and the C3435T polymorphism in exon 26.A strong linkage disequilibrium was observed among the 3 SNPs. The frequencies of the 4 major haplotypes, 1236C-2677A-3435C, C-G-C, T-G-C, and T-T-T, were 16.4%, 18.6%, 21.6%, and 32.2%, respectively. Fexofenadine disposition varied considerably among the groups. In the 2677AA/3435CC genotype group (n=3), the values of area under the concentration-time curve from time 0 to 24 hours [AUC(0-24)] were significantly lower (P=.014) than those of the other 5 genotype groups (GG/CC, GT/CT, TT/TT, GA/CC, and TA/CT). As compared with the 2677GG/3435CC subjects, the AUC(0-24) values were 17% lower in the 2677AA/3435CC subjects and 47% higher in the 2677TT/3435TT subjects (GG/CC versus AA/CC versus TT/TT, 4017 +/- 1137 ng . h/mL versus 3315 +/- 958 ng . h/mL versus 5934 +/- 2,064 ng . h/mL; P=.018). By stratification for genotypes at position 3435, homozygous 3435TT subjects were found to have significantly higher AUC(0-24) (P=.024) and maximum plasma concentration (P=.040) values than CC subjects [AUC(0-24), 5934 +/- 2064 ng . h/mL versus 3998 +/- 1241 ng . h/mL; maximum plasma concentration, 958 +/- 408 ng/mL versus 673 +/- 242 ng/mL].The plasma concentrations of fexofenadine after a single oral administration were lower in 2677AA/3435CC subjects than in subjects with the other 5 genotype combinations of the SNPs of G2677T/A and C3435T. These findings confirm the importance of analyzing MDR1 haplotypes and provide a plausible explanation for the conflicting results regarding the effect of MDR1 polymorphisms on the disposition of P-gp substrates.

Published

2004