Your search keyword '"Sang-Goo, Shin"' showing total 262 results

1. Academic recognition and reality reflected in the poems of Seok Gok Lee, GyuJun

Author

Sang-Goo Shin

Subjects

Psychoanalysis, Poetry, Psychology

Published

2015

2. Prediction and visualization of CYP2D6 genotype-based phenotype using clustering algorithms

Author

Jae-Gook Shin, Sang-Goo Shin, and Eun Young Kim

Subjects

0301 basic medicine, clustering analysis, dextromethorphan, Receiver operating characteristic, CYP2D6, phenotype, Concordance, genotype, Computational biology, 030105 genetics & heredity, Biology, Phenotype, Standard deviation, 03 medical and health sciences, 030104 developmental biology, Genotype, Cutoff, Pharmacology (medical), Original Article, Allele, Cluster analysis

Abstract

This study focused on the role of cytochrome P450 2D6 (CYP2D6) genotypes to predict phenotypes in the metabolism of dextromethorphan. CYP2D6 genotypes and metabolic ratios (MRs) of dextromethorphan were determined in 201 Koreans. Unsupervised clustering algorithms, hierarchical and k-means clustering analysis, and color visualizations of CYP2D6 activity were performed on a subset of 130 subjects. A total of 23 different genotypes were identified, five of which were observed in one subject. Phenotype classifications were based on the means, medians, and standard deviations of the log MR values for each genotype. Color visualization was used to display the mean and median of each genotype as different color intensities. Cutoff values were determined using receiver operating characteristic curves from the k-means analysis, and the data were validated in the remaining subset of 71 subjects. Using the two highest silhouette values, the selected numbers of clusters were three (the best) and four. The findings from the two clustering algorithms were similar to those of other studies, classifying *5/*5 as a lowest activity group and genotypes containing duplicated alleles (i.e., CYP2D6*1/*2N) as a highest activity group. The validation of the k-means clustering results with data from the 71 subjects revealed relatively high concordance rates: 92.8% and 73.9% in three and four clusters, respectively. Additionally, color visualization allowed for rapid interpretation of results. Although the clustering approach to predict CYP2D6 phenotype from CYP2D6 genotype is not fully complete, it provides general information about the genotype to phenotype relationship, including rare genotypes with only one subject.

Published

2017

3. Antipsychotic discontinuation in first episode psychosis: a prospective study using [18F]DOPA and [11C]raclopride PET

Author

Eun-Sang Kim, Soo Yeon Kim, and Sang-Goo Shin

Subjects

Pharmacology, Pediatrics, medicine.medical_specialty, business.industry, medicine.medical_treatment, Discontinuation, 11c raclopride, Psychiatry and Mental health, 18f dopa, Neurology, First episode psychosis, medicine, Pharmacology (medical), Neurology (clinical), Antipsychotic, Prospective cohort study, business, Biological Psychiatry

Published

2019

4. Effects of HM30181, a P-glycoprotein inhibitor, on the pharmacokinetics and pharmacodynamics of loperamide in healthy volunteers

Author

Hyesun Han, Seo Hyun Yoon, Seung Hwan Lee, In-Jin Jang, Kyung Mi Park, Howard Lee, Sang-Goo Shin, Tae Eun Kim, Kyoung Soo Lim, Joo Youn Cho, and Kyung Sang Yu

Subjects

Pharmacology, Quinidine, Loperamide, business.industry, Crossover study, Bioavailability, Intestinal mucosa, Pharmacokinetics, Pharmacodynamics, medicine, Pharmacology (medical), Adverse effect, business, medicine.drug

Abstract

Aims HM30181 is a third generation P-glycoprotein (P-gp) inhibitor currently under development. The objectives of this study were to evaluate the effects of a single dose of HM30181 on the pharmacodynamics and pharmacokinetics of loperamide, a P-gp substrate, and to compare them with those of quinidine. Methods Eighteen healthy male subjects were administered loperamide alone (period 1) or with loperamide plus quinidine or HM30181 in period 2 or 3, respectively. In period 3, subjects randomly received one of three HM30181 doses: 15, 60 or 180 mg. Changes in pupil size, alertness, oxygen saturation and the oral bioavailability of loperamide were assessed in each period. In addition, the pharmacokinetics of HM30181 were determined. Results Pupil size, alertness and oxygen saturation did not change over time when loperamide alone or loperamide plus HM30181 was administered while HM30181 significantly increased the systemic exposure to loperamide, i.e. the geometric mean ratio (90% confidence interval) of AUC(0,tlast) for loperamide with and without HM30181 was 1.48 (1.08, 2.02). Co-administered quinidine significantly increased the systemic exposure to loperamide 2.2-fold (1.53, 3.18), which also markedly reduced pupil size, resulting in a decrease of 24.7 mm h in the area under the effect curve of pupil size change from baseline compared with loperamide alone. Conclusions HM30181 inhibits P-gp mainly in the intestinal endothelium, which can be beneficial because pan-inhibition of P-gp, particularly in the brain, could lead to detrimental adverse events. Further studies are warranted to investigate adequately the dose–exposure relationship of HM30181, along with its duration of effect.

Published

2014

5. Performance evaluation of BD Barricor™ with BD PST™ and BD SST II™

Author

H.D. Park, Sang-Goo Shin, and Jaewon Oh

Subjects

Biochemistry (medical), Clinical Biochemistry, General Medicine, Biochemistry

Published

2019

6. Pharmacokinetic-Pharmacodynamic Modelling of Biomarker Response to Sitagliptin in Healthy Volunteers

Author

In-Jin Jang, Bo Hyung Kim, Joo Youn Cho, Sang-Goo Shin, Sung Eun Kim, Dongwoo Kang, Kyoung Soo Lim, Kyung Sang Yu, Seo Hyun Yoon, and Jung-Ryul Kim

Subjects

Adult, Blood Glucose, Male, medicine.medical_specialty, Incretin, Pharmacology, Toxicology, Models, Biological, Sitagliptin Phosphate, Young Adult, Pharmacokinetics, Glucagon-Like Peptide 1, Internal medicine, medicine, Humans, Hypoglycemic Agents, Dose-Response Relationship, Drug, business.industry, Reproducibility of Results, General Medicine, Triazoles, Glucagon-like peptide-1, Healthy Volunteers, Dose–response relationship, Endocrinology, Pyrazines, Sitagliptin, Pharmacodynamics, Biomarker (medicine), business, Biomarkers, medicine.drug

Abstract

Pharmacokinetic/pharmacodynamic (PK/PD) models can be useful tools in new drug development and also optimal drug therapy in patients. This study was designed to develop a PK/PD model of sitagliptin based on the physiology of incretin. The PK/PD data included information derived from two different studies. Study 1 was conducted as a one-sequence, three-period, repeated-dose, dose escalation (sitagliptin 25, 50 and 100 mg q.d.) design in twelve healthy volunteers. Study 2 was a first-in-man study for the newly developed dipeptidyl peptidase-4 (DPP-4) inhibitor in healthy volunteers. In study 1, blood samples were collected to measure sitagliptin concentrations, DPP-4 activity and active glucagon-like peptide-1 (GLP-1) concentrations. In study 2, only data from the 'placebo group' were used, and blood samples were collected to measure DPP-4 activity, active GLP-1 concentrations and glucose concentrations. A PK/PD analysis was conducted using a non-linear mixed effects modelling approach. Sitagliptin pharmacokinetics was modelled using a two-compartment model with first-order absorption. Changes in DPP-4 inhibition were linked to the PK model using a sigmoid Emax model, whereas the active GLP-1 changes were explained using an indirect response model; this model incorporated the glucose and DPP-4 inhibition models. The PK/PD model developed adequately described the changes in sitagliptin concentration, DPP-4 inhibition and active GLP-1 concentration in healthy volunteers.

Published

2013

7. Increased Systemic Exposure of Fimasartan, an Angiotensin II Receptor Antagonist, by Ketoconazole and Rifampicin

Author

Min Goo Lee, Seo Hyun Yoon, Kyung Sang Yu, In-Jin Jang, Kyoung Soo Lim, So Jeong Yi, Tae Eun Kim, Im-Sook Song, Jung Won Kim, Sang-Goo Shin, and Joo Youn Cho

Subjects

Pharmacology, medicine.medical_specialty, business.industry, CYP3A, Cmax, Angiotensin II receptor antagonist, Crossover study, Endocrinology, Pharmacokinetics, Internal medicine, medicine, Pharmacology (medical), Fimasartan, Ketoconazole, business, Rifampicin, medicine.drug

Abstract

The authors studied the effects of ketoconazole and rifampicin on the pharmacokinetics of a single dose of fimasartan (BR-A-657), a newly developed angiotensin II receptor antagonist for the treatment of hypertension, in 22 healthy participants. Ketoconazole increased the maximumplasma concentration (Cmax) and area under the plasma concentration vs time curve to infinity (AUC∞ of fimasartan by 2.47-fold (90% confidence interval [CI], 1.61-3.79) and 2.03-fold (1.56-2.64), respectively. Concomitant administration of rifampicin increased the C(max) and AUC∞ of fimasartan by 10.33-fold (90% CI, 6.74-15.81) and 4.60-fold (3.54-5.97). In vitro studies indicated that ketoconazole inhibited the uptake of fimasartan into cells expressing OATP1B1 with a K(i) of 107.7 µM, and rifampicin inhibited OAT1- and OATP1B1-mediated fimasartan transport with a K(i) of 212 µM and 12.2 µM, respectively. The systemic exposure of fimasartan was significantly increased by coadministration of ketoconazole or rifampicin in healthy volunteers. This is consistent with the in vitro results, in which fimasartan is a substrate of CYP3A and OATP1B1.

Published

2013

8. Apple juice greatly reduces systemic exposure to atenolol

Author

Seo Hyun Yoon, Kyoung Soo Lim, In-Jin Jang, Hyewon Jeon, Ichiro Ieiri, Tsutomu Kotegawa, Kyung Sang Yu, Joo Youn Cho, Kyoichi Ohashi, Sang-Goo Shin, and Seung Hwan Lee

Subjects

Pharmacology, Malus, biology, medicine.drug_class, Chemistry, Absorption (skin), biology.organism_classification, Atenolol, Crossover study, Intestinal absorption, Pharmacokinetics, medicine, Ingestion, Pharmacology (medical), Antihypertensive drug, medicine.drug

Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • Atenolol is an antihypertensive drug, of which negligible amounts are metabolized. • Fruit juices may decrease the oral absorption of drugs by inhibiting intestinal drug transporters, as demonstrated in vitro and in vivo. WHAT THIS STUDY ADDS • The pharmacokinetic characteristics of atenolol were determined according to the SLCO2B1 genotype after apple juice administration in healthy Korean volunteers. • Apple juice ingestion markedly reduced the systemic exposure to atenolol, but genetic variations in SLCO2B1 were unlikely to contribute substantial variability to the pharmacokinetics of atenolol. AIM Fruit juice reduces the plasma concentrations of several β-adrenoceptor blockers, likely by inhibiting OATP2B1-mediated intestinal absorption. The aim of this study was to investigate the effects of apple juice on the pharmacokinetics of atenolol. METHODS Twelve healthy Korean volunteers with genotypes of SLCO2B1 c.1457C> T (*1/*1 (n= 6) and *3/*3 (n= 6)) were enrolled in this study. In a three-phase, one-sequence crossover study, the pharmacokinetics (PK) of atenolol was evaluated after administration of 50 mg atenolol. Subjects received atenolol with either 300 ml water, 1200 ml apple juice or 600 ml apple juice. RESULTS Apple juice markedly reduced the systemic exposure to atenolol. The geometric mean ratios (95% confidence intervals) of apple juice : water were 0.18 (0.13, 0.25, 1200 ml) and 0.42 (0.30, 0.59, 600 ml) for the AUC(0,tlast). In this study, the PK parameters of atenolol responded in a dose-dependent manner to apple juice. CONCLUSIONS Apple juice markedly reduced systemic exposure to atenolol. The genetic variation of SLCO2B1 c.1457C>T had a minimal effect on the pharmacokinetics of atenolol when the drug was administered with water or apple juice.

Published

2012

9. Multiple-dose pharmacokinetics of fesoterodine sustained-release in healthy Korean volunteers

Author

Dongseong Shin, Seung Hwan Lee, Sang-Goo Shin, Joo Youn Cho, KyoungSoo Lim, Kyung Sang Yu, In-Jin Jang, and Kwang-Hee Shin

Subjects

Adult, Male, Pharmacology, CYP2D6, Korea, business.industry, Antagonist, Cmax, Muscarinic Antagonists, Middle Aged, Cytochrome P-450 CYP2D6, Double-Blind Method, Pharmacokinetics, Delayed-Action Preparations, Fesoterodine, Humans, Medicine, Pharmacology (medical), Tolterodine, Benzhydryl Compounds, business, Adverse effect, Active metabolite, medicine.drug

Abstract

OBJECTIVE Fesoterodine is a pro-drug of the active metabolite 5-hydroxymethyl tolterodine (5-HMT), a muscarinic receptor antagonist. This study aimed to evaluate the safety profile and pharmacokinetic characteristics of multiple oral doses of sustained-release fesoterodine (fesoterodine SR) in healthy Korean males. METHODS A randomized, double-blind, placebo-controlled, multiple-dose study with two oral doses (4 mg and 8 mg) was conducted in healthy Korean male participants. The study drug was administered once daily for 5 days. The plasma concentration of 5-HMT was measured up to 72 hours after the last drug administration. The CYP2D6 genotype was analyzed using polymerase chain reaction (PCR) methods to assess the effect of genetic polymorphisms on the pharmacokinetic parameters. RESULTS 20 participants completed the study. The mean (SD) areas under the plasma concentration-time curves during the dosing interval (AUCτ) of the 4 mg and 8 mg dose groups were 26.1 (8.0) and 64.2 (30.5) μg·h/ml and the mean peak concentrations (Cmax) were 2.6 (0.7) and 6.0 (2.0) μg/ml, respectively, at steady-state. The mean AUCτ and Cmax of 5-HMT increased in approximately the same proportion as the dose increased. Fesoterodine SR was well tolerated without any serious adverse events or abnormal clinical laboratory findings. CONCLUSION Systemic 5-HMT exposure showed dose-proportional characteristics in the 4 mg to 8 mg dose range in healthy Korean males. Thus, 4 mg or 8 mg doses of fesoterodine SR taken once-daily were tolerable in healthy Korean males.

Published

2012

10. Reduced Valproic Acid Serum Concentrations Due to Drug Interactions With Carbapenem Antibiotics

Author

Kyung Sang Yu, Tae Eun Kim, Sang-Goo Shin, Hye Kyung Han, In-Jin Jang, So Jeong Yi, Kwang-Hee Shin, Joo Youn Cho, Kyoung Soo Lim, and Min Kyu Park

Subjects

Adult, Male, Drug, Imipenem, Carbapenem, Adolescent, media_common.quotation_subject, Pharmacology, Infections, Meropenem, Young Adult, chemistry.chemical_compound, Seizures, polycyclic compounds, medicine, Humans, Drug Interactions, Pharmacology (medical), Aged, Retrospective Studies, media_common, Valproic Acid, medicine.diagnostic_test, business.industry, Middle Aged, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Anti-Bacterial Agents, Carbapenems, chemistry, Therapeutic drug monitoring, Concomitant, bacteria, Female, lipids (amino acids, peptides, and proteins), Drug Monitoring, business, Ertapenem, Half-Life, medicine.drug

Abstract

The plasma concentrations of valproic acid (VPA) are known to decrease during the concomitant administration of carbapenem antibiotics, such as meropenem, imipenem, and ertapenem. This study summarizes 6 cases of drug-drug interactions between VPA and carbapenem antibiotics.To investigate the onset and severity of the reductions in the concentration of VPA in patients with or without the coadministration of carbapenem antibiotics, the authors performed a retrospective evaluation of therapeutic drug monitoring (TDM) reports that described a decrease in the serum concentrations of VPA during the concomitant use of carbapenem antibiotics from January 2008 to December 2010 in the Seoul National University Hospital. The evaluated TDM reports included 6 cases. The decrement ratio of the VPA serum concentration was calculated from the TDM reports, and the change in the half-life of the VPA was also estimated.Six cases presented with changes in the VPA serum concentration before and after the administration of carbapenem antibiotics. (Three cases were treated with meropenem, 2 were treated with ertapenem, and 1 was treated with imipenem.) The VPA concentrations reduced by (mean ± SD) 88.7 ± 5.3% (3 cases of meropenem), 74.0 ± 9.8% (2 cases of ertapenem), and 73.3% (1 case of imipenem), respectively, and the half-life of VPA reduced by 80.1 ± 9.0%, 64.4 ± 24.2%, and 50.6%, respectively.The interaction between VPA and carbapenem antibiotics caused decreases in the VPA serum concentrations; the extent of this decrease was greater in the meropenem-treated patients than in the imipenem-treated or ertapenem-treated cases. Because the therapeutic effect of VPA depends on its serum concentration, it should be recognized that there may be a loss of seizure control in patients using VPA with carbapenem antibiotics.

Published

2012

11. Assessment of the pharmacokinetics of co-administered metformin and lobeglitazone, a thiazolidinedione antihyperglycemic agent, in healthy subjects

Author

In-Jin Jang, Dong Hoon Shin, Sang-Goo Shin, Joo Youn Cho, Seo Hyun Yoon, Tae Eun Kim, and Kyung Sang Yu

Subjects

Adult, Male, Drug, medicine.medical_specialty, medicine.drug_class, media_common.quotation_subject, Cmax, Lobeglitazone, Pharmacology, law.invention, Pharmacokinetics, Randomized controlled trial, Tandem Mass Spectrometry, law, Internal medicine, Republic of Korea, medicine, Humans, Hypoglycemic Agents, Drug Interactions, PPAR alpha, Thiazolidinedione, media_common, Cross-Over Studies, business.industry, General Medicine, Middle Aged, Crossover study, Metformin, PPAR gamma, Pyrimidines, Endocrinology, Thiazolidinediones, business, Chromatography, Liquid, medicine.drug

Abstract

Lobeglitazone as a thiazolidinedione antihyperglycemic agent activates peroxisome proliferator-activated receptor (PPAR) γ and may be suitable as monotherapy or in combination with other antihyperglycemic agents. The primary objective of this study was to investigate potential pharmacokinetic interactions between lobeglitazone and metformin in healthy Korean subjects.A randomized, open-label, multiple-dose, three-treatment, three-period, three-sequence, crossover study was conducted in 24 healthy Korean male volunteers. Serial blood samples were collected after lobeglitazone (0.5 mg/day) and metformin (1000 mg/day) were administered alone or concomitantly for 5 days in each period, and drug concentrations were determined by liquid chromatography-tandem mass spectrometry. CLINICAL TRAIL REGISTRATION NUMBER: NCT01005160.The steady-state maximum plasma concentrations (C(max, ss); mean ± standard deviation) of lobeglitazone and metformin alone were 29.38 ± 5.25 ng/mL and 1661.84 ± 471.88 ng/mL, respectively; the C(max, ss) during co-administration were 27.15 ± 5.75 ng/mL and 1779.92 ± 405.20 ng/mL, respectively. The steady-state areas under the concentration-time curves during the dose interval (AUC(τ, ss); mean ± standard deviation) of sole administration of lobeglitazone and metformin were 277.53 ± 65.25 ng*h/mL and 9650.27 ± 2089.81 ng*h/mL, respectively. When lobeglitazone and metformin were administered concomitantly, the AUC(τ, ss) were 257.29 ± 60.61 ng*h/mL and 10600.58 ± 1960.40 ng*h/mL, respectively. The geometric mean ratios (90% confidence interval) of co-medication to lobeglitazone alone were 0.92 (0.87-0.97; C(max, ss)) and 0.93 (0.87-0.99; AUC(τ, ss)), and those for co-medication to metformin monotherapy were 1.09 (0.99-1.19; C(max, ss)) and 1.11 (1.04-1.19; AUC(τ, ss)). Both monotherapies and combination therapy were well tolerated; 52 self-resolving, non-serious adverse events were reported from 17 subjects.Lobeglitazone did not significantly affect the pharmacokinetics of metformin or vice versa when both drugs were co-administered. Lobeglitazone can be co-administered with metformin without dose adjustment for either agent. Therefore further patient studies are needed to corroborate these results.

Published

2012

12. The Effect of Fimasartan, an Angiotensin Receptor Type 1 Blocker, on the Pharmacokinetics and Pharmacodynamics of Warfarin in Healthy Korean Male Volunteers: A One-Sequence, Two-Period Crossover Clinical Trial

Author

In-Jin Jang, Won Seok Nam, Sung Eun Kim, Seo Hyun Yoon, Sang-Goo Shin, Kyung Sang Yu, Kyoung Soo Lim, Bo Hyung Kim, Namyi Gu, and Joo Youn Cho

Subjects

Adult, Male, Population, Tetrazoles, Angiotensin II receptor antagonist, Angiotensin Receptor Antagonists, Young Adult, Pharmacokinetics, Tandem Mass Spectrometry, Republic of Korea, Humans, Medicine, Drug Interactions, Pharmacology (medical), Fimasartan, International Normalized Ratio, education, Chromatography, High Pressure Liquid, Pharmacology, education.field_of_study, business.industry, Biphenyl Compounds, Warfarin, Anticoagulants, Stereoisomerism, Crossover study, Pyrimidines, Tolerability, Area Under Curve, Anesthesia, Pharmacodynamics, business, medicine.drug

Abstract

Fimasartan is an angiotensin II receptor antagonist used to treat hypertension.The aim of this study was to evaluate the effects of fimasartan on the pharmacodynamics and pharmacokinetics of warfarin in healthy volunteers to meet regulatory requirements for drug marketing and labeling in Korea.An open-label, 1-sequence, 2-treatment, 2-period crossover study was conducted in healthy male volunteers. The subjects were administered a single-dose of warfarin 25 mg on day 1. After a 7-day washout period, once-daily fimasartan 240 mg was administered every morning from day 8 to day 16. On day 11, warfarin 25 mg was administered concomitantly with fimasartan. Serial blood samples were collected for 144 hours after each warfarin dose. The plasma concentrations of R- and S-warfarin were analyzed by using HPLC-MS/MS, and the pharmacokinetic parameters were estimated by using noncompartmental analysis. The maximal international normalized ratio (INR) and the AUC-INR curve were evaluated to assess warfarin pharmacodynamics. Tolerability was assessed via vital sign measurements, physical examinations, ECGs, clinical laboratory tests, and adverse events.A total of 15 healthy Korean men aged 20 to 39 years (mean [SD], 26.7 [5.1] years) and weighing 60.2 to 85.7 kg (mean, 71.4 [8.3] kg) participated in the study; 12 completed the study. The geometric mean ratios (GMRs [90% CIs]) of C(max) and AUC(0-last) for R-warfarin were 1.06 (0.97-1.16) and 1.07 (1.03-1.12), respectively. For S-warfarin, the GMRs (90% CIs) of C(max) and AUC(0-last) were 1.02 (0.94-1.11) and 0.99 (0.94-1.04). The INR values reached 1.93 (0.31) and 1.96 (0.37) at 36 hours and decreased to1.2 at 144 hours after warfarin treatment alone and coadministered with fimasartan, respectively. The GMRs (90% CIs) of the maximal INR and AUC-INR curve were 1.01 (0.97-1.05) and 0.98 (0.96-1.01). One (7.7%) of the 13 subjects reported epistaxis during treatment with warfarin alone, and 2 (16.7%) of 12 subjects receiving the combination treatment experienced headache, skin erosion, and an increase in blood creatine phosphokinase. No subjects had an elevated INR4 or reported any symptoms related to hypotension, including fainting or dizziness.Multiple doses of fimasartan did not seem to alter the pharmacodynamics or pharmacokinetics of warfarin in this small, select population of healthy male volunteers.

Published

2012

13. Pharmacokinetic and Pharmacodynamic Properties of the Calcimimetic Agent Cinacalcet (KRN1493) in Healthy Male Korean Subjects: A Randomized, Open-Label, Single Ascending–Dose, Parallel-Group Study

Author

Namyi Gu, In-Jin Jang, Seung Hwan Lee, Sang-Goo Shin, Kyung Sang Yu, Kyoung Soo Lim, and Bo Hyung Kim

Subjects

Adult, Male, medicine.medical_specialty, Cinacalcet, Population, Administration, Oral, Naphthalenes, Pharmacology, Gastroenterology, Young Adult, Pharmacokinetics, Tandem Mass Spectrometry, Internal medicine, Republic of Korea, medicine, Humans, Pharmacology (medical), education, Adverse effect, Chromatography, High Pressure Liquid, Serum Albumin, education.field_of_study, Dose-Response Relationship, Drug, business.industry, Phosphorus, medicine.disease, Tolerability, Parathyroid Hormone, Area Under Curve, Pharmacodynamics, Population study, Calcium, Secondary hyperparathyroidism, business, medicine.drug

Abstract

Background Cinacalcet (KRN1493) was developed to manage secondary hyperparathyroidism in patients with chronic kidney disease. The characteristics of cinacalcet have not been studied in the Korean population. Objective The aim of this study was to evaluate the pharmacokinetic (PK) and pharmacodynamic (PD) properties and tolerability of single-dose cinacalcet 50 to 100 mg in healthy male Korean subjects for the purposes of a New Drug Application package for the Korean Food and Drug Administration. Methods A randomized, open-label, single ascending–dose, parallel-group study was conducted in healthy male Korean subjects. Subjects were randomly assigned to receive a single oral dose of cinacalcet 50, 75, or 100 mg. Serial blood samples for PK/PD analysis were taken for up to 96 hours after administration. Plasma cinacalcet concentrations were analyzed by HPLC-MS/MS. PK parameters were determined using noncompartmental methods. Plasma intact parathyroid hormone (iPTH) concentrations, albumin-corrected serum calcium concentrations, and serum phosphorus concentrations were measured for PD evaluation. For the evaluation of tolerability, adverse events (AEs) were collected using investigators' questionnaires, subjects' spontaneous reports, clinical laboratory tests, ECG, and physical examinations including vital sign measurements. Results Sixteen subjects in the 50-mg group, 16 in the 75-mg group, and 6 in the 100-mg group completed the study and were included in the PK/PD analysis. The mean (SD) age, height, and weight of the study population were 4.3 (3.0) years, 174.8 (4.9) cm, and 68.2 (7.5) kg, respectively. The median T max value in each of the 3 dose groups was 6.0 hours. Mean C max values in the 50-, 75-, and 100-mg dose groups were 12.0 (5.5), 17.2 (14.9), and 43.1 (15.5) μg/L; mean AUC 0–∞ values were 126.6 (56.4), 184.3 (87.9), and 417.4 (169.9) μg · h/L. Characteristics were not linear, based on the data over the dose range of 50 to 100 mg. Mean plasma iPTH concentrations in the 50-, 75-, and 100-mg dose groups were decreased from baseline by 64.0% (11.7%), 63.1% (14.6%), and 70.6% (6.3%). Albumin-corrected serum calcium concentrations displayed patterns similar to those of the plasma iPTH concentrations. Sixteen AEs were reported in 11 subjects. No clinically significant abnormalities were observed in the tolerability assessments. Conclusions A single oral dose of cinacalcet was well-tolerated up to 100 mg in this small, selected population of healthy male Korean subjects. In addition, the PK characteristics of cinacalcet and its accompanying PD changes—the decreases in the concentrations of plasma iPTH and albumin corrected serum calcium—were demonstrated in the same population. ClinicalTrials.gov identifier: NCT00942773.

Published

2012

14. Quantitative and Qualitative Analysis of CKD-501, Lobeglitazone, in Human Plasma and Urine Using LC–MS/MS and Its Application to a Pharmacokinetic Study

Author

Hyun Suk Shin, Jung-Ryul Kim, In-Jin Jang, Sang-Goo Shin, Kyung Soo Lim, Bora Kim, Seo Hyun Yoon, Joo Youn Cho, and Kyung Sang Yu

Subjects

Chromatography, Chemistry, Organic Chemistry, Clinical Biochemistry, Selected reaction monitoring, Lobeglitazone, Urine, Biochemistry, Analytical Chemistry, Qualitative analysis, Pharmacokinetics, Human plasma, Lc ms ms, medicine, medicine.drug, Glipizide

Abstract

A simple, rapid and sensitive LC–MS/MS method in positive ion mode was developed and validated to determine CKD-501, lobeglitazone, in human plasma and urine using glipizide as an internal standard (IS). Lobeglitazone is a novel thiazolidinedione (TZDs)-based peroxisome proliferator-activated receptor (PPAR) agonist, used for the management of type-2 diabetes. After mixing the IS, dissolved in acetonitrile, with a plasma or urine sample containing lobeglitazone, 10 μL of supernatant was injected into the LC–MS/MS system. Quantification was performed in the multiple reaction monitoring (MRM) mode using transition of 481.5 → 152.2 (m/z) for lobeglitazone and 446.1 → 321.2 (m/z) for the IS. The method showed good linearity over concentration ranges of 0.5–1,000 ng mL−1 for plasma and 0.2–250 ng mL−1 for urine (r 2 ≥ 0.9996). The mean percent extraction recovery of lobeglitazone was 90.8 % for plasma and 87.3 % for urine, while the recoveries of the IS were greater than 86.4 % for both. The intra-day and inter-day precision of plasma ranged from 1.1 to 3.7 and 2.5 to 3.3 % (RSD), respectively, and the intra- and inter-day precision of urine ranged from 1.5 to 2.7 and 3.2 to 3.5 %, respectively. This method is simple, sensitive, and applicable for the pharmacokinetic study of lobeglitazone in human plasma. Most of the urine concentrations of lobeglitazone were below the LLOQ because the lobeglitazone is extensively metabolized.

Published

2012

15. Pharmacodynamic comparison of two formulations of Acarbose 100-mg tablets

Author

Hyeong-Seok Lim, In-Jin Jang, Kyung Sang Yu, Sang-Goo Shin, Seung Hwan Lee, Kyoung-Sup Hong, Jae Yong Chung, Seung Hee Yang, and S. Y. Byun

Subjects

Pharmacology, business.industry, Bioequivalence, Placebo, Crossover study, Confidence interval, Pharmacokinetics, Pharmacodynamics, Medicine, Pharmacology (medical), Dosing, business, Acarbose, medicine.drug

Abstract

Summary What is known and Objective: Acarbose, an α-glycosidase inhibitor, is used to treat diabetic patients. Pharmacokinetic evaluation of acarbose is difficult because

Published

2012

16. Tolerability and Pharmacokinetics of a New P-Glycoprotein Inhibitor, HM30181, in Healthy Korean Male Volunteers: Single- and Multiple-Dose Randomized, Placebo-Controlled Studies

Author

In-Jin Jang, Tae Eun Kim, Sang-Goo Shin, Namyi Gu, Seo Hyun Yoon, Kyung Mi Park, Kyung Sang Yu, and Joo Youn Cho

Subjects

Adult, Male, Pharmacology, business.industry, Tetrazoles, Urine, Isoquinolines, Placebo, Bioavailability, Young Adult, Double-Blind Method, Tolerability, Pharmacokinetics, Oral administration, Anesthesia, Humans, Medicine, Benzopyrans, Pharmacology (medical), ATP Binding Cassette Transporter, Subfamily B, Member 1, Dosing, Adverse effect, business

Abstract

HM30181 is an oral P-glycoprotein (P-gp) inhibitor developed to enhance the oral bioavailability of P-gp substrate drugs.The objective of this study was to investigate the tolerability and pharmacokinetic properties of HM30181 after single and multiple oral administrations to healthy Korean male volunteers. The study was performed to meet regulatory criteria for marketing the test product in South Korea.A dose-block-randomized, double-blind, placebo-controlled, dose-escalation study was performed in 180-, 360-, 600-, and 900-mg single-dose groups and 60-, 180-, and 360-mg multiple-dose groups with 10 subjects (8 active; 2 placebo) per group. In the single-dose study, blood and urine samples were collected for up to 120 hours after drug administration. In the multiple-dose study, subjects received the study drug or placebo orally once daily for 5 days. Blood samples were collected up to 624 hours after the last dose, and up to 24 hours after the first dose to evaluate the accumulation index. Urine samples were collected up to 120 hours after the last dose. Pharmacokinetic analysis was performed using noncompartmental methods. Adverse events were collected by the spontaneous reporting of the subjects or when subjects were asked general health-related questions.Thirty and 70 healthy male volunteers completed the single- and multiple-dose studies, respectively. Mean (SD) age and body weight of subjects in the single administration group were 24.0 (1.8) years and 68.8 (7.4) kg, respectively, and those of the multiple administration group were 24.5 (2.6) years and 67.6 (7.7) kg, respectively. The plasma concentrations peaked at 14 to 42 hours and declined with t(½) of 75.7 to 169.3 hours after single administration, and peaked at 5.5 to 8.0 hours and declined with t(½) of 153.5 to 215.2 hours after multiple administrations. C(max) and area under the concentration curve within dosing intervals (AUC(τ)) increased dose dependently after single administration; however, dose-dependent increases in C(max) and AUC(τ) were not observed after multiple administrations. The fraction of drug excreted unchanged in urine was minimal, with values0.01% in all dose groups. HM30181 accumulated after multiple administrations with an accumulation index of 4.0 to 7.4. All adverse events reported were mild in intensity; there were no serious adverse events reported. The most frequently reported adverse event was gastrointestinal disorder.HM30181 was well tolerated after oral administration within the dose range evaluated, with the exception of the repeated administration of 360 mg, for which gastrointestinal disorders were frequently reported. The systemic exposure of HM30181 was relatively low, and dose proportional properties of HM30181 were not observed.

Published

2012

17. Assessment of the Drug–Drug Interactions Between Fimasartan and Hydrochlorothiazide in Healthy Volunteers

Author

Seo Hyun Yoon, Sang-Goo Shin, Kyung Sang Yu, Kyoung Soo Lim, In-Jin Jang, Joo Youn Cho, Hyewon Jeon, JaeWoo Kim, and Kwang-Hee Shin

Subjects

Adult, Male, Drug, Angiotensin receptor, media_common.quotation_subject, Administration, Oral, Tetrazoles, Pharmacology, law.invention, Young Adult, Hydrochlorothiazide, Pharmacotherapy, Randomized controlled trial, Pharmacokinetics, Tandem Mass Spectrometry, law, Renin, Healthy volunteers, medicine, Humans, Drug Interactions, Fimasartan, Aldosterone, Antihypertensive Agents, Chromatography, High Pressure Liquid, media_common, business.industry, Biphenyl Compounds, Middle Aged, Pyrimidines, Drug Therapy, Combination, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Fimasartan is a selective angiotensin II receptor blocker. Hydrochlorothiazide (HCTZ), which is used to treat hypertension and edematous conditions, is coadministered with many antihypertensive agents.An open-label, randomized, multiple-dosing, 2-arm, 1-sequence, 2-period study was conducted to assess the effects of fimasartan (240 mg) on HCTZ (25 mg) or vice versa in 18 and 14 healthy male volunteers, respectively. During each drug administration period, drugs were given once daily for 7 days, with a 7-day washout period between the 2 administration periods.The respective geometric mean ratios of fimasartan for AUC τ,ss and C max,ss with HCTZ were 1.30 [90% confidence interval (CI), 0.84-2.01] and 1.17 (90% CI, 0.93-1.47) compared with fimasartan alone. The respective geometric mean ratios of HCTZ for AUC τ,ss and C max,ss with fimasartan were 0.94 (90% CI, 0.84-1.04) and 0.88 (90% CI, 0.80-0.97) compared with HCTZ alone. Plasma renin activity indicated no significant differences between fimasartan monotherapy and coadministered treatment.Fimasartan administered alone or in combination with HCTZ was well tolerated at the described dosages. Coadministration of fimasartan increased the urinary excretion of HCTZ and urine volume, but these observations are unlikely to have any clinical relevance.

Published

2012

18. Tolerability and Pharmacokinetics of Lobeglitazone (CKD-501), a Peroxisome Proliferator-Activated Receptor-γ Agonist: A Single- and Multiple-Dose, Double-Blind, Randomized Control Study in Healthy Male Korean Subjects

Author

Joo Youn Cho, In-Jin Jang, Kyung Sang Yu, Dal Hyun Kim, Hyun Suk Shin, Jung Won Kim, Jung-Ryul Kim, Seo Hyun Yoon, Sang-Goo Shin, So Jeong Yi, and Kwang-Hee Shin

Subjects

Adult, Male, Agonist, medicine.drug_class, Lobeglitazone, Urine, Pharmacology, Placebo, law.invention, Placebos, Double-Blind Method, Pharmacokinetics, Randomized controlled trial, Reference Values, law, medicine, Humans, Hypoglycemic Agents, Pharmacology (medical), Adverse effect, business.industry, PPAR gamma, Pyrimidines, Tolerability, Area Under Curve, Thiazolidinediones, business, Chromatography, Liquid, medicine.drug

Abstract

Background Lobeglitazone, a peroxisome proliferator-activated receptor-γ (PPAR-γ) agonist with partial PPAR-α affinity, was developed to treat type 2 diabetes mellitus. Objective This study's aim was to evaluate the tolerability and pharmacokinetic (PK) properties of lobeglitazone to satisfy regulatory requirements for marketing approval in Korea. Methods A block-randomized, double-blind, placebo-controlled, single- and multiple-dose study was conducted in healthy subjects. In the pilot study, 4 subjects were administered 0.5 mg, including 1 receiving a placebo. Then, the single-dose study was conducted with 1, 2, 4, and 8 mg doses (8 subjects in each group, including 2 receiving placebos), followed by the multiple-dose study with 1, 2, and 4 mg doses (once daily for 7 days; 8 subjects in each group, including 2 receiving placebos). Serial samples of blood and urine were collected and drug concentrations were determined by high turbulence liquid chromatography-LC/MS/MS. Tolerability assessments were performed throughout the study. Adverse events (AEs) were determined from general health-related questions and self-reports. Results Thirty-six (mean [SD]; age, 23.6 [2.7] years; weight, 70.0 [6.9] kg) and 25 Korean male subjects (age, 23.5 [3.1] years; weight 69.4 [9.4] kg) were enrolled in the single- and multiple-dose studies, respectively. The data from subjects administered lobeglitazone who completed the study (27, single; 18, multiple) was included in the PK analyses. In the single-dose study, the AUC and C max of lobeglitazone increased with the dose. After repeated dosing for 7 days, the accumulation ratio ranged from 1.1 to 1.4. A total of 25 AEs were reported by 11 (30.6%) and 8 subjects (33.3%) in the single- and multiple-dose studies, respectively. All AEs were mild in intensity and not serious. Conclusions Lobeglitazone was well tolerated in this small, selected group of healthy male Korean volunteers. The AUC and C max of lobeglitazone increased in a dose-proportional manner from 1 to 4 mg.

Published

2011

19. Pharmacokinetic Comparison of a New Sustained-Release Formulation of Glimepiride/Metformin 1/500 mg Combination Tablet and a Sustained-Release Formulation of Glimepiride/Metformin 2/500 mg Combination Tablet in Healthy Korean Male Volunteers: A Randomized, 2-Sequence, 2-Period, 2-Treatment Crossover Study

Author

Kyung Sang Yu, Joo Youn Cho, Seo Hyun Yoon, In-Jin Jang, Sang-Goo Shin, Sung Eun Kim, and Kwang-Hee Shin

Subjects

Adult, Male, Fixed-dose combination, Pharmacology, Pharmacokinetics, Reference Values, Tandem Mass Spectrometry, Diabetes mellitus, medicine, Humans, Hypoglycemic Agents, Pharmacology (medical), Dosing, Adverse effect, Cross-Over Studies, business.industry, Middle Aged, medicine.disease, Crossover study, Metformin, Drug Combinations, Glimepiride, Sulfonylurea Compounds, Delayed-Action Preparations, business, Chromatography, Liquid, Half-Life, medicine.drug

Abstract

Background The combination of glimepiride and metformin is used for glycemic control in patients with diabetes mellitus. A fixed-dose combination of glimepiride/metformin 2/500 mg slow-release (SR) formulation was developed to improve compliance in polymedicated patients. To accommodate the various dosing regimens of glimepiride, a glimepiride/metformin 1/500 mg SR tablet was also developed. Objective The goal of this study was to compare the pharmacokinetic properties of SR fixed-dose combinations of glimepiride/metformin 2/500 mg and the newly developed glimepiride/metformin 1/500 mg formulation to meet the regulatory requirements for marketing in Korea. Methods An open-label, randomized, 2-treatment, 2-period, 2-sequence crossover study was conducted with healthy male volunteers. Eligible subjects were randomly assigned to receive a single dose of glimepiride/metformin 1/500 mg SR (test) or glimepiride/metformin 2/500 mg SR (reference) followed by a 1-week washout period and then administration of the alternate treatment. Serial blood samples were collected immediately before and after dosing for 30 hours, and plasma concentrations were determined by using LC-MS/MS with validated methods. Adverse events were assessed by subjects' self-report and interviews addressing general health-related issues. Safety profiles were evaluated throughout the study. Results Thirty-three subjects were enrolled (mean [SD] age: 27.9 [4.95] years [range, 21–40 years]). Safety profiles were assessed for all 32 subjects who were administered the study drugs, and pharmacokinetic characteristics were evaluated in the 30 subjects who completed the study. The geometric mean ratios (90% CIs) of test to reference for the dose-normalized C max and AUC 0–last of glimepiride were 0.98 (0.90–1.07) and 1.06 (0.98–1.14), respectively. In the case of metformin, the geometric mean ratios (90% CIs) of test to reference for C max and AUC 0–last were 1.06 (0.98–1.15) and 1.04 (0.97–1.12), respectively. Nine adverse events were reported. Among them, loose stool, abdominal pain, and headache were considered to be likely related to the study drug. All reported adverse events were mild in intensity. Conclusions Dose-proportional characteristics of glimepiride and comparable pharmacokinetic properties of metformin were observed between the SR fixed-dose combinations of glimepiride/metformin 1/500 mg and 2/500 mg. A single dose of either treatment was well tolerated, and the safety profiles of the 2 treatments were comparable in this small, selected all-male group of healthy Korean volunteers. ClinicalTrials.gov identifier: NCT00934323.

Published

2011

20. Pharmacokinetic Profiles of Ceftazidime after Intravenous Administration in Patients Undergoing Automated Peritoneal Dialysis

Author

Sang-Goo Shin, Ki-Won Kim, Kwang-Hee Shin, Young Hwan Hwang, Curie Ahn, In-Jin Jang, Kook Hwan Oh, Min-Gul Kim, Yun Kyu Oh, Han Ro, and Kyung Sang Yu

Subjects

Adult, Male, medicine.medical_specialty, Metabolic Clearance Rate, medicine.medical_treatment, Population, Urology, Ceftazidime, Peritoneal dialysis, chemistry.chemical_compound, Pharmacokinetics, medicine, Humans, Pharmacology (medical), In patient, education, Aged, Pharmacology, education.field_of_study, Creatinine, business.industry, PK Parameters, Middle Aged, Anti-Bacterial Agents, Surgery, Automated peritoneal dialysis, Infectious Diseases, chemistry, Injections, Intravenous, Female, business, Peritoneal Dialysis, medicine.drug

Abstract

The pharmacokinetics (PK) of ceftazidime after intravenous (i.v.) administration during automated peritoneal dialysis (APD) and their dependence on peritoneal membrane transport are the targets of the present study. Eleven patients receiving a single i.v. dose of ceftazidime (15 mg/kg of body weight) (seven males, median [interquatile] age, 59 [36 to 62]) were recruited. Serum and dialysate samples were collected at the beginning, middle, and end of each of the five dwells during a 24-h period, with dwells 1, 2, and 3 using an automated cycler (designated on-cycler) and dwells 4 and 5 being manual exchanges (designated off-cycler), together with urine collection during the same period. Population PK analysis was employed to estimate the PK parameters. Peritoneal equilibration tests were performed for all patients, and correlations between peritoneal clearance (CL PD ) for ceftazidime and dialysate-to-plasma ratios for creatinine (D/P cr ) were obtained using the Spearman's product correlation coefficient (ρ). Ceftazidime renal clearance (CL renal ) was 0.052 ml/min/kg, and CL PD was 0.063 ± 0.050 ml/min/kg. CL PD for on- and off-cycler were 0.071 and 0.058 ml/min/kg ( P = 0.164), respectively. A significant correlation between CL PD and D/P cr was observed, with one outlier excluded, suggesting that CL PD for ceftazidime during APD is dependent upon the peritoneal small-solute transport rate. A model prediction yielded adequate serum and dialysate concentrations of ceftazidime throughout a 24-h period for sensitive organisms (MIC, 8 μg/ml) by either i.v. (at 15 mg/kg) or intraperitoneal (i.p.; at 20 mg/kg) administration during off-cycler dwells. The present study suggests that the i.v. administration of ceftazidime at 15 mg/kg or i.p. administration of ceftazidime at 20 mg/kg during a long dwell every 24 h can be recommended for treating systemic or intraperitoneal infections of APD patients.

Published

2011

21. Calculating Occupancy when One does not have Baseline: A Comparison of Different Options

Author

In-Jin Jang, Jae Min Jeong, Shitij Kapur, Sang-Goo Shin, Jae Sung Lee, Oliver D. Howes, Euitae Kim, Kyung Sang Yu, and Jun Soo Kwon

Subjects

Adult, Male, Occupancy, Intraclass correlation, Population, Aripiprazole, Quinolones, Pharmacology, Piperazines, Young Adult, Alkaloids, Dopamine receptor D2, Statistics, Methods, medicine, Humans, Baseline (configuration management), education, education.field_of_study, Receptors, Dopamine D2, Reproducibility of Results, Binding potential, Substitution method, Neurology, Positron-Emission Tomography, Schizophrenia, Original Article, Neurology (clinical), Cardiology and Cardiovascular Medicine, Psychology, Antipsychotic Agents, Protein Binding, medicine.drug

Abstract

Dopamine D2 receptor occupancy of antipsychotic drugs is calculated relative to the subject's D2 receptor binding potential (BP) in the drug-free state (baseline BP). Because baseline BP is seldom known in patients with schizophrenia, population means from unrelated control samples are often used to estimate it. However, this is likely to introduce bias and error into the occupancy measure. There is thus a need for a method to reliably estimate baseline BP for patient populations in whom it may be impractical or unethical to get baseline measurements. It has been previously found that the relationship between plasma concentration and dopamine receptor occupancy by antipsychotic drugs follows a sigmoid Emax model. Based on this, we developed a method for calculating dopamine D2 receptor occupancy by antipsychotic drugs using an inhibitory Emax model ( Imax method) that estimates individual baseline BPs. To validate this, we compared the result from the Imax method with actual occupancy and estimated occupancy calculated from the average baseline BP (substitution method). The data for validation were obtained from two different receptor occupancy studies with the antipsychotic medications YKP1358 and aripiprazole. We estimated the reliability between the true measured occupancy and the predicted occupancy using the intraclass correlation coefficient (ICC), and the variability of occupancy was also compared between the Imax and substitution methods. In YKP1358 study, all the ICCs of the Imax method were above 0.8, but those of the substitution method showed values lower than 0.8. In aripiprazole study, the ICCs of the Imax method were higher than those of the substitution method, but all the ICCs showed higher values than 0.8. The variability of Imax method was significantly smaller than that of substitution method in both studies. The Imax method shows better reliability and less variability than the substitution method. The Imax method can be applied for receptor occupancy study, and bring more reliability and accuracy to the occupancy study in patients with schizophrenia.

Published

2011

22. The use of healthy volunteers instead of patients to inform drug dosing studies: a [11C]raclopride PET study

Author

Euitae Kim, Jae Min Jeong, Jung Shin Park, Yong Gil Kim, Kyung Sang Yu, In-Jin Jang, Su Jin Kim, Jae Sung Lee, Sang-Goo Shin, Bo-Hyung Kim, Shitij Kapur, Oliver D. Howes, Federico Turkheimer, and Jun Soo Kwon

Subjects

Pharmacology, Raclopride, medicine.medical_specialty, medicine.medical_treatment, medicine.disease, Gastroenterology, Confidence interval, Pharmacokinetics, Dopamine receptor, Schizophrenia, Dopamine receptor D2, Internal medicine, medicine, Aripiprazole, Antipsychotic, Psychology, medicine.drug

Abstract

Receptor occupancy study has been performed to evaluate pharmacokinetic profiles in new antipsychotic drug development. While these findings highlight the value of positron emission tomography (PET) for dose-finding study, what is unclear is if it is necessary to conduct these studies in patients with schizophrenia or whether studies in healthy volunteers are adequate. To determine if it is necessary to conduct dopamine receptor occupancy studies in patients with schizophrenia or whether studies in healthy volunteers are adequate for dose-finding study, we compared the concentration–occupancy relationship in terms of EC50 between patients and healthy volunteers. Ten healthy volunteers and eight patients with schizophrenia participated in the study. We measured dopamine receptor occupancy using [11C]raclopride PET and plasma concentration of YKP1358, a novel antipsychotic drug under clinical development, at a number of time points after the administration of YKP1358. Pharmacokinetic data including area under the plasma concentration versus time curve, elimination half-life, maximum observed plasma concentration, and the time to reach the maximum observed plasma concentration were obtained. We explored the relationship between plasma concentration and dopamine D2 receptor occupancy using E max model and calculated EC50. The elimination half-life was longer in healthy volunteers than in patients. Other pharmacokinetic parameters were not significantly different between two groups. The EC50 was 7.6 ng/ml (95% confidence interval (CI) 6.2–9.0) in healthy volunteers and 8.6 (95% CI 7.4–9.9) in patients. The antipsychotic concentration–occupancy relationship in patients can be estimated from the EC50 data of healthy volunteers.

Published

2011

23. Translational and Clinical Pharmacology: Note from the new Editor-in-Chief

Author

Sang-Goo Shin

Subjects

medicine.medical_specialty, Editorial, Clinical pharmacology, business.industry, law, medicine, Editor in chief, MEDLINE, Pharmacology (medical), Medical physics, business, law.invention

Published

2019

24. Simultaneous LC–MS–MS Determination of HM30181A, [2-(2-{4-[2-(6,7-Dimethoxy-3,4-dihydro-1H-isoquinolin-2-yl)-ethyl]-phenyl}-2H-tetrazol-5-yl)-4,5-dimethoxyphenyl]amide, as a new P-Glycoprotein Inhibitor and Its Two Metabolites, M1 and M2, in Human Plasma: Application to a Pharmacokinetic Study

Author

In-Jin Jang, Sang-Goo Shin, Han Kyong Kim, Tae Eun Kim, Young Hee Choi, Namyi Gu, Joo Youn Cho, Kyung Sang Yu, Seul Oh, Seo Hyun Yoon, and Eun-Young Kim

Subjects

Chromatography, Chemistry, Formic acid, Metabolite, Organic Chemistry, Clinical Biochemistry, Ether, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, chemistry.chemical_compound, Liquid–liquid extraction, Liquid chromatography–mass spectrometry, Amide, Chemosensitizing agent

Abstract

A simultaneous simple, rapid, and sensitive LC–MS–MS method was developed and validated for the determination of HM30181A, [2-(2-{4-[2-(6,7-dimethoxy-3,4-dihydro-1H-isoquinolin-2-yl)-ethyl]-phenyl}-2H-tetrazol-5-yl]-4,5-dimethoxy-phenyl]amide, as a P-glycoprotein inhibitor and its two metabolites, M1 and M2, in human plasma using docetaxel as an internal standard (IS). The analytes were extracted from 200 μL of biological sample by liquid–liquid extraction using 1 mL of methyl-t-butyl ether. Chromatographic separation was carried on a Luna C8 column at 30 °C with mobile phase consisting of distilled water with 0.1% formic acid and acetonitrile (75:25, v/v) at a flow rate of 0.7 mL min−1 for human plasma samples. The method was linear over concentration ranges of 0.5–50, 0.1–10, and 0.1–10 ng mL−1 for HM30181A, M1, and M2, respectively, in human plasma. The values of coefficient variation for the assay precision were

Published

2011

25. Relative Bioavailability and Tolerability of Two Formulations of Bicalutamide 50-mg Tablets: A Randomized-Sequence, Open-Label, Two-Period Crossover Study in Healthy Korean Male Subjects

Author

Kyung Sang Yu, Seung Hwan Lee, Joo Youn Cho, In-Jin Jang, Sang-Goo Shin, and Seo Hyun Yoon

Subjects

Adult, Male, medicine.medical_specialty, Bicalutamide, Administration, Oral, Biological Availability, Bioequivalence, Pharmacology, Dosage form, law.invention, Tosyl Compounds, Young Adult, Randomized controlled trial, Pharmacokinetics, law, Internal medicine, Nitriles, Republic of Korea, Drugs, Generic, Humans, Medicine, Anilides, Pharmacology (medical), Cross-Over Studies, business.industry, Androgen Antagonists, Middle Aged, Crossover study, Bioavailability, Tolerability, Area Under Curve, business, Tablets, medicine.drug

Abstract

Background Bicalutamide is an oral nonsteroidal antiandrogenic drug used in the treatment of prostate cancer. A new generic 50-mg tablet formulation of bicalutamide has recently been developed. Objective This study evaluated the relative bioavailability and tolerability of the new generic formulation of bicalutamide 50-mg tablets (test) and the currently marketed formulation (reference) in healthy Korean male subjects. The study was conducted to meet Korean regulatory requirements for authorization to market the generic formulation. Methods This was a randomized-sequence, open-label study in which healthy Korean male subjects (aged 20–55 years) received single doses of the test and reference formulations in a 2-period crossover fashion, with a 6-week washout period between doses. Blood samples for the determination of plasma bicalutamide concentrations were obtained at regular intervals over 672 hours after dose administration. Pharmacokinetic parameters were determined using noncompartmental methods. Relative bioavailability was evaluated by comparing the log-transformed C max and AUC 0–672 of the 2 formulations; Korean regulatory requirements for the assumption of bioequivalence were met if the 90% CIs fell within the range of 0.80 to 1.25. Tolerability was assessed based on physical examinations, vital signs, clinical laboratory tests, electrocardiograms (ECGs), and adverse events (AEs) (spontaneously reported or observed by investigators). Results Of 47 volunteers screened for inclusion, 38 were enrolled and 32 completed the study (mean [SD] age, 24.9 [3.7] years; mean height, 173.8 [6.2] cm; mean weight, 66.1 [7.1] kg). Median T max was 24 hours for both formulations. The C max of the test and reference formulations was 1176.2 (191.6) and 1118.9 (209.5) μg/L, respectively. The corresponding values for AUC 0–672 were 277,503 (66,865) and 271,961 (75,597) μg · h/L. The 90% CIs for the geometric mean ratios of log-transformed C max and AUC 0–672 were 1.00 to 1.11 and 0.99 to 1.07, respectively. Thirty-three AEs were reported, including 17 events in 9 subjects who received the test formulation and 16 events in 12 subjects who received the reference formulation. All AEs were mild, and no subjects discontinued the study because of AEs. Conclusions In this single-dose study in healthy Korean male subjects, the pharmacokinetic parameters of the new generic formulation of bicalutamide 50-mg tablets did not differ significantly from those of the reference formulation. The new generic formulation met Korean regulatory criteria for the assumption of bioequivalence to the currently marketed formulation. Both formulations were well tolerated. Korea Food and Drug Administration registration number: PSPD 3057.

Published

2010

26. Pharmacokinetic and pharmacodynamic comparison of two recombinant human erythropoietin formulations after single subcutaneous administration: An open-label, sequence-randomized, two-treatment crossover study in healthy Korean male volunteers

Author

Kyu-Pyo Kim, Bo-Hyung Kim, In-Jin Jang, Sang-Goo Shin, Tae Eun Kim, and Kyung Sang Yu

Subjects

Adult, Male, medicine.medical_specialty, Reticulocytes, Anemia, Injections, Subcutaneous, Cmax, Hematocrit, Gastroenterology, Young Adult, Pharmacokinetics, Internal medicine, Republic of Korea, medicine, Humans, Pharmacology (medical), Erythropoietin, Pharmacology, Cross-Over Studies, medicine.diagnostic_test, business.industry, Epoetin alfa, medicine.disease, Crossover study, Recombinant Proteins, Epoetin Alfa, Therapeutic Equivalency, Area Under Curve, Pharmacodynamics, Anesthesia, Hematinics, business, medicine.drug

Abstract

Background: Recombinant human erythropoietin is indicated for the treatment of anemia resulting from chronic renal failure or chemotherapy. It is also used for patients at high risk for transfusions because of significant blood loss during surgery. A new recombinant human erythropoietin (epoetin alfa) that excludes fetal bovine serum and human serum albumin from among its ingredients was developed in Korea. This study was planned as part of a product development project at the request of the Korean regulatory agency. Objective: The aim of this study was to compare the pharmacokinetic and pharmacodynamic characteristics of a new recombinant human erythropoietin (test) formulation with an existing branded (reference) for- mulation after a single subcutaneous administration. Methods: An open-label, sequence-randomized, 2-period, 2-sequence, 2-treatment crossover study was conducted. Healthy male subjects were randomly assigned with a random number table into 1 of 2 sequence groups, and each subject was given recombinant human erythropoietin 4000 IU SC in the upper arm as the test formulation in one period and the reference formulation in the other period, according to the sequence group. Each period was separated by a 4-week washout period. Serial blood samples were taken up to 120 hours after drug administration for the pharmacokinetic assessments and up to 240 hours for reticulocyte counts as the pharmacodynamic end point. Pharmacokinetic analysis was performed without baseline correction. Adverse events (AEs) were collected by spontaneous reporting of the subjects or solicited by asking general health-related questions. Results: Twenty healthy men (mean [range] age, 25.6 [21–36] years; height, 175 [167–187] cm; weight, 70 [57.6–85.5] kg) were enrolled in and completed the study. The mean (SD) baseline erythropoietin plasma concentrations were 10.4 (2.4) mIU/mL for the test formulation and 10.8 (3.5) mIU/mL for the reference formulation. After the injection of 4000 IU SC per subject, the erythropoietin plasma concentrations reached a maximum at a median Tmax of 10 hours for both formulations (range: test formulation, 7.00–95.95 hours; reference formulation, 6.98–24.13 hours). The mean (SD) Cmax values for the test and reference formulations were 74.34 (30.63) and 80.46 (30.56) mIU/mL, respectively; the mean AUC0–last values were 3664 (731.5) and 3553 (723.2) mIU·h/mL. The ratios of the geometric mean (test/reference) for Cmax and AUC0–last were 0.92 (90% CI, 0.81–1.05) and 1.03 (90% CI, 0.98–1.09). The mean baseline hemoglobin, hematocrit, and reticulocyte counts were 15.4 g/dL, 45.5%, and 49.6 · 103/μL, respectively, for the test formulation and 15.5 g/dL, 45.3%, and 47.5 · 103/μL for the reference formulation. The mean reticulocyte counts slowly reached Tmax for both formulations at a median of 120 hours after administration (test formulation, 120.0 hours [range, 95.5–240.8 hours]; reference formulation, 120.1 hours [range, 72.0–240.5 hours]). The mean (SD) maximum reticulocyte counts for the test and reference formulations were 77.7 (12.2) · 103/μL and 80.7 (15.2) · 103/μL, respectively; values for area under the effect curve to the last observation (AUEC0–last) were 14,781.5 (2439.2) · 103/μL · h and 14,783.8 (2415.4) · 103/μL · h. The 2 agents did not exhibit any significant differences in maximum reticulocyte counts or AUEC0–last. During the study, a total of 6 AEs were reported, which were mild in severity. After the administration of test formulation, 1 case each of rhinorrhea, epigastric discomfort, and joint sprain (left ankle) were reported. After the administration of reference formulation, 2 cases of rhinorrhea and 1 case of cough were reported. Conclusion: In this small, selected group of healthy male volunteers, there were no significant differences in pharmacokinetic parameters or effects on reticulocytes between a test formulation and a reference formulation of recombinant human erythropoietin.

Published

2010

27. Effects of Pregnane X Receptor (NR1I2) and CYP2B6 Genetic Polymorphisms on the Induction of Bupropion Hydroxylation by Rifampin

Author

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

Subjects

Male, Receptors, Steroid, Genotype, CYP2B6, Pharmaceutical Science, Pharmacology, Biology, Hydroxylation, Polymorphism, Single Nucleotide, chemistry.chemical_compound, Asian People, Pharmacokinetics, medicine, Humans, Drug Interactions, Bupropion, Antibacterial agent, Pregnane X receptor, Pregnane X Receptor, Oxidoreductases, N-Demethylating, Hydroxybupropion, Cytochrome P-450 CYP2B6, chemistry, Female, Aryl Hydrocarbon Hydroxylases, Rifampin, medicine.drug

Abstract

We investigated genetic polymorphisms in the pregnane X receptor (NR1I2) in Korean individuals (n = 83) and the effects of NR1I2 genotypes on rifampin-mediated induction of bupropion hydroxylation. The pharmacokinetics of bupropion and hydroxybupropion were evaluated after an oral dose of bupropion (150 mg) administered before and after rifampin treatment for 7 days in 35 healthy subjects. The area under the time-concentration curve (AUC) ratio of hydroxybupropion to bupropion in CYP2B6*6 carriers was significantly lower than that in CYP2B6*6 noncarriers in both the basal and rifampin-induced states (p = 0.012). Among the CYP2B6*6 carriers (n = 13), the NR1I2 TGT (-25385T + g.7635G + g.8055T) carriers exhibited a significantly lower AUC ratio, representing the CYP2B6 hydroxylation activity, compared with the TGT noncarriers, in the induced state (11.9 versus 20.3, p = 0.045). The percent difference in the AUC ratio between the basal and induced states was also significantly different (212% versus 58.8%, p = 0.006). However, no significant difference was observed among the NR1I2 TGT genotypes for the CYP2B6*6 noncarriers (n = 22). In conclusion, it is suggested the NR1I2 TGT genotype decreases the bupropion hydroxylation induced by treatment with rifampin, particularly in CYP2B6*6 carriers.

Published

2010

28. Comparison of the bioavailability and tolerability of fixed-dose combination glimepiride/metformin 2/500-mg tablets versus separate tablets: A single-dose, randomized-sequence, open-label, two-period crossover study in healthy Korean volunteers

Author

Jung-Ryul Kim, Hyun Suk Shin, Namyi Gu, In-Jin Jang, Sang-Goo Shin, Joo Youn Cho, HyouYoung Rhim, Kyung Sang Yu, Jae Yong Chung, Bo Hyung Kim, and Seo Hyun Yoon

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Fixed-dose combination, Bioequivalence, Pharmacology, Gastroenterology, Young Adult, Asian People, Pharmacokinetics, Tandem Mass Spectrometry, Internal medicine, Humans, Hypoglycemic Agents, Medicine, Pharmacology (medical), Cross-Over Studies, Korea, business.industry, Crossover study, Metformin, Bioavailability, Drug Combinations, Glimepiride, Sulfonylurea Compounds, Therapeutic Equivalency, Tolerability, Area Under Curve, Drug Therapy, Combination, Female, business, Chromatography, Liquid, Tablets, medicine.drug

Abstract

Objective: This study compared the bioavailability and tolerability of a fixed-dose combination (FDC) tablet of glimepiride/metformin 2/500 mg and glimepiride 2-mg + metformin 500-mg tablets administered separately in healthy Korean subjects. Methods: In this single-dose, open-label, 2-period crossover study, healthy Korean volunteers were randomly assigned to receive, in 1 of 2 randomized sequences, an FDC tablet of glimepiride/metformin 2/500 mg (test) and glimepiride 2-mg + metformin 500-mg tablets administered separately (reference), with a 1-week washout period between treatments. Plasma concentrations of glimepiride and metformin were measured using LC/MS-MS. Pharmacokinetic parameters were analyzed using noncompartmental methods. Bioequivalence was concluded if the 90% CIs of the geometric mean test/reference ratios (GMRs) of the logarithm-transformed C max , AUC from 0 to 30 hours (AUC 0–30 ), and AUC 0−∞ values were within the predetermined regulatory range of 80% to 125%. Tolerability was assessed using physical examination and laboratory analysis. Results: A total of 32 subjects were enrolled (16 men [mean (SD) age, 21.8 (2.7) years (range, 18–26 years); weight, 68.9 (8.3) kg (range, 55.5–85.0 kg)]; 16 women [age, 23.5 (4.5) years (range, 20–38 years); weight, 51.7 (3.5) kg (range, 46.8–58.0 kg)]). The GMRs (90% CI) of glimepiride C max , AUC 0–30 , and AUC 0−∞ were 1.01 (0.91–1.11), 0.98 (0.92–1.03), and 0.97 (0.93–1.04), respectively. For metformin, these values were 0.96 (0.87–1.06), 0.96 (0.90–1.03), and 0.96 (0.90–1.03). A total of 49 adverse events (AEs) were reported in 10 subjects (31.3%) with the FDC and in 13 subjects (40.6%) with the separate tablets. The most commonly reported AEs with the test and reference treatments were dizziness (6 [19%] and 7 [22%]) and sweating (4 [13%] and 7 [22%]), respectively. The severity of all of the AEs was considered to be mild, and there were no significant differences in the prevalences of AEs between the 2 formulations. Conclusions: In this study in healthy Korean subjects, the requirements for bioequivalence of the glimepiride/metformin 2/500-mg FDC and coadministration of separate tablets of each drug were met. Both formulations were generally well tolerated.

Published

2010

29. A study of ways to vitalize of the coming-of-age ceremony by making use of an old street - around Sinmunwangno

Author

Sang-Goo Shin

Subjects

Win-win game, Courtesy, media_common.quotation_subject, Id, ego and super-ego, Political science, Media studies, Ceremony, media_common

Published

2010

30. Pharmacokinetics and pharmacodynamics of LC15-0444, a novel dipeptidyl peptidase IV inhibitor, after multiple dosing in healthy volunteers

Author

Joo Youn Cho, Kyung Sang Yu, Kyoung Soo Lim, Dong-Kyu Kim, Jung-Ryul Kim, Sung-Ho Kim, In-Jin Jang, Bo-Hyung Kim, Hwa-Sook Kim, Sang-Goo Shin, Sung-Hack Lee, and Hyeon Joo Yim

Subjects

Adult, Male, Metabolic Clearance Rate, Administration, Oral, Themed section: Obesity, Pharmacology, Placebo, Dipeptidyl peptidase, law.invention, Young Adult, Double-Blind Method, Pharmacokinetics, law, Humans, Medicine, Pharmacology (medical), Dosing, Organic Chemicals, Piperidones, Dipeptidyl-Peptidase IV Inhibitors, Korea, Clinical pharmacology, Dose-Response Relationship, Drug, business.industry, Gemigliptin, Pyrimidines, Drug development, Area Under Curve, Pharmacodynamics, business

Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • The importance of efficient drug development using biomarkers has been increasingly emphasized, from preclinical studies to clinical trials. • However, as yet few ‘validated’ or ‘qualified’ biomarkers are used in early-stage drug development in terms of clinical pharmacology and disease pathophysiology. WHAT THIS STUDY ADDS • This first-time-in-human study provides evidence of the pharmacological activity of LC15-0444 in humans, by using dipeptidyl peptidase IV activity and active glucagon-like peptide-1 concentrations. • LC15-0444 possesses pharmacokinetic and pharmacodynamic characteristics that support a once-daily dosing regimen. AIMS LC15-0444 is a selective and competitive inhibitor of dipeptidyl peptidase (DPP) IV with potential for the treatment of Type 2 diabetes. The aim was to investigate the pharmacokinetic (PK) and pharmacodynamic (PD) profiles after multiple oral ascending doses of LC15-0444 in healthy male subjects. METHODS A dose block-randomized, double-blind, placebo-controlled, parallel group study was performed in three groups with 10 subjects (eight for active drug; two for placebo) per group; each group received 200, 400 or 600 mg of LC15-0444 once daily for 10 days. Blood and urine samples were collected up to 24 h after the first dosing and up to 72 h after the last dosing. RESULTS The LC15-0444 concentration–time profiles exhibited characteristics of multicompartment disposition. No dose- or time-dependent change in PK parameters was observed. Mean elimination half-life was in a range 16.6–20.1 h in the dose groups. Mean renal clearance and fraction of unchanged drug excreted in urine was 18.6–21.9 and 0.40–0.48 l h−1, respectively. In the steady state, mean accumulation ratios by dose groups were between 1.22 and 1.31. More than 80% inhibition of DPP IV activity from baseline was sustained for >24 h in all dose groups. CONCLUSIONS This study provides evidence of the pharmacological activity of LC15-0444 in humans. LC15-0444 possesses PK and PD characteristics that support a once-daily dosing regimen.

Published

2009

31. Pharmacokinetic comparison of a new glimepiride 1-mg + metformin 500-mg combination tablet formulation and a glimepiride 2-mg + metformin 500-mg combination tablet formulation: A single-dose, randomized, open-label, two-period, two-way crossover study in healthy, fasting Korean male volunteers

Author

Sang-Goo Shin, In-Jin Jang, Kyung Sang Yu, Kwang-Hee Shin, Kyoung Soo Lim, Jung-Ryul Kim, Kyu-Pyo Kim, Joo Youn Cho, JaeWoo Kim, and Bo-Hyung Kim

Subjects

Adult, Male, medicine.medical_specialty, Chemistry, Pharmaceutical, Fixed-dose combination, Cmax, Pharmacology, Gastroenterology, Young Adult, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Hypoglycemic Agents, Pharmacology (medical), Adverse effect, Cross-Over Studies, business.industry, Fasting, Crossover study, Metformin, Drug Combinations, Glimepiride, Sulfonylurea Compounds, Tolerability, Area Under Curve, business, Half-Life, Tablets, medicine.drug

Abstract

Background: Coadministration of glimepiride and metformin has been used to achieve glucose control. Because compliance with a multiple medication regimen can be difficult for some patients, combination tablets of glimepiride + metformin might be a suitable alternative for these patients. Objective: This study was conducted to compare the pharmacokinetics of test and reference formulations of glimepiride + metformin fixed-dose combination tablets under fasting conditions to meet the regulatory requirements for marketing approval of a new drug in Korea. Methods: This was a single-dose, randomized, open-label, 2-period, 2-way crossover study conducted between March 2007 and May 2007. Healthy fasting Korean men were randomized to 1 of 2 dosing sequences: a single oral administration of a fixed-dose glimepiride 1-mg + metformin 500-mg combination tablet (test) followed by single oral administration of a fixed-dose glimepiride 2 mg + metformin 500 mg combination tablet (reference), separated by a 1-week washout period between doses; or a single oral administration of a fixed-dose glimepiride 2-mg + metformin 500-mg combination tablet followed by single oral administration of a fixed-dose glimepiride 1 mg + metformin 500-mg combination tablet, separated by a 1-week washout period between doses. Serial samples of blood were collected up to 24 hours after oral administration, and drug concentrations in plasma were determined by HPLC-MS/MS. Tolerability was assessed based on adverse events and changes in clinical parameters. Serious adverse events included those that resulted in death, a life-threatening condition, congenital anomaly or birth defect, or required hospitalization or prolongation of existing hospitalization. Results: A total of 30 healthy male subjects (mean age, 25.6 years [range, 20–36 years]; weight, 69.5 kg [range, 58.2–90.7 kg]) participated in the study. After administration of the test and reference formulations, glimepiride was rapidly absorbed, reaching C max with a median T max of 1.75 and 2.0 hours, respectively, and then declined exponentially with an average t½ of 8.2 and 8.5 hours. The individual C max and AUC last of glimepiride were observed to be proportionally increased according to the administered glimepiride dose. The mean (SD) dose-normalized Cmax values of glimepiride 1 and 2 mg were 168.2 (54.9) and 149.9 (47.4) ng/mL/mg, respectively; the mean dose-normalized AUC last values of glimepiride 1 and 2 mg were 681.5 (190.3) and 635.8 (194.1) ng · h/mL/mg. Individual plots of dose-normalized C max and AUC last values identified a similarity between the 2 groups but no significant between-group differences. A total of 25 adverse events (12 after the test dose and 13 after the reference dose) were reported by 13 of the 30 subjects. All adverse events were considered mild. Twenty-one adverse events were considered related to the study drug (8 after the test dose and 13 after the reference dose). Adverse events believed to be related to the test formulation were diarrhea (4 cases), dizziness (1), headache (1), tingling sensation (1), and weakness (1). Adverse events believed to be related to the reference formulation were diarrhea (6 cases), headache (3), cold sweats (1), dyspepsia (1), epigastric discomfort (1), and lethargy (1). There were no clinically significant findings in the laboratory test results or vital sign monitoring during the study. There were no serious adverse events reported. Conclusions: The C max and AUC last of glimepiride increased proportionally according to the administered glimepiride dose in this study of healthy, fasting Korean men. The safety profiles of the 2 combination tablets were comparable.

Published

2009

32. Effects ofAngelicae tenuissima radix, Angelicae dahuricae radixandScutellariae radixExtracts on CytochromeP450Activities in Healthy Volunteers

Author

Joo Youn Cho, Sojeong Yi, Jang Hee Hong, Kyoung Soo Lim, Kyu-Pyo Kim, Sang-Goo Shin, In-Jin Jang, JaeWoo Kim, Kyung Sang Yu, and Bo-Hyung Kim

Subjects

Adult, Male, Midazolam, Metabolite, Herb-Drug Interactions, Pharmacology, Toxicology, Dextromethorphan, Losartan, law.invention, Young Adult, chemistry.chemical_compound, Cytochrome P-450 CYP1A2, Tandem Mass Spectrometry, law, Caffeine, Republic of Korea, medicine, Humans, Radix, CYP2C9, Chromatography, High Pressure Liquid, Omeprazole, Angelica, Cytochrome P-450 CYP2C9, Traditional medicine, business.industry, CYP1A2, Cytochrome P-450 CYP2E1, General Medicine, Cytochrome P-450 CYP2C19, Chlorzoxazone, Cytochrome P-450 CYP2D6, chemistry, Aryl Hydrocarbon Hydroxylases, business, Phytotherapy, Chromatography, Liquid, Drugs, Chinese Herbal, Scutellaria baicalensis, medicine.drug

Abstract

Three kinds of herbal medicines, commonly used in Korea, Angelicae tenuissima radix, Angelicae dahuricae radix and Scutellariae radix were studied to evaluate their effect on cytochrome P450 (CYP) activities in healthy volunteers. A total of 24 healthy male volunteers were assigned to one of three parallel herbal treatment groups, each consisting of eight volunteers. A cocktail of probe drugs for CYP enzymes was orally administered before and after multiple administrations of herbal medicines, three times a day for 13 days. Probe drugs used to measure CYP activities were caffeine (CYP1A2), losartan (CYP2C9), omeprazole (CYP2C19), dextromethorphan (CYP2D6), chlorzoxazone (CYP2E1) and midazolam (CYP3A4). The probe drugs and their metabolites were quantified in plasma or urine using HPLC or LC-MS/MS. Changes in each CYP activity was evaluated by metabolic ratio of the probe drug (concentration ratio of metabolite to parent form at reference time point) following the herbal medication period, compared to the baseline values. A. dahuricae radix significantly decreased CYP1A2 activity to 10% of baseline activity (95% CI: 0.05-0.21). S. radix also showed significant changes in CYP2C9 and CYP2E1 activities. Compared to baseline values, the metabolic activities of losartan were decreased to 71% (0.54-0.94). In addition, S. radix showed a 1.42-fold (1.03-1.97) increase in chlorzoxazone metabolic activity. However, CYP activities were not meaningfully influenced by A. tenuissima radix. Changes in certain CYP activities were observed after the administration of S. radix and A. dahuricae radix in healthy volunteers. Therefore, herbal medicines containing S. radix or A. dahuricae radix are candidates for further evaluation of clinically significant CYP-mediated herb-drug interactions in human beings.

Published

2009

33. Comparison of the pharmacokinetics of ticlopidine between administration of a combined fixed-dose tablet formulation of ticlopidine 250 mg/Ginkgo extract 80 mg, and concomitant administration of ticlopidine 250-mg and ginkgo extract 80-mg tablets: An open-label, two-treatment, single-dose, randomized-sequence crossover study in healthy Korean male volunteers

Author

In-Jin Jang, Yong-Oh Lee, Hyunsuk Shin, Kyu-Pyo Kim, Sang-Goo Shin, Kyung Hee Lee, Kyung Sang Yu, Sojeong Yi, Tae Eun Kim, Bo-Hyung Kim, and JaeWoo Kim

Subjects

Male, Ticlopidine, Chemistry, Pharmaceutical, Bioequivalence, Mass Spectrometry, Electrocardiography, Pharmacokinetics, Bleeding time, medicine, Humans, Pharmacology (medical), Chromatography, High Pressure Liquid, Pharmacology, Cross-Over Studies, Korea, medicine.diagnostic_test, Plant Extracts, business.industry, Ginkgo biloba, Crossover study, Drug Combinations, Area Under Curve, Anesthesia, Concomitant, Platelet aggregation inhibitor, business, Platelet Aggregation Inhibitors, Half-Life, Blood sampling, medicine.drug

Abstract

Background: Ticlopidine is an antiplatelet agent used for the prevention of vascular accidents. In clinical practice in Korea, ginkgo extract may be administered along with ticlopidine to enhance the inhibition of platelet aggregation. Objective: To meet the requirements for marketing a combined fixed-dose formulation in Korea, the investigators compared the pharmacokinetic characteristics of ticlopidine in a combined fixed-dose tablet of ticlopidine/ginkgo extract with the concomitant administration of ticlopidine and ginkgo extract tablets. Methods: An open-label, 2-period, 2-treatment, single-dose, randomized-sequence crossover study was conducted in healthy Korean male volunteers. Subjects were randomly allocated to 2 sequence groups. In one period, a combined ticlopidine 250 mg/ ginkgo extract 80-mg fixed-dose tablet was administered and, in the other period, ticlopidine 250-mg and ginkgo extract 80-mg tablets were concomitantly administered. A 7-day washout separated the 2 periods. For analysis of pharmacokinetic properties, including C max , T max , t ½ , AUC 0−∞ , and AUC 0−last , serial blood sampling was performed up to 48 hours after study drug administration during each period. Ticlopidine concentrations in plasma were determined by a validated method using LC-MS/MS. In order for the 2 treatments to be considered bioequivalent, the 90% CI of the geometric means ratios for C max and AUC needed to be between 80% and 125%. Bleeding time was determined before dosing (0 hour) and at 5 and 24 hours after dosing. Adverse events (AEs) were identified through patient interview, recording of blood pressure, heart rate, and body temperature, physical examination, 12-lead ECG, and laboratory assessments. Results: Twenty-four healthy Korean male subjects (mean [range] age, 23.9 [22–38] years; height, 174.0 [162–184] cm; weight, 67.4 [56–80] kg) completed the study. Median (range) T max of ticlopidine was 1.5 (0.5–2.0) hours in both groups. The mean (SD) t ½ of ticlopidine in the combined fixed-dose formulation and the concomitant administration groups was 19.5 (3.4) and 19.0 (3.3) hours after study drug administration, respectively. The geometric means ratios of ticlopidine AUC 0−last , AUC 0–∞ , and C max between the combined fixed-dose formulation and concomitant administration were 1.04 (90% CI, 0.96–1.13), 1.04 (90% CI, 0.96–1.13), and 1.09 (90% CI, 0.96–1.23), respectively. The mean (SD) bleeding time at predose (0), and 5 and 24 hours after dose administration was 4.5 (1.6) to 5.4 (1.7) minutes in the combined fixed-dose formulation group and 4.4 (1.6) to 5.1 (1.1) minutes in the concomitant administration group. Five subjects (3 in the combined fixed-dose formulation group and 2 in the concomitant administration group) had bleeding times >8 minutes, but this was not considered to be clinically significant. A total of 24 AEs were reported in 13 of 24 subjects: nausea (3 cases), diarrhea (3), dizziness (3), epigastric discomfort (2), headache (2), rhinorrhea (2), purulent sputum (2), dyspepsia (1), upper abdominal pain (1), cough (1), pharyngolaryngeal pain (1), oropharyngeal swelling (1), dysphonia (1), and dysphagia (1). All were considered mild or moderate in nature. There was no statistically significant difference between the 2 treatments in the number of AEs or in the number of subjects who reported an AE. Conclusion: Administration of a single dose of a combined fixed-dose formulation of ticlopidine 250 mg/ ginkgo extract 80-mg tablets and concomitant administration of ticlopidine and ginkgo extract tablets did not result in statistically significant differences in the pharmacokinetics of ticlopidine in these healthy Korean male volunteers

Published

2009

34. Influence of alcohol on the hemodynamic effects and pharmacokinetic properties of mirodenafil: A single-dose, randomized-sequence, open-label, crossover study in healthy male volunteers in Korea

Author

Kyoung Soo Lim, Bo-Hyung Kim, In-Jin Jang, Sojeong Yi, JaeWoo Kim, Kyu-Pyo Kim, Bongyong Lee, Kyung Sang Yu, and Sang-Goo Shin

Subjects

Adult, Male, Time Factors, Randomization, medicine.drug_mechanism_of_action, Phosphodiesterase Inhibitors, Hemodynamics, Blood Pressure, Pyrimidinones, Electrocardiography, Young Adult, Pharmacokinetics, Humans, Medicine, Drug Interactions, Pharmacology (medical), Pharmacology, Sulfonamides, Mirodenafil, Cross-Over Studies, Korea, Ethanol, business.industry, Phosphodiesterase 5 Inhibitors, Crossover study, Blood pressure, Tolerability, Area Under Curve, Anesthesia, business, Phosphodiesterase 5 inhibitor

Abstract

Background: Mirodenafil is a phosphodiesterase type 5 (PDE-5) inhibitor developed for the treatment of erectile dysfunction. Mirodenafil has the possibility of being administered with alcohol. Objective: This study assessed the hemodynamic effects and pharmacokinetic properties of mirodenafil administered with alcohol. Methods: This single-dose, randomized-sequence, open-label, crossover study was conducted in healthy male volunteers at the Clinical Trials Center, Seoul National University Hospital, Seoul, Korea. Volunteers were randomly allocated to 1 of 3 randomized-sequence groups, each of which consisted of 3 administration phases, each separated by a 1-week washout period: oral mirodenafil 100 mg, alcohol 0.5 g/kg, and both. Vital signs (systolic blood pressure [SBP], dia-stolic BP [DBP], and pulse rate) were measured before (baseline) and at 0.5, 1, 1.5, 2, 2.5, 3, 3.5, 4, 5, 6, 8, 12, and 24 hours after administration. Because volunteers were given a standardized meal at 4 hours after mirodenafil and/or alcohol administration, hemody-namic results were assessed using the maximum decrease from baseline during a period of up to 4 hours after administration. For pharmacokinetic assessment, serial blood samples were collected before (baseline) and at 0.5, 1, 1.25, 1.5, 2, 2.5, 3, 4, 6, 8, 12, and 24 hours after administration. Tolerability was assessed using monitoring of adverse events (AEs), clinical laboratory parameters, and results of 12-lead electrocardiography. Results: A total of 20 subjects participated in the study (mean [range] age, 25.5 years [20–41 years]; weight, 69.8 kg [57.4–87.2 kg]; and height, 174.7 cm [168–186 cm]). Up to 4 hours after the administration of mirodenafil, alcohol, and mirodenafil + alcohol, the mean (SD) maximum decreases in SBP were 8.5 (3.5), 13.5 (7.8), and 15.1 (6.7) mm Hg, respectively, and the maximum decreases in DBP were 6.4 (4.8), 13.3 (7.4), and 13.8 (5.2) mm Hg. Simultaneous administration of mirodenafil + alcohol was associated with additional mean (95% CI) decreases in SBP and DBP of 1.7 mm Hg (−6.0 to 2.6 mm Hg) and 0.6 mm Hg (−4.7 to 3.6 mm Hg) compared with alcohol alone. Pharmacokinetic parameters of mirodenafil were not significantly different when the drug was administered with or without alcohol. The mean (SD) AUC 0−t values were 842.0 (434.7) ng/mL/h with mirodenafil and 833.4 (398.2) ng/mL/h with mirodenafil + alcohol. The most common AEs considered at least possibly related to study drug were nasal congestion (7 subjects [35%]), headache (3 [15%]), nausea (1 [5%]), and hiccups (1 [5%]). Conclusions: The concurrent administration of mirodenafil with alcohol was not associated with clinically significant hemodynamic changes in these healthy male volunteers in Korea. The pharmacoki-netics of mirodenafil were not significantly altered by this concurrent administration. Mirodenafil administered with alcohol had a tolerability profile comparable to that of mirodenafil alone.

Published

2009

35. Pharmacokinetics, pharmacodynamics, and tolerability of the dipeptidyl peptidase IV inhibitor LC15-0444 in healthy Korean men: A dose—block-randomized, double-blind, placebo-controlled, ascending single-dose, phase I study

Author

Joo Youn Cho, Sang-Goo Shin, Kyoung Soo Lim, Yunjung Choi, Jung-Ryul Kim, Kyung Sang Yu, In Jin Jang, Kwang-Hee Shin, J.Y. Kim, Kyu-Pyo Kim, Jang Hee Hong, Dal-Mi Hwang, O. Hwan Kwon, and Hyunsuk Shin

Subjects

Adult, Blood Glucose, Male, medicine.medical_specialty, Adolescent, Urinalysis, Metabolic Clearance Rate, Urine, Placebo, Gastroenterology, Food-Drug Interactions, Young Adult, Double-Blind Method, Pharmacokinetics, Glucagon-Like Peptide 1, Internal medicine, medicine, Humans, Insulin, Pharmacology (medical), Organic Chemicals, Chromatography, High Pressure Liquid, Piperidones, Pharmacology, Dipeptidyl-Peptidase IV Inhibitors, Korea, Dose-Response Relationship, Drug, medicine.diagnostic_test, business.industry, Gemigliptin, Pyrimidines, Endocrinology, Blood chemistry, Tolerability, Area Under Curve, Pharmacodynamics, business, Half-Life

Abstract

Background : LC15-0444 is a selective inhibitor of dipeptidyl peptidase (DPP) IV under investigation in Korea for the treatment of type 2 diabetes. Objective : The aim of this study was to investigate the pharmacokinetic (PK), pharmacodynamic (PD), and tolerability profiles of a single dose of LC15-0444 in healthy male subjects. Methods : A dose—block-randomized, double-blind, placebo-controlled, ascending single-dose, Phase I study was performed in healthy Korean male subjects assigned to receive 25, 50, 100, 200, 400, or 600 mg of LC15-0444 capsules. Blood and urine samples were collected up to 72 hours after administration. Plasma and urine drug concentrations were determined by tandem mass spectrometry coupled with high-performance liquid chromatography. DPP IV activity was measured by continuous spectrophotometric assay. An additional food effect study was performed in the 100-mg dose group; changes in PK and PD parameters after highfat diet were evaluated. Adverse events (AEs) were detected through investigator inquiries, spontaneous reports, and clinical evaluations such as physical examinations, vital sign measurements, 12-lead electrocardiography, clinical laboratory tests (eg, hematology, blood chemistry, coagulation, urinalysis), and computerized impedance cardiography. Results : Sixty Korean men (mean age, 25.3 years [range, 19-39 years]; weight, 68.3 kg [range, 53.6-84.9 kg]) were enrolled, providing 10 subjects for each dose group. After administration, LC15-0444 reached T max at 0.5 to 5.1 hours, and was eliminated with a t ½ of 16.7 to 21.3 hours. The mean fraction of unchanged drug excreted in urine ranged from 0.21 to 0.34 and mean renal clearance was 15.5 to 23.6 L/h. The dose-normalized AUC exhibited dose-linearity over the range of 50 to 400 mg. All doses of LC15-0444 =200 mg were found to inhibit 80% of DPP IV activity for 24 hours. High-fat diet did not significantly influence the AUC of LC15-0444. LC15-0444 was generally well tolerated. None of the subjects developed any serious clinical or laboratory AEs or discontinued the study due to an AE. All AEs were mild or moderate, and no dose-related trends were observed. Fortysix AEs were reported in 18 subjects (30.0%). AEs considered to be related to the study drug were headache (6 cases), dizziness (2), nausea (1), epistaxis (1), and increased heart rate (1). All AEs resolved spontaneously. Conclusions : A single dose of LC15-0444 exhibited linear PK properties over the range of 50 to 400 mg in these healthy Korean male subjects. PK characteristics were not significantly influenced by food. In addition, doses ≥200 mg of LC15-0444 inhibited plasma DPP IV activity by >80% over a 24-hour dosing interval, and a 600-mg dose increased active glucagon-like peptide-1 levels after a standardized meal. LC15-0444 was generally well tolerated.

Published

2008

36. 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

37. Duplex pyrosequencing assay of the 388A>G and 521T>C SLCO1B1 polymorphisms in three Asian populations

Author

Jae-Gook Shin, Sang-Goo Shin, Ji-Hong Shon, Sang-Seop Lee, Ho-Jung Shin, Eun Young Kim, and Doo-Yeoun Cho

Subjects

Adult, Male, Concordance, Clinical Biochemistry, Organic Anion Transporters, Biology, Biochemistry, Asian People, Humans, Amino Acids, Allele, Genotyping, Allele frequency, Alleles, Genetics, Polymorphism, Genetic, Liver-Specific Organic Anion Transporter 1, Biochemistry (medical), Haplotype, Sequence Analysis, DNA, General Medicine, Molecular biology, Haplotypes, Duplex (building), biology.protein, Pyrosequencing, Female, SLCO1B1

Abstract

Background We developed a method for detecting important SLCO1B1 polymorphisms and compared the haplotype frequencies in 3 Asian populations. Methods We designed a duplex pyrosequencing assay to detect simultaneously the 388A > G and 521T > C variants of SLCO1B1 ; this method can identify SLCO1B1⁎1b , SLCO1B1⁎5 , and SLCO1B1⁎15 . The method was validated by direct sequencing of 96 Korean subjects. In addition, duplex genotyping and the monoplex method were compared and validated with 469 Korean subjects. To characterize the haplotype frequencies based on the 2 polymorphisms, we genotyped 106 Chinese and 104 Vietnamese subjects, as well as Korean subjects, using the new method. Results The results showed 100% concordance among the monoplex and duplex pyrosequencing assays and direct sequencing method. The allele frequencies were similar in the 3 Asian populations: the most common allele was SLCO1B1⁎1b , while SLCO1B1⁎5 was rare or absent. The frequencies of functional SLCO1B1⁎15 alleles differed statistically between Chinese (8.2%) and Korean (14.0%) and Vietnamese (16.3%) ( p χ 2 -test). Conclusions The duplex pyrosequencing assay appears to be an accurate, rapid, and cost-effective genotyping method to detect major SLCO1B1 important alleles in Asian populations.

Published

2008

38. Modeling of Brain D2 Receptor Occupancy-Plasma Concentration Relationships with a Novel Antipsychotic, YKP1358, Using Serial PET Scans in Healthy Volunteers

Author

Jae Min Jeong, Jai Young Cho, Ji-Won Kwon, Won Jun Kang, Euitae Kim, Hwa-Sook Kim, Sang-Goo Shin, Jung-Ryul Kim, So Young Yoo, Jae Sung Lee, Kyoung Soo Lim, Kyung-Ho Yu, and Jang Ij

Subjects

Adult, Male, medicine.medical_specialty, medicine.drug_class, Administration, Oral, Atypical antipsychotic, Pharmacology, Models, Biological, Alkaloids, Pharmacokinetics, Dopamine, Internal medicine, Dopamine receptor D2, medicine, Humans, Pharmacology (medical), Carbon Radioisotopes, Raclopride, Dose-Response Relationship, Drug, medicine.diagnostic_test, Receptors, Dopamine D2, business.industry, Antagonist, Brain, Half-life, Dopamine D2 Receptor Antagonists, Endocrinology, Positron emission tomography, Area Under Curve, Positron-Emission Tomography, Dopamine Antagonists, business, Algorithms, Antipsychotic Agents, Half-Life, medicine.drug

Abstract

YKP1358 is a novel serotonin (5-HT2A) and dopamine (D2) antagonist that, in preclinical studies, fits the general profile of an atypical antipsychotic. We conducted a D2 receptor occupancy study with YKP1358 in healthy volunteers using positron emission tomography (PET) to measure the D2 receptor occupancy of YKP1358 and to characterize its relationship to plasma drug concentrations. A single oral dose, parallel group, dose-escalation (100, 200, and 250 mg) study was performed in 10 healthy male volunteers with the PET radiotracer [11C]raclopride. The D2 receptor occupancy of striatum was measured pre-dose, and at 2, 5, and 10 h after YKP1358 administration. Serial blood samples were taken for measurement of plasma YKP1358 concentrations. D2 receptor occupancy by YKP1358 increased to 53–83% at 2 h, and then decreased afterwards, ranging from 40–64% at 5 h to 20–51% at 10 h. The YKP1358 dose-plasma concentration relationship exhibited extensive variability, but there was a good relationship between plasma concentrations and D2 receptor occupancy that was well predicted by a sigmoid Emax model using nonlinear mixed effects modeling. To our knowledge, this is the first study in which the relationship between plasma concentration and the biomarker of D2 receptor occupancy was modeled using nonlinear mixed effects modeling. It is anticipated that these results will be useful in estimating for subsequent studies the initial doses of YKP1358 required to achieve a therapeutically effective range of D2 receptor occupancy. Clinical Pharmacology & Therapeutics (2007) 81, 252–258. doi:10.1038/sj.clpt.6100049

Published

2007

39. Effects of DRD2 and CYP2D6 genotypes on delta EEG power response to aripiprazole in healthy male volunteers: a preliminary study

Author

Euitae Kim, Joo Youn Cho, Yong-Wook Shin, In-Jin Jang, Sang-Goo Shin, So Young Yoo, Kyung Sang Yu, Jun Soo Kwon, and Young Youn Kim

Subjects

Adult, Male, CYP2D6, medicine.medical_specialty, Genotype, Metabolite, Aripiprazole, Quinolones, Pharmacology, Piperazines, chemistry.chemical_compound, Polymorphism (computer science), Internal medicine, medicine, Humans, Pharmacology (medical), Allele, Polymorphism, Genetic, Receptors, Dopamine D2, Reverse Transcriptase Polymerase Chain Reaction, Half-life, Electroencephalography, Psychiatry and Mental health, Phenotype, Endocrinology, Cytochrome P-450 CYP2D6, Neurology, chemistry, Area Under Curve, Pharmacodynamics, Neurology (clinical), Psychology, Antipsychotic Agents, Half-Life, medicine.drug

Abstract

The aim of the present study was to evaluate the effects of polymorphisms in dopamine D2 receptor (DRD2) and cytochrome P450 (CYP) 2D6 genes on delta EEG power response to aripiprazole in healthy male volunteers. Seventeen volunteers were recruited according to the DRD2 Taq1A genotype, and separated into the following groups: homozygous wild-type (A2/A2, n = 7), heterozygous (A2/A1, n = 5) and homozygous variant-type (A1/A1, n = 5) groups. After enrollment in this study, they were genotyped for CYP2D6. The volunteers received single 10 mg oral doses of aripiprazole, in accordance with an open-label parallel group study design. Plasma levels of aripiprazole and its metabolite were determined and EEGs were obtained simultaneously. The pharmacodynamic parameter was absolute delta power in the Cz channel. The changes of delta power were not different according to DRD2 Taq1A genotypes. As to the CYP2D6 allele, the subjects had the following CYP2D6 genotypes: *10/*10 (n = 4), *1/*10 (n = 5), *1/*5 (n = 2), *1/*1 (n = 3), *2/*41 (n = 1), *2/*2 (n = 1), *2N/*10 (n = 1). Subjects exhibiting the *1/*5 and *1/*10 genotypes showed a trend toward high area under the plasma aripiprazole concentration-time curve (AUC), which was linearly related to area under the EEG response-time curve (AUEC). Our results demonstrate a need for further evaluation of the CYP2D6 genotypic effect on the pharmacodynamics of aripiprazole.

Published

2006

40. 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

41. 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

42. Genetic Polymorphisms of SULT1A1 and SULT1E1 and the Risk and Survival of Breast Cancer

Author

Sei Hyun Ahn, Sang-Goo Shin, Jeong Soo Kim, Hye Won Chung, Kyoung Mu Lee, Ari Hirvonen, Ji Yeob Choi, Keun-Young Yoo, Sue Kyung Park, Daehee Kang, Wonshik Han, Dong Young Noh, and In Jin Jang

Subjects

Adult, Oncology, medicine.medical_specialty, Genotype, Epidemiology, Breast Neoplasms, Polymorphism, Single Nucleotide, Breast cancer, Risk Factors, Surveys and Questionnaires, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Aged, Proportional Hazards Models, Genetics, Korea, business.industry, Proportional hazards model, Smoking, Haplotype, Hazard ratio, Cancer, Odds ratio, Middle Aged, medicine.disease, Survival Analysis, Haplotypes, Case-Control Studies, Population study, Female, business

Abstract

We examined whether common single nucleotide polymorphisms (SNP) in SULT1A1 (c.779G>A, *14A>G, and *85C>T) and SULT1E1 (IVS1-447C>A, IVS4-1653T>C, and *959G>A) genes influenced the risk and survival of breast cancer. Our study population consisted of 989 histologically confirmed sporadic breast cancer patients and 1,054 controls without history of cancer recruited from three teaching hospitals in Seoul. Odds ratios (OR) and 95% confidence intervals (95% CI) were estimated by logistic regression model. In the survival analysis for 529 breast cancer patients with completed treatments, the hazard ratios (HR) were calculated with Cox proportional hazard model. Women with the SULT1E1 *959 GA/AA genotype had a moderately decreased breast cancer risk compared with those with the GG genotypes (OR, 0.8; 95% CI, 0.70-1.00). When the haplotypes were considered, the homozygous *959 AA genotype together with the IVS4-1653 T>C base change (CTA-CCA haplotype) was associated with halved breast cancer risk (OR, 0.5; 95% CI, 0.24-0.88) compared with the wild type CTG-CTG haplotype. No other significant overall association was observed between the SULT1A1 and SULT1E1 SNPs nor haplotypes and breast cancer risk. When stratified by survival, patients with the SULT1E1 IVS4-1653 TC/CC genotypes showed a >3-fold risk of recurrence (HR, 3.2; 95% CI, 1.39-7.48) compared with those with the TT genotype. Moreover, when the haplotypes were considered, the SULT1E1 *959 G>A base change together with the IVS4-1653 T>C base change (CTG-CCA haplotype) was associated with a >4-fold risk of breast cancer (OR, 4.2; 95% CI, 1.15-15.15). These findings suggest that genetic polymorphisms of SULT1E1 are associated with increased risk and a disease free survival of breast cancer in Korean women.

Published

2005

43. 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

44. 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

45. 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

46. Sensitive liquid chromatography assay with ultraviolet detection for a new phosphodiesterase V inhibitor, DA-8159, in human plasma and urine

Author

Joo Youn Cho, Sang-Goo Shin, Kyung-Sang Yu, Hyeong Seok Lim, In Jin Jang, and Hyun Joo Shim

Subjects

Phosphodiesterase Inhibitors, Potassium, Clinical Biochemistry, chemistry.chemical_element, Urine, Sensitivity and Specificity, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, chemistry.chemical_compound, 3',5'-Cyclic-GMP Phosphodiesterases, Liquid–liquid extraction, Potassium phosphate, Blood plasma, Humans, Chromatography, High Pressure Liquid, Cyclic Nucleotide Phosphodiesterases, Type 5, Sulfonamides, Chromatography, Phosphoric Diester Hydrolases, Chemistry, Extraction (chemistry), Reproducibility of Results, Cell Biology, General Medicine, Pyrimidines, Spectrophotometry, Ultraviolet, Quantitative analysis (chemistry)

Abstract

A sensitive high-performance liquid chromatographic (HPLC) method with ultraviolet absorption detection (292 nm) was developed and validated for the determination of the new phosphodiesterase V inhibitor, DA-8159 (DA), in human plasma and urine. A single step liquid–liquid extraction procedure using ethyl ether was performed to recover DA and the internal standard (sildenafil citrate) from 1.0 ml of biological matrices combined with 200 μl of 0.1 M sodium carbonate buffer. A Capcell Pak C18 UG120 column ( 150 mm ×4.6 mm I.D., 5 μm) was used as a stationary phase and the mobile phase consisted of 30% acetonitrile and 70% 20 mM potassium phosphate buffer (pH 4.5) at a flow rate of 1.0 ml/min. The lower limit for quantification was 5 ng/ml for plasma and 10 ng/ml for urine samples. Within- and between-run accuracy and precision were ≤15 and ≤10%, respectively, in both plasma and urine samples. The recovery of DA from human plasma and urine was greater than 70%. Separate stability studies showed that DA is stable under the conditions of analysis. This validated assay was used for the pharmacokinetic analysis of DA during a phase I, rising dose study.

Published

2003

47. Effect of Peritoneal Dialysis on Plasma and Peritoneal Fluid Concentrations of Isoniazid, Pyrazinamide, and Rifampin

Author

Ki-Won Kim, Suhnggwon Kim, Sang-Goo Shin, Curie Ahn, Kook-Hwan Oh, J.G. Lee, Yon-Su Kim, Kyung Yi Lee, Myung Don Oh, In Jin Jang, Jin Suk Han, and Jung Sang Lee

Subjects

Adult, Male, medicine.medical_treatment, Antitubercular Agents, Pharmacology, Peritoneal dialysis, Peritoneal Dialysis, Continuous Ambulatory, Pharmacokinetics, Isoniazid, medicine, Ascitic Fluid, Humans, Antibacterial agent, business.industry, Peritoneal fluid, Continuous ambulatory peritoneal dialysis, General Medicine, Middle Aged, Pyrazinamide, Nephrology, Female, Rifampin, business, Rifampicin, medicine.drug

Abstract

♦ Objective This study was performed to elucidate the pharmacokinetic profiles of antimycobacterial regimens for peritoneal dialysis patients. ♦ Patients Nine patients on maintenance continuous ambulatory peritoneal dialysis (CAPD) were included in this study. ♦ Methods After administering a conventional oral dose of antituberculosis medications, we measured plasma and peritoneal fluid concentrations of isoniazid by fluorometry, and rifampin and pyrazinamide by high performance liquid chromatography. The assay data were subjected to pharmacokinetic analysis. ♦ Results Average peak plasma concentrations of isoniazid, rifampin, and pyrazinamide were 3.3 mg/L, 6.5 mg/L, and 30.9 mg/L, respectively, all of which much exceed the minimum inhibitory concentration (MIC) for Mycobacterium tuberculosis. Peritoneal fluid concentrations of isoniazid and pyrazinamide were maintained well above the MICs for M. tuberculosis; however, peritoneal fluid concentration of rifampin was below the therapeutic range most of the time. ♦ Conclusion For the treatment of systemic or pulmonary tuberculosis in CAPD patients, no dose adjustments are required for isoniazid, rifampin, or pyrazinamide. On the contrary, for the treatment of tuberculous peritonitis, oral rifampin therapy is not expected to be effective because of its low peritoneal fluid concentration.

Published

2003

48. 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

49. Current status of the institutional review boards in Korea: constitution, operation, and policy for protection of human research participants

Author

Byung Joo Park, Ock Joo Kim, Sang-Goo Shin, Dong Ryul Sohn, and Seung Mi Lee

Subjects

Response rate (survey), Research design, Medical education, Research ethics, business.industry, Constitution, media_common.quotation_subject, education, Public policy, General Medicine, Indemnity, Institutional review board, humanities, Politics, Medicine, business, health care economics and organizations, media_common, Research Article

Abstract

The institutional review board is crucial to ensure the scientific and ethical quality of human participant research. This paper analyzes a survey on the current constitution and operation of institutional review boards (IRBs) in Korea, conducted by the Korean Association of Institutional Review Boards in April 2002. Out of 74 IRBs, 63 responded to the survey (85.1% response rate). IRB membership has a male-to-female ratio of approximately 80:20, a predominance of male clinicians (60%) and an underrepresentation of community people unaffiliated to the institutions (less than 10%). Most IRBs (around 80%) confine the scope of their reviews to the clinical evaluation of drugs or devices, leaving the remaining areas of research involving human participants untouched. As their role is limited, the majority of IRBs do not operate actively: 72% of responding IRBs reviewed less than one protocol per month in 2001. Sixty two percent of institutions have never discussed the need for insuring research participants' risks or making indemnity arrangements. This survey reveals many shortcomings and points for improvement by the institutional support bodies, including the need to establish regular education programs for IRB members and investigators.

Published

2003

50. Omeprazole hydroxylation is inhibited by a single dose of moclobemide in homozygotic EM genotype for CYP2C19

Author

Sang-Goo Shin, Joo Youn Cho, Kyung Sang Yu, In-Jin Jang, Dong-Seok Yim, and Byung-Hwan Yang

Subjects

Pharmacology, Chemistry, Cmax, CYP2C19, Drug interaction, Crossover study, Pharmacokinetics, Oral administration, Moclobemide, medicine, Pharmacology (medical), Omeprazole, medicine.drug

Abstract

Aims The pharmacokinetics of omeprazole and its metabolites in healthy subjects were evaluated to determine if a single dose of moclobemide inhibited CYP2C19 activity. Methods Sixteen volunteers, of whom eight were extensive metabolizers (EM) and eight were poor metabolizers for CYP2C19, participated in two studies. Venous blood samples were collected for 24 h after oral ingestion of 40 mg omeprazole with or without 300 mg moclobemide coadministration. The pharmacokinetic change of omeprazole, omeprazole sulphone and 5-hydroxyomeprazole concentrations were assessed to test for an interaction between omeprazole and moclobemide. Results The coadministration of moclobemide in EMs approximately doubled the mean AUC (from 1834 to 3760 ng ml−1 h) and Cmax (from 987 to 1649 ng ml−1) of omeprazole, and increased the AUC of omeprazole sulphone without changing AUC ratio of omeprazole to omeprazole sulphone. Moclobemide coadministration more than doubled the AUC ratio of omeprazole to 5-hydroxyomeprazole (from 2.5 to 5.3) in EMs, too. There was a significant decrease in Cmax and AUC of 5-hydroxyomeprazole in PMs but no significant changes were seen in the results for omeprazole and omeprazole sulphone AUCs. Conclusions A single dose of moclobemide resulted in significant suppression of CYP2C19 activity in EMs. We conclude that physicians prescribing moclobemide should pay attention to its pharmacokinetic interactions even on the first day of coadministration with CYP2C19 substrates.

Published

2002